Next Article in Journal
Exploring the Effectiveness and Durability of Trans-Kingdom Silencing of Fungal Genes in the Vascular Pathogen Verticillium dahliae
Next Article in Special Issue
1H NMR Metabolite Monitoring during the Differentiation of Human Induced Pluripotent Stem Cells Provides New Insights into the Molecular Events That Regulate Embryonic Chondrogenesis
Previous Article in Journal
Antimicrobial Peptide Mechanisms Studied by Whole-Cell Deuterium NMR
 
 
Search for Articles:
Title / Keyword
Author / Affiliation / Email
Journal
Article Type
 
 
Advanced Search
 
Section
Special Issue
Volume
Issue
Number
Page
 
Journals
IJMS
Volume 23
Issue 5
10.3390/ijms23052741
ijms-logo
Submit to this Journal Review for this Journal Propose a Special Issue
Article Menu

Article Menu

share Share announcement Help format_quote Cite question_answer Discuss in SciProfiles
first_page
settings
Order Article Reprints
Font Type:
Arial Georgia Verdana
Font Size:
Aa Aa Aa
Line Spacing:
Column Width:
Background:
Review

Ventx Family and Its Functional Similarities with Nanog: Involvement in Embryonic Development and Cancer Progression

by
Shiv Kumar
1,*,†,
Vijay Kumar
2,†,
Wenchang Li
1 and
Jaebong Kim
2,*
1
School of Psychology and Neuroscience, University of St Andrews, St. Mary’s Quad, South Street, St. Andrews KY16 9JP, UK
2
Department of Biochemistry, Institute of Cell Differentiation and Aging, College of Medicine, Hallym University, Chuncheon 24252, Gangwon-Do, Korea
*
Authors to whom correspondence should be addressed.
These authors contributed equally to this work.
Int. J. Mol. Sci. 2022, 23(5), 2741; https://doi.org/10.3390/ijms23052741
Submission received: 28 December 2021 / Revised: 21 February 2022 / Accepted: 27 February 2022 / Published: 1 March 2022
(This article belongs to the Special Issue Signals in Embryonic Germ Layer Specification)
Browse Figures
Versions Notes

Abstract

The Ventx family is one of the subfamilies of the ANTP (antennapedia) superfamily and belongs to the NK-like (NKL) subclass. Ventx is a homeobox transcription factor and has a DNA-interacting domain that is evolutionarily conserved throughout vertebrates. It has been extensively studied in Xenopus, zebrafish, and humans. The Ventx family contains transcriptional repressors widely involved in embryonic development and tumorigenesis in vertebrates. Several studies have documented that the Ventx family inhibited dorsal mesodermal formation, neural induction, and head formation in Xenopus and zebrafish. Moreover, Ventx2.2 showed functional similarities to Nanog and Barx1, leading to pluripotency and neural-crest migration in vertebrates. Among them, Ventx protein is an orthologue of the Ventx family in humans. Studies have demonstrated that human Ventx was strongly associated with myeloid-cell differentiation and acute myeloid leukemia. The therapeutic potential of Ventx family inhibition in combating cancer progression in humans is discussed. Additionally, we briefly discuss genome evolution, gene duplication, pseudo-allotetraploidy, and the homeobox family in Xenopus.

1. Introduction

Xenopus laevis is an established animal model for studying vertebrate development, neurobiology, immunology, cell biology, and toxicology [1,2]. Xenopus is a pseudo-tetraploidy organism [3,4]. Its genome tetraploidy arose from the merging of two progenitor ancestral frog genomes millions of years ago [3,4,5,6]. During genome evolution, the Xenopus laevis genome was subdivided into a longer subgenome (L-subgenome) and a shorter subgenome (S-subgenome). There is some gene duplication. However, most of the functional genes are located in the L-subgenome, while the majority of non-functional genes or pseudogenes are in the S-subgenome, formed by either the deletion of exons or frameshifts by single-nucleotide insertion/deletion [4,5,6,7]. The presence of non-functional genes or pseudogenes leads to doses compensation. Many families of transcriptional factors have evolved in vertebrates to regulate a wide network of downstream genes in a temporospatial-dependent manner to orchestrate orderly embryonic development and organogenesis [8,9,10]. Among those families, the homeobox domain-containing families, including the Ventx family, play crucial roles during embryonic development and are widely involved in tumorigenesis in vertebrates [9,11]. The Ventx family is a transcription-repressor family belonging to the NKL subclass. The NKL subclass is one of the subclasses of ANTP (the antennapedia gene, one of the Hox genes identified within the ANT-C homeotic complex of Drosophila) superfamily [8,9,11]. The Ventx family has been extensively studied in Xenopus, zebrafish, and humans. BMP4/Smad1 and FGF/Xbra signaling initiates the expression of the Ventx family members in Xenopus [12,13,14,15]. Recent studies have shown that BMP4/Smad1 and FGF/Xbra controlled the Ventx family expression in both Xenopus [13] and humans [16,17,18]. BMP4/Smad1 is involved in a signaling path leading to the positive regulation of the expression of Vega family genes (a homolog of Ventx family in Xenopus) in zebrafish [19,20,21]. Smad1 and Xenopus brachyury (Xbra) physically interact within the 5′-upstream regions of ventx1.1 and ventx2.1, either in combination or separately, to augment ventx1.1 and ventx2.1 transcription in Xenopus [13,14,16,22,23,24,25,26]. In addition, Ventx2.2 is an ortholog of Nanog in Xenopus and exhibited a sequential and functional similarity to Nanog and Barx1 [27,28]. Although studies have revealed that Ventx synteny has been evolutionarily conserved in cats (Chr28), humans (Chr10, q26.3 loci), Gallus (Chr6), zebrafish (Chr13 and Chr10), and Xenopus (Chr7), it is absent in rodents, including rats and mice (Figure 1) [13,29]. Ventx family genes are clustered at chromosome 7 in Xenopus, though it has been identified as non-clustered in zebrafish (Chr13 and Chr10). In humans, seven pseudogenes of the Ventx family have been discovered, dispersed throughout different chromosomal locations, including VENTXP1 (Xp21.3), VENTXP2 (13q31.1), VENTXP3 (12q21.1), VENTXP4 (3p24.2), VENTXP5 (8p12), VENTXP6 (8q21.11), and VENTXP7 (3p24.3) [11]. The Ventx family proteins play various roles during axial patterning, germ cell specification, and cell differentiation during the embryonic development of vertebrates [30,31,32,33,34,35,36,37,38]. Additionally, the Ventx family members trigger ventral mesoderm, ectoderm, and ventral-blood-island (VBI) formations [22,30,35,39,40,41,42]. In contrast, increased levels of the Ventx family directly suppresses the dorso-anterior development, inhibiting head formation and primary neurogenesis in Xenopus and zebrafish [15,30,33,34,38,43,44,45]. In Xenopus, the ectopic expression of Ventx family members attenuated the expression of organizer-specific genes, including goosecoid (gsc), chordin, noggin, and foxd4l1.1b (an early neural marker); and the same occurred for zic3 (a neuroectodermal marker) in Xenopus embryos at St.11 [13,30,33,34,35,45,46,47]. This attenuation caused the inhibition of dorsal mesoderm formation and neuroectodermal induction. The suppressed expression of organizer-specific genes resulted in a headless phenotype. Studies have shown that Ventx2.2/Xom acts as a Nanog-like pluripotency marker in Xenopus [48,49]. Overexpressed Ventx2.2 stabilizes the cells’ pluripotency and inhibits multiple-cell-lineage commitment during the embryonic development of X. laevis.
Similarly to Xenopus, BMP4/Smad1 controls the expression of the Vega family members [34,38,45]. The ectopic expression of Vega family members diminishes the dorsal and organizer-specific markers, leading to embryonic ventralization. Studies have found elevated levels of Ventx in acute-myeloid-leukemia (AML) cells, macrophages, and dendritic cells to promote their differentiation and leukemogenesis in humans and animal models [18,32,50,51]. Studies have shown that p53 transactivates the expression of p21 (p21Cip1/Waf1, an endogenous cell-cycle inhibitor) to inhibit the activity of cyclin–CDK complexes, including cyclin–Cdk1, cyclin–Cdk2, and cyclin–Cdk4/6 during G1 and S phases [52,53]. During DNA damage response, p53–p21 leads to cell senescence by inhibiting the CDK2/4–cyclinE/D1 complex, which arrests cell cycles. In contrast, Wu et al. (2011) revealed that Ventx directly transactivated the tumor suppression pathways in a p53–p21 and p16ink4a-Rb (a molecular link protein between cell senescence and tumor suppression)-dependent manner, leading to cellular senescence [54]. These studies suggested that the Ventx family plays multifaceted roles in hematopoietic cell differentiation and AML progression, tumor suppression, and apoptotic-pathway activation. We review these roles of the Ventx family in Xenopus, zebrafish, and humans and discuss the therapeutic potential of utilizing the Ventx family crosstalk pathways to inhibit cancer progression in humans. Additionally, we discuss the pseudo-tetraploidy, genome evolution, and gene duplication in Xenopus, Xenopus’s classes of the homeobox superfamily, and functional similarities of Ventx2.2 to Nanog and Barx1.

1.1. Xenopus laevis: Genome Evolution, Pseudo-Tetraploidy, and Gene Duplication

Polyploidization has been found in many animal species from annelids to insects, including some fish and amphibians [55]. However, polyploid animal species are relatively rare, as compared to those found in plants, and the possible barriers to generating polyploidization include the presence of sex chromosomes, the prevalence of cross-fertilization, and the histological complexity in evolutionally advanced animals. Despite these barriers, hermaphroditic polypoid species of amphibians continue to be discovered. Among vertebrates, the only diploid and polyploid hermaphroditic species are amphibians. (For reviews, see Schmid M. et al., 2015, and Becak et al., 2014 [55,56]). Two Xenopus species (i.e., X. laevis and X. tropicalis) have been used extensively for developmental, toxicological, immunological, genetic, and neurobiological studies [1,2]. Xenopus laevis is a polyploid species and an ideal model for studying the genome duplication. Xenopus laevis contains 36 chromosomes, nearly twice as many as in its close relative diploid X. tropicalis with 20 chromosomes [7]. Studies have reported that the allotetraploidy of X. laevis began by genome partitioning into two homoeologous S-subgenomes that then evolved separately and asymmetrically around 34 million years ago [6,57]. Around 17–18 million years ago, the genomes of these two diploid progenitor species combined to form an allotetraploid species (X. laevis) [5,6]. These two subgenomes are distinct but share the same nucleus (separate recombination identities). After the genomic merge, more than 56% of the genes were retained in two homoeologous copies on L and S chromosomes [6]. The L-subgenome retains most of the functional genes and more consistently resembles its progenitor’s condition, whereas the S-subgenome contains the majority of non-functional or pseudogenes due to deletions, insertions, rearrangements, and reduced expression. Therefore, X. laevis is considered a pseudo-tetraploid species. This asymmetry between the L and S-subgenomes could possibly have resulted from the intrinsic differences between their ancestral diploid progenitors. Additionally, the activation of transposable-elements-based remodeling of the S-subgenome might have been responsible for the L–S genome divergence itself. The L-subgenome of X. laevis is more closely related to the human genome than the S-subgenome of X. tropicalis [6]. A study reported that a single gene of X. tropicalis corresponded to precisely two co-orthologs in X. laevis, yet showed similar functionality in X. laevis [4]. The same study tested more than 2200 cases of gene duplication to show that the X. laevis genome possessed two co-orthologs of a gene in X. tropicalis. In contrast, single copies of X. laevis genes did not show similar outcomes to the ortholog of X. tropicalis. Duplicated genes can differ in expression levels and patterns, but not in molecular and biological functions. The duplication of gene sets is retained through a process of subfunctionalization (dosage compensation) and/or the relaxation of constraints on both copies of ancestral genes [4]. X. laevis thus provides a model for testing theories of whole genome duplication and significance, as its tetraploidization is neither too recent for studying the functions of a duplicated locus nor too ancient for measuring the impacts of single-nucleotide polymorphisms (SNPs) [4]. In addition, a recent genome-wide comparative study of aquaporins (AQPs) in allotetraploid X. laevis and diploid X. tropicalis revealed that the number of AQPs in X. laevis was nearly double (32) that of X. tropicalis (19) [3]. Meanwhile, a synteny-based analysis showed that the L-subgenome contained 17 AQPs, while the shorter S-subgenome had 15 AQPs. Additionally, six members of AQPs have been lost through evolution (i.e., two from the L-subgenome and four from the S-subgenome). These lost members are pseudogenized via either exon deletion or frameshift insertion and deletion. The merging of two ancestral genomes in the allotetraploid Xenopus laevis and the evolution of non-functional gene-duplication has indicated that Xenopus laevis is a pseudo-allotetraploid organism [2,3,5,6,7,55,57]. Consequently, the allotetraploidy of Xenopus laevis genome has become an important model in which to study polyploidy and aneuploidy formation. Tetraploidy and aneuploidy have been reported as having associations with various kinds of diseases in humans, such as cancers, Parkinson’s, aging disorders, Alzheimer’s, and neuromuscular developmental disorders [58,59,60,61,62,63,64,65,66].

1.2. Homeobox Domain (HD)

Homeobox domain is a well-conserved 60-aa-long DNA-binding domain (except the TALE superclass, which contains 63 aa instead of 60 aa), identified first in Drosophila [10,67]. In the last two decades, our understanding of the homeobox domain has expanded, and a large number of homeobox proteins in plants and animals have been discovered (see Burglin and Affolter 2016 for review) [9]. There are 16 known major classes in animals, including ANTP (HOXL and NKL), PRD, PRD-like, POU, HNF, CUT (subclasses ONECUT, CUX, SATB, CMP), LIM, ZF, CERS, PROS, and SIX/SO, along with the TALE superclass (subclasses IRO, MKX, TGIF, PBC, MEIS) (Figure 2). These homeobox proteins play diverse biological roles during development, such as in cell proliferation, pluripotency, and differentiation in a temporospatial and context-dependent manner [9]. The HD proteins are either transcription activators or repressors that directly interact with the 5′-upstream regions of genes to modulate gene transcription. ANTP inherited its name from the antennapedia (ANTP) gene, one of the Hox genes identified within the ANT-C homeotic complex of Drosophila [11]. The ANTP superfamily is the largest class of all homeobox-bearing families and contains two subclasses: Hox-like (HOXL) and NK-like (NKL). The defining features of the HOXL subclass are its arginine (Arg) residue at position 5 and a glutamine (Gln) residue at position 50 (or lysine at 51) in the HD sequence (Table 1) [9]. The signature of the NKL subclass is an arginine residue at position 5 (or glutamine at position 6) and a glutamine at position 50 in the HD. The HOXL subclass has 53 members, and the NKL subclass contains 60 members. The NKL subclass is further divided into various subfamilies, including Nkx, EN, Ventx, Vax, Emx, NOTO, etc. These subfamilies contain several homeobox-bearing proteins similar to Ventx (in Xenopus and humans) and Vega (in zebrafish), Barx1, and Nanog. In Xenopus, there have been 251 identified homeobox proteins (Table 2) [11]. The Ventx family is one of the recently identified groups that contains six genes in Xenopus and three genes in zebrafish. These members play important roles in embryogenesis, such as axial patterning, germ-layer specification, cell positioning, proliferation and differentiation, and pluripotency. The HD of the NKL class contains three helix domains, of which domains 2 and 3 form a helix–turn–helix (HTH). The HD directly binds with 5′-TAA(T/A)T-3 cis-acting consensus elements in the 5′-flanking regions of target genes and modulates their transcription in a temporospatial and context-dependent manner [8,13,26]. Additionally, there is a well-conserved motif of K/Q/R(I/T/V)WF in the three helices of all the HD classes [8,9,27]. However, the functional role of this motif remains largely unclear. However, a role in determining the HD-binding specificity to their target DNA has been suggested [8].

2. Ventx Family in Xenopus

In Xenopus, the Ventx family has six members, including Ventx1.1, Ventx1.2, Ventx2.1 Ventx2.2, Ventx3.1, and Ventx3.2 (Figure 3A). The phylogenetic tree of the Ventx family members in the Xenopus has indicated that Ventx1.1 and Ventx1.2 come from the same ancestor and showed 80.46% similarity in their protein sequences. However, Ventx3.1 and Ventx3.2 are the most differentiated members in the Ventx cluster and showed 51.15% similarity in their amino acid sequences in Xenopus laevis (Figure 3B,B’). All members of the Ventx family are positively regulated by BMP4/Smad1/5/8 signaling in the gastrulae, leading to ventral mesoderm, ectodermal formation, and embryonic ventralization [14,30,35]. Some members, such as Ventx1.1, Ventx2.1, and Ventx1.2, are also positively regulated by FGF/Xbra signaling in animal-cap explants, leading to mesodermal formation [13,23,35,70]. All members of Ventx are expressed in the ectoderm and ventral mesoderm of Xenopus embryos after mid-blastula transition (MBT) during gastrulation. The detailed functional and molecular mechanisms of these members are discussed below.

2.1. Ventx1.1

Ventx1.1 is also known as Ventx1.1a, Ventx1.1b, and posterior-ventral 1 (PV.1a). It consists of 282 aa with a molecular weight of approximately 32 kDa. The protein acts as an endogenous neural repressor, reaching a peak during gastrulation and then diminishing during the neurulation stage of Xenopus embryos. Moreover, high levels of ventx1.1 expression have been reported in the ventral marginal zone and ectoderm in gastrulation stage embryos. A study demonstrated that BMP4/Smad1 signaling enhanced the expression of ventx1.1 while blocking BMP4 signaling via a constitutively inactive, truncated form of BMP4 receptor I (DN-BR/tBR) that eliminated ventx1.1 expression in uncommitted ectodermal explants of Xenopus embryos [71]. The ectopic expression of Ventx1.1 inhibits the ectoderm-to-neuroectodermal transition in intact embryos, leading to the inhibition of primary neurogenesis. Studies have shown that an elevated level of Ventx1.1 has led to embryonic ventralization and partially counteracted the effects of the dorsalizing agent lithium chloride (LiCl), a GSK3β inhibitor. It also counteracted the neurulation activity of Spemann-organizer-specific factors, including chordin, noggin, gsc, and activin, in Xenopus embryos [30,71], all of which led to the formation of the central nervous system. It is the C-terminal of Ventx1.1 that represses the dorsal and Spemann-organizer-specific genes in Xenopus, which results in a headless phenotype when ectopically expressed [33,72]. Moreover, the inhibition of Ventx1.1 by the engrailed–fused N-terminal region of Ventx1.1 (N-PV.1-EnR) in the ventral marginal zone (VMZ) induced a partial secondary axis. The inhibition of Ventx1.1 activity by an antimorphic form of Ventx1.1 (N-Ventx1.1-EnR) in VMZ triggered the expression of dorsal-specific genes, promoting secondary head formation.
A study showed that embryonic FGF (eFGF) inhibited BMP4-induced erythropoiesis in a Ventx1.1-dependent manner in the VMZ of Xenopus embryos [42]. eFGF/Ventx1.1 reduced the BMP4-induced erythropoietic markers, namely, gata2 and α-globin, to inhibit erythropoiesis in Xenopus gastrulae. A recent study indicated that FGF signaling controlled the dorso–ventral mesodermal transition in Xenopus embryos [35]. In DMZ, the blocking of FGF signaling by the constitutively inactive form of FGF receptor (DNFR) or DN-Ras led the conversion of DMZ to VMZ in Xenopus laevis. Moreover, the inhibition of FGF signaling recovered the activin-reduced expression of ventral mesodermal markers in DMZ, including ventx1.1, gata2, and α-globin. Furthermore, FGF inhibition in DMZ induced ventx1.1 expression to eliminate the expression of the organizer and dorsal-mesodermal-specific markers, including chordin and noggin, in the gastrulae [73,74,75]. These studies have suggested that Ventx1.1 is involved in ventral mesodermal formation and hematopoiesis in Xenopus. The ectopic expression of Ventx1.1 directly attenuated the mRNA levels and promoter activity of neuroectodermal specifiers, specifically zic3 and foxd4l1.1, in Xenopus laevis embryos [76,77]. Ventx1.1 interacted within the promoter regions of neural and dorsal genes, such as zic3, foxd4l1.1, and noggin, in Xenopus. This reduction resulted in inhibiting the primary neurogenesis in Xenopus gastrulae. A recent study demonstrated that BMP4/Smad1 and FGF/Xbra cooperated synergistically to activate ventx1.1 transcription, which led to the VMZ formation in Xenopus embryos [13]. BMP4/BMPR-I/II leads to the Smad1 (pS463/465) phosphorylation to catalyze the interaction of Smad1 with Xbra. This complex directly binds with the ventx1.1-promoter region and activates ventx1.1 transcription in the VMZ. Furthermore, Smad1/Xbra-induced Ventx1.1 suppresses the DNBR-induced expression of early and late neural-specific markers, such as foxd4l1.1, ncam, ngnr, and otx2, consequently resulting in neural inhibition in the uncommitted explants of Xenopus embryos. A recent study documented that FoxD4l1.1 inhibited ventx1.1 transcription directly as well as indirectly in the neuroectodermal region of Xenopus gastrulae. FoxD4l1.1 directly bonded within the proximal-promoter region of ventx1.1 in Xenopus embryos. Apart from the direct inhibition of ventx1.1 transcription, the ectopic expression of FoxD4l1.1 repressed Smad1/Xbra-induced synergistic transcription activation of ventx1.1 in Xenopus. Additionally, FoxD4l1.1 physically interacted with Xbra and diminished the Xbra-binding within the 5′-upstream-promoter region to inhibit ventx1.1 transcription. FoxD4l1.1 also reduced C-terminal phosphorylation of Smad1 to arrest nuclear localization of Smad1, which then repressed Smad1-induced ventx1.1 transcription and led to neuroectodermal formation in Xenopus gastrulae [78,79]. A study reported that an elevated level of Ventx1.1 also repressed VMZ markers, including ventx1.1, ventx1.2, and ventx2.1, without affecting the bmp4 expression during gastrulation in Xenopus embryos [80]. Moreover, Ventx1.1 reduced the xcad2-induced (a transcriptional activator of ventral signaling [81]) expression of ventral mesoderm-specific markers in animal-cap explants. Ventx1.1 directly bonded within its own promoter region and negatively regulated its own transcription in gastrulae. Interestingly, Ventx1.1 and Xcad2 share the same cis-acting Ventx1.1-binding-response elements (VRE) to regulate VMZ-specific genes in an opposite manner. Ventx1.1 attenuated ventral mesodermal markers while Xcad2 promoted the expression of these markers in animal-cap explants [80]. The concomitant expression of Ventx1.1 and Xcad2 competed and reduced the direct binding of Xcad2 within the 5′-upstream regions of ventx1.1 to inhibit the Xcad2-induced expression of the Ventx family genes, including ventx1.1. The Ventx1.1-mediated inhibition of its own expression in a recurrent inhibitory loop suggests that Ventx1.1 controls its own concentration in the ventral mesoderm and the ectoderm in order to guide the orderly dorsoventral patterning during development. These studies have shown that Ventx1.1 is critical in axial patterning, hematopoiesis, and VMZ formation in Xenopus.

2.2. Ventx1.2/Xvent1

Ventx1.2 is also known as Vent1 in Xenopus. Ventx1.2, composed of 264 aa and containing a 60-aa-long DNA-binding domain (DBD) called homeobox, binds within the 5′-updtream region of its targets. The molecular weight of Ventx1.2 is approximately 30 kDa (Figure 3A). Being similar to ventx1.1, Ventx1.2 is also a homeobox transcription factor and an endogenous neural repressor. BMP4/Smad1 also led to the expression of ventx1.2, which was differentially expressed in the ventral mesodermal zone, ectoderm, and VBIs of Xenopus [46,82]. Ventx1.2 supressed dorsal-lip-specific and Spemann-organizer-specific genes, including xfd-1 (a neural specifier and anterior–posterior neural-patterning marker) and gsc, inhibiting head formation and embryonic ventralization [43]. This inhibition was caused by the direct binding of Ventx1.2 within the 5′-upstream region of xfd-1 and the blocking of xfd-1 transcription in Xenopus embryos. Moreover, the inhibition of Ventx1.2 has promoted the transcription of xfd-1 to trigger neural induction in uncommitted explants of Xenopus embryos.
A recent study indicated that the loss of ventx1.2 in VMZ resulted in a partial secondary axial induction and embryonic dorsalization [47]. Moreover, the loss of Ventx1.2 enhanced the expression of anterior neural specifiers, including xag1 (cement gland marker), en-2 (anterior marker), and ncam (pan-neural marker) in uncommitted animal-cap explants. Interestingly, an elevated level of Ventx1.2 also induced stem-cell-leukemia (scl) expression in uncommitted explants of Xenopus gastrulae. Scl is a hematopoiesis marker that synergistically triggers the hematopoietic cell differentiation with GATA1 and LMO2 (yolk-sac-erythropoiesis marker) in Xenopus [82]. In summary, Ventx1.2 may actively participate in hematopoiesis, cell fate determination, and embryonic ventralization in Xenopus.

2.3. Ventx2.1

Other names for Ventx2.1 include Vox, Xvent2, and Ventx2.1a/b. Ventx2.1 is the longest member of the Ventx transcriptional repressor family at 336 aa in length, and it has a molecular weight of approximately 38 kDa (Figure 3A). Ventx2.1 contains three distinct domains: the N-terminal transactivation domain (TAD), the DNA-binding homeobox domain (DBD), and the C-terminal repressor domain (RD). The expression of Ventx2.1 is primarily reported during blastulation after the mid-blastula transition (MBT) and leads to the development of the ventral mesodermal and ectodermal regions of Xenopus embryos. Studies have reported that BMP4/Smad1 directly induced the expression of ventx2.1 in VMZ and ectoderm in Xenopus laevis [24,82]. The TAD of Ventx2.1 activates the transcription of ventral and ectodermal specifiers, namely, ventx1.1, bmp4, and itself, in a positive feedback loop during the embryonic development of Xenopus embryos [14,24,25]. Additionally, Ventx2.1 directly binds to the 5′-upstream regions of bmp4 and ventx1.1 and activates their transcription in embryos’ gastrulae, leading to embryonic ventralization.
Studies have reported that a morpholino-based knockdown of ventx2.1 caused a partial secondary axis and expanded the Spemann-organizer region in Xenopus embryos [24,47,83]. The knockdown of ventx2.1 in the VMZ region induced the expression of Spemann-organizer specifiers, including noggin, chordin, and gsc, in Xenopus embryos. Moreover, FGF/Xbra also bonded within the 5′-upstream regions of ventx2.1 in Xenopus gastrulae. The FGF/Xbra pathway positively induced ventx2.1 transcription to trigger ventral mesodermal and ectodermal formation in Xenopus [13]. A study has also reported that the physical interaction of Ventx2.1 and GATA2 induced the expression of bmp4 in an auto-positive feedback loop to augment ventx1.2 expression, which led to embryonic ventralization and ventral mesodermal formation in Xenopus embryos [22]. Lee et al. (2011) showed that Ventx2.1 alone could activate ventx1.1 transcription after the direct binding of Ventx2.1 within the 5′-upstream regions of ventx1.1 during gastrulation in Xenopus [14]. The RD of Ventx2.1 formed a complex with the MH1 domain of Smad1 in VMZ to synergistically activate ventx2.1 transcription. This activation was synergized in a positive feedback loop, which led to embryonic ventralization and mesodermal formation [12]. Recently, it was documented that the concomitant expression of Ventx2.1 and Ventx1.2 repressed the expression of early neuroectodermal progenitor markers, including sox3, sox2, geminin, in Xenopus embryos [84]. This repression might be caused by the repressor domains (RDs) of Ventx2.1 and Ventx1.2 in Xenopus, inhibiting the head and neural formation. It has been shown that activin could induce the expression of ventx2.1 in uncommitted explants [85]. However, the function of the activin-mediated induction of ventx2.1 was unknown until recently. Ventx2.1 promoted BMP4 signaling in a positive feedback loop to support dorsoventral axial patterning and germ-layer specification.

2.4. Ventx2.2/Xom/Xbr-1

Ventx2.2 is also known as Xvent-2 and Xom-A. The structural details of Ventx2.2 are available in Figure 3A. Being similar to Ventx2.1, Ventx2.2 comprises three domains: the N-terminal transactivation domain, the middle DNA-binding domain (DBD), and the C-terminal repressor domain. BMP4/Smad1 has also induced ventx2.2 expression in the VMZ and the ectodermal region of Xenopus laevis [26]. The ectopic expression of Ventx2.2 promoted embryonic ventralization by directly inhibiting the expression of gsc (gsc is an endogenous transcriptional inhibitor of ventral-specific genes). Ventx2.2 physically interacted within the 5′-upstream regions of gsc, leading to the transcriptional inhibition of gsc in Xenopus embryos. A previous study showed that Ventx2.2 had been phosphorylated in a GSK3β-like domain (DpSGYEpS) and was degraded in a GSK3β-independent manner in Xenopus gastrulae [86]. The phosphorylated Ventx2.2 interacted with E3 ubiquitin ligase, SCF-βTrCP, to degrade Ventx2.2 during early gastrulation in Xenopus embryos.
Moreover, the dorsal injection of a phospho-dead mutant of Ventx2.2 (i.e., Xom-2SA) repressed the dorsally expressed genes effectively during the gastrulation of Xenopus embryos. This repression of dorsal genes then led to ventralization and a headless phenotype. A recent study has reported that the N-terminal (TAD) of Ventx2.2 interacted with LEF1/TCFs, a high mobility group box-containing transcription factor, and transactivated the LEF1/TCFs-mediated transcription of ventrally expressed genes in Xenopus embryos [87]. In addition, the N-terminal-deleted Ventx2.2 failed to induce the TAD-mediated transactivation of ventral-specific genes, while retaining its repressor activity to suppress gsc transcription in Xenopus animal-cap explants. Additionally, the TAD-lacking Ventx2.2 failed to activate bmp4 expression and resulted in an apoptosis-like response in Xenopus embryos [88,89]. Another recent study showed that Ventx2.2 balanced the concentrations of β-cat and GSK3β in the dorsal and ventral regions, respectively, leading to dorsoventral axial patterning during the embryonic development of Xenopus [90]. Ventx2.2 triggered the β-cat proteolysis in a GSK3β-dependent manner in the ventral region. Ventx2.2 induced gsk3β expression while GSK3β catalyzed the phosphorylation and degradation of β-cat in the VMZ to initiate the orderly patterning of the dorsoventral axis during embryonic development. These studies indicated that Ventx2.2 acts as a vital player during dorsoventral axial patterning and neural crest differentiation in Xenopus.

2.5. Ventx2.2 Maintains Cellular Pluripotency in Xenopus Similarly to Nanog in Other Animals

Xenopus lacks the Nanog gene, a pluripotent and proliferative marker in humans, mice, and zebrafish [91]. Nanog is a homeobox transcription factor and is expressed in mammalian pluripotent cells and developing germ cells. Nanog expression is considered as a hallmark of pluripotency in vivo as well as in vitro [92]. The deletion of Nanog in mammalian cells causes embryonic lethality. The constitutive expression of Nanog has resulted in the self-renewal of embryonic stem cells (ESCs) and sustained their uncommitted state [92]. Additionally, Nanog-null cells showed multi-lineage differentiation both in fetal and adult mice. Multiple lines of evidence have suggested that Ventx2.2 may play a similar role to Nanog in the development of Xenopus. The sequence homologies between Ventx2.2 and Nanog within the BarH subclass of the NKL family indicated that they may have descended from the same ancestor. Both Ventx2.2 and Nanog contain the BarH-specific threonine (Thr) residue and the conserved serine (Ser) residue outside the HD, which are absent in all other BarH-subclass proteins. In addition, the temporal expressions of Xenopus ventx2.2 and zebrafish Nanog (zNanog) are very similar, and overexpression of either results in the same phenotype [91]. Furthermore, both Ventx2.2 and Nanog dimerized, directly interacted with Oct25, and inhibited the expression of dorsalizing factors gsc and chordin in zebrafish. Ventx2.2 not only led to ventral mesodermal differentiation and embryonic ventralization but also determined the pluripotency in embryonic cells, such as those in animal caps. A recent study proposed that Ventx2.2 acts as a Nanog ortholog to maintain cellular pluripotency in Xenopus [48]. In Xenopus, the overexpression of murine Nanog (mNanog) has led to dorsal mesodermal formation by suppressing the effect of BMP4 in uncommitted ectodermal cells [85]. In addition, overexpressed mNanog induced the expression of chordin and gsc (endogenous inhibitors of BMP4 signaling), causing a secondary axis in Xenopus. mNanog inhibited the expression of Ventx2.2 (a positive regulator of BMP4 signaling), suppressed BMP4 signaling, and retained the expression of dorsal-specific markers, including chordin, Xnot, and gsc, to trigger dorsal mesodermal formation in the uncommitted ectoderm of Xenopus embryos [85]. A recent study showed that the antisense-morpholino-based combined inactivation of Ventx1 and Ventx2 (Ventx1/2) reduced the expression of the multipotency marker oct91 and premature differentiation in Xenopus blastulae [48]. The expression of oct91 is required to maintain the pluripotency and premature cell differentiation during Xenopus blastulae. The concomitant overexpression of Ventx1/2 obstructed the lineage commitment of a dorsoventral fate; and the overexpression of Ventx1/2 and mNanog reduced the expression of germ cell specification, separately, in a similar manner [48]. A knockdown of Ventx1/2 repressed pluripotency markers and led to premature cell commitments during blastulae [48,49]. Ventx1/2 notably reduced the expression levels of organizer-specific genes, including gsc, hhex, and Xnot, to inhibit the dorsal mesodermal differentiation in animal-cap explants, similarly to mNanog. In addition, similarly to the dorsal mesoderm, the concomitant expression of Ventx1/2 mRNA also suppressed the expression of the ventral mesodermal (bmp4) and early ectodermal markers (lim5 and foxi1a). Conversely, Ventx1/2 and mNanog significantly reduced the expression of genes involved in epidermis (tfap2a), axial (xbra), and paraxial mesodermal (myf5) in Xenopus. These results indicate that Ventx1/2 inhibits the dorsoventral fate commitment in Xenopus, similar to mNanog. Strikingly, the ectopic expression of mNanog mediated the Ventx1/2 deficiency in Xenopus embryos, leading to embryonic dorsalization. These studies showed that Ventx1/2 acted as a Nanog ortholog in Xenopus by maintaining pluripotency in Xenopus blastulae to delay the multiple-cell lineage commitment and differentiation, and inhibited the onset of dorsoventral axial patterning in Xenopus [48]. Recently, a study indicated that MEK1 (Map2k1), an upstream kinase of the MAPK family, phosphorylated Ventx2.2 in the PEST-like destruction motif (a region rich in proline (Pro), glutamate (Glu), Serine (Ser), and threonine (Thr)) and destabilized Ventx2.2, leading to uneven dorsoventral gradients of Ventx2.2 during the embryonic development of Xenopus [49]. By destabilizing Ventx2.2, MEK1 promoted multiple-cell lineage commitments and differentiation to initiate gastrulation in Xenopus embryos. An elevated level of Ventx2.2 blocked neuroectodermal differentiation and promoted the inhibition of neural progenitor markers, including sox2 and sox3, in Xenopus embryos [84]. A recent study demonstrated that the ectopic expression of Ventx2.2 regulated the reprogramming of uncommitted ectoderm towards an early neural-crest cell identity in Xenopus, leading to ectomesenchyme differentiation [93]. Ventx2.2 helped to maintain a population of multipotent progenitor cells in the pre-existing sensory neurons and pigment neural borders and led to skeletogenic neural-crest formation. Ventx2.2 also induced the expression of neural-crest specifiers at the neural plate border (foxd3, twist1, snail1/2, and soxE, a pan-vertebrate neural crest marker) and stem-cell marker (pou5f3.1/oct4), along with other reprogramming-associated genes (chd7, tert, tet3, kdm4a, and smarc4a) in Xenopus embryos. Additionally, the morpholino-based knockdown of ventx2.2 reduced the expression of neural-crest- and multipotency-specific markers and caused severe defects in the cranial neural crest (CNC) and ectomesenchyme formation in Xenopus. In summary, Ventx2.2 has the potential to regulate multiple steps of the neural-crest-gene regulatory network in Xenopus.

2.6. Ventx2.2 Leads to Ectomesenchyme Proliferation and Mandibular Cartilage Development in Xenopus as Barx1 Does in Rodents and Fruit Flies

As we have discussed above, Ventx synteny was absent in rodents and the fruit fly, D. melanogaster. The genes closely related to Ventx2.2 in mice (BarH1 and BarX1) and Drosophila (BarH1) belong to the Bar family of the homeobox. Both the Ventx and the Bar families share a rare amino acid substitution (Thr instead of Val/Ile) at position 47 of the third helix of the HD. In Xenopus, Ladher et al. (1996) and Papalopulu et al. (1996) independently isolated ventx2.2 and named it “Xom” for its similarity to the Om(1D) Drosophila annasae homologue of D. melanogaster BarH1 and Xenopus Bar-related (Xbr-1) [27,28]. Xom and Xbr-1 share similarities in sequence (approximately 55%) and expression patterns to the HD of Drosophila BarH1/Om(1D). Similarly to Ventx2.2, BarX1 promoted ectomesenchyme development and neural-crest cell migration, leading to craniofacial skeleton formation in vertebrates. As we discussed above, Ventx2.2 is also involved in neural-crest cell migration and ectomesenchyme formation [93]. Neural-crest cells originate from four major parts of the neural axis: cranial, cardiac, Vagal, and trunk [94]. These cells further differentiate into various types of cells, including neurons, connective tissue cells, myocytes, enteric ganglia, melanocytes, sympathetic ganglia, etc. Studies have shown that Barx1 was expressed in pharyngeal dentition and required for tooth development in mice and zebrafish [95,96,97]. A recent study demonstrated that Barx1 led to tooth and musculoskeletal attachment but not tooth initiation and morphogenesis in zebrafish [97]. In Barx1 mutants, the intermandibular muscles were disorganized, failed to attach to Meckel’s cartilage, and invaded the cartilage gaps instead (Meckel’s cartilage gap is a hallmark of jaw-joint identity). In addition, sternohyal muscles were shorter, and hyohyal muscles were reversed in their orientation. These muscles were specified clearly but failed to attach to their skeletal scaffolds, resulting in craniofacial defects. The repression of Barx1 at the mandibular arch is required for the development of the mandibular moveable joint, and its overexpression is needed for chondrocyte differentiation to form cartilage and support the craniofacial skeletal’s formation. BMP4 induced the expression of barx1 in the pharyngeal arch region of zebrafish and led to chondrocyte differentiation and condensation [98]. The loss of Barx1 resulted in the inhibition of chondrocyte differentiation and a reduction in the odontogenic marker, dlx2b, which is needed for chondrogenesis in zebrafish. In addition, the loss of Barx1 regulated jaw-joint patterning by inducing gdf5 (a joint and cartilage marker) and chordin (a jaw-joint-patterning marker) expression, promoting the development of the craniofacial skeleton. These studies indicated that Barx1 is a downstream target of BMP4 signaling, like Ventx2.2, and plays a role in neural-crest cell migration and ectomesenchyme proliferation in zebrafish.
Ventx2.2/Xom is also known as a canonical Wnt/β-cat inhibitor in human and Xenopus [87,99]. Ventx2.2/Xom physically interacted with LEF/TCF and blocked its interaction with β-cat, promoting ventral gene expression in Xenopus. LEF/TCF and Ventx2.2/Xom diminished the β-cat level in cells and inhibited the dorsalizing effect of Wnt/β-cat during embryonic development. Similarly, Barx1 inhibited Wnt signaling in a sFRP1/2-dependent (a secreted-Wnt antagonist) manner in mice [100]. Wnt/β-cat led to gastric endodermal differentiation instead of epithelial differentiation. The Barx-1-mediated inhibition of Wnt/β-cat promoted stomach-specific epithelial differentiation and suppressed endodermal differentiation in mice. A recent study showed that the loss of Barx1 caused defects in the positioning and expansion of the spleen (a mesothelium-lining-originated organ) in a WT1-dependent manner [101]. The loss of Barx1 in mice reduced the expression of WT1 (a mesothelium marker that is important in spleen morphogenesis). Therefore, Barx1 is critical for spleen development and its positioning during gastrointestinal organogenesis. In conclusion, both Ventx2.2 and Barx1 are highly involved in neural-crest migration, ectomesenchyme and chondrocyte differentiation, and organogenesis.

2.7. Ventx3.1

Ventx3.1 is also known as Vent-3 and consists of 261 aa with a molecular weight of approximately 30 kDa (Figure 3A). The functions of Ventx3.1 have not yet been studied in Xenopus laevis.

2.8. Ventx3.2/Vex1

Ventx3.2, also known as Vex-1, is one of least studied members of the Ventx family in Xenopus. Ventx3.2 is composed of 285 aa and its molecular weight is approximately 32 kDa (Figure 3A). Ventx3.2 is one of the direct downstream targets of BMP4/Smad1 signaling [37,102]. It is expressed in VMZ and the ectodermal region throughout gastrulation.
Overexpressed Ventx3.2 led to embryonic ventralization in a dose-dependent manner and remedied the effect of DNBR-inhibited BMP4 in Xenopus embryos [102]. Moreover, the overexpression of Ventx3.2 directly inhibited the expression of dorsal- and anterior-specific neural genes, including gsc and otx2, in animal-cap explants. Antisense RNA and the morpholino-mediated inhibition of ventx3.2 in VMZ resulted in embryo dorsalization and secondary axial formation by enhancing the expression of gsc and chordin in the VMZ of Xenopus. These studies indicated that Ventx3.2 functioned similarly to most other Ventx family members and promoted ventral mesodermal formation and neural inhibition in Xenopus laevis. The Ventx family signaling crosstalks that are regulated by BMP4/Smad1, FGF/Xbra, and activin are summarized in Figure 4.

3. Vega Family in Zebrafish

The Vega family in zebrafish is also known as the Vent family. It is the equivalent to the Ventx family in Xenopus laevis, as they have identical physiological roles. The Vega family synteny in zebrafish are located on two different chromosomes: Vega1 and Vega2 on chromosome 13; and Ved on chromosome 10 (Table 3). The evolutionary phylogenetic tree of the Vega/Ventx family cluster in zebrafish indicates that Vega1 and Vega2 descended from a common ancestor and that Ved was once a member of the Vega family (Figure 3C,C’). During evolution, Ved might have shifted to chromosome 13, since Vega1/2 and Ved follow the root of common ancestors in zebrafish. Similarl7 to the Ventx family in Xenopus, BMP4/Smad1/5 signaling upregulated Vega family expression in zebrafish, leading to dorsoventral axial patterning and VMZ formation [21]. The functions of the Vega family in zebrafish are described below.

3.1. Vega1/Vox

Vega1 is one of the first identified members of the Vega family in zebrafish. Vega1 consists of 242 aa, including a 66-aa-long C-terminal repressor domain, and its molecular weight is approximately 28 kDa (Figure 3A). The transcription of vega1 is activated in the mid-blastula transition (MBT) during blastulation, and it is downregulated dorsally before gastrulation onset. The expression of vega1 has been reported in the VMZ region, and elevated levels have been shown to inhibit the expression of a dorsal-specific gene named bozozok/dharma (boz/dha), which is required for organizer formation and embryo dorsalization), chordin (dino), and gsc genes in zebrafish [34,44]. The reduced levels of dorsal-specific genes caused a headless phenotype and organizer-expansion inhibition, similarly to Ventx1.1 in Xenopus. Additionally, the dominant-negative mutant of Vega1 mitigated the effects of gsc and boz/dha in VMZ and led to embryonic dorsalization and secondary axial formation in zebrafish. Therefore, Vega1 is required for dorsoventral axial patterning in zebrafish.

3.2. Vega2/Vent1/Vent

Vega2 is also known as a ventral-expressed homeobox (Figure 3A). The transcription of vega2 is found in the VMZ during blastulation, and it is downregulated dorsally, similarly to Vega1. The expression of vega2 partially overlapped with a dorsal-specific gene, gsc, in zebrafish embryos. Similarly to the Ventx family members, the expression of vega2 was also positively regulated by BMP4/Smad1 signaling in the VMZ region of zebrafish embryos. Overexpressing Vega2 in DMZ inhibited gsc and caused a headless phenotype during the embryonic development of zebrafish. The interaction of Vega2 and Vega1 synergistically inhibited the transcription of gsc, causing ventralization and VMZ formation in zebrafish [44,45]. Additionally, the dominant-negative mutant of Vega2 induced gsc expression in VMZ and resulted in embryonic dorsalization in zebrafish. Vega2 thus supported dorsoventral axial patterning and germ-layer specification in zebrafish. These studies also suggested that vega1 and Vega2 could possibly act as negative regulators for organizer expansion and head formation in zebrafish.

3.3. Ved

Unlike Vega1 and Vega2, Ved is located on chromosome 10 in zebrafish (Table 3). Ved is the longest member of the Vega family, being 278 aa in length, and it has a molecular weight of approximately 31 kDa (Figure 3A). Ved is also a transcription repressor, and it expresses ventrally in zebrafish. Ved has been reported as a direct target of Boz/Dha in zebrafish. A recent study has shown that BMP4 signaling ventrally controlled the expression of Ved, and the dorsal, combined inhibition of dino and gsc induced the expression of ved in the DMZ of zebrafish embryos, leading to embryonic ventralization, a shortened anterior structure, and a headless phenotype [103]. A study showed that the combined morpholino-based knockdown of ved, vega1, and vega2 in zebrafish embryos enhanced the expression of boz/dha, gsc, and dino, resulting in an organizer-center expansion [38].
These studies collectively indicated that the Vega family works as one of the downstream targets of BMP4 signaling and triggers embryonic ventralization and VMZ formation. Furthermore, the inhibition of the Vega family resulted in the organizer-region expansion and embryonic dorsalization. Taken together, the studies indicated that the entire Vega family plays an essential role in the dorsoventral axial patterning of zebrafish embryos. The functions of the Vega family are summarized in Figure 4.

4. Human Ventx (VENT-like Homeobox Protein 2)

Ventx might be the only reported active member of the Ventx family in humans (Figure 3A). It is also known as VENTX2 and HPX42B. Human Ventx showed 39%–67.66% similarity to Ventx family members in Xenopus and zebrafish (Table 3) [17]. The ectopic expression of human Ventx in zebrafish embryos caused the loss of the anterior structure, resulting in the failure of notochord formation. In addition, overexpressed Ventx also leads to embryonic ventralization in Xenopus and zebrafish. Similarly to the Ventx family in Xenopus and zebrafish, the expression of human Ventx was also led by BMP4 signaling [108]. Human Ventx works downstream of BMP4/Smad1 signaling and causes embryonic ventralization in Xenopus and zebrafish. A study reported that Ventx was aberrantly expressed in CD34+ acute myeloid leukemia (AML), and its maximum expression was found in CD33+ myeloid cells but not in normal CD34+/CD38 leukemic cells [18]. In addition, the abnormal expression of Ventx in normal CD34+ cells could disturb the development of hematopoietic cells, leading to myeloid cell differentiation rather than lymphoid generation, both in vivo and in vitro. The shRNA-mediated knockdown of Ventx resulted in the failure of AML cell proliferation [18]. These studies indicated that Ventx may play a vital role in postnatal hematopoiesis and malignant myelopoiesis.
Ventx led to macrophage differentiation, depending on the cytokines involved, such as CSFs and IL-3. The inhibition of Ventx in primary monocytes suppressed monocyte-to-macrophage differentiation, suggesting that Ventx plays a significant role in macrophage differentiation and the ensuing activation of cytokines [51]. A recent study has shown that Ventx was dramatically reduced in tumor-associated macrophages (TAMs), which are critical components of the tumor microenvironment (TME). The suppression of the immune system in TME was one of the key hurdles in developing effective immunotherapies to treat tumors [109]. In addition, Ventx potentiated the cell growth and terminal differentiation of hematopoietic and immune cells in isolated samples of cancer patients. Moreover, Ventx regulated TAM plasticity, resulting in the M1-like phenotype of TAMs. Ventx suppressed the immune system in the TME, inhibited regulatory T-cell (Treg) differentiation, and promoted CD8 tumor-infiltrating lymphocytes [109]. In addition, Ventx modulated TAM functions by inhibiting the immune suppression of TAM plasticity in the TME during tumorigenesis in colon-cancer models. The involvement of Ventx in macrophage differentiation and the suppression of TAM plasticity in TME indicates that Ventx could be a novel agent for targeting tumorigenesis. Recently, Le et al. (2020) showed that the expression level of Ventx was notably decreased in the pancreatic ductal adenocarcinoma-(PDA)-associated macrophages (TAMs) collected from verified human patients [110]. The study showed that Ventx was necessary for regulating the phagocytosis, and the restored level of Ventx triggered phagocytosis by regulating the expression of Toll-like receptors 2/9, MyD88, and Mapk38 in PDA TAMs. Furthermore, the ectopic expression of Ventx inhibited the SHP1/2 phosphorylation level (the downstream molecules of SIRPa-CD47 signaling) to trigger phagocytosis. Ventx also induced phosphorylation focal adhesion kinase (FAK), leading to phagocytosis. Moreover, the elevated level of Ventx promoted the M1-like TAM phenotypes over M2-like TAM phenotypes to provide immunity against PDA by promoting the CD8 T-cell population over the Treg cell population in the PDA-associated tumor microenvironment. A study has shown that the M1/M2 and CD8/Treg ratio was associated with PDA prognosis [111], and the increased population of M1-like TAMs promoted immunity against pancreatic cancers. These findings indicate that Ventx could be a valuable candidate to improve PDA prognosis through the promotion of M1-like and CD8 populations and phagocytosis in PDA.
An elevated level of Ventx was reported in immature human hematopoietic cells. The knockdown of the Ventx expression significantly expanded the population of human stem cells and multipotent progenitor cells (HSC/MPP) and promoted the survival of HSC, ex vivo [112]. The suppression of Ventx in grafted HSC/MPP cells also increased the engraftment potential of HSC/MPP in NOD/SCID/IL2Rγ2null murine models. This suggested that Ventx could be a potent target for the application of HSC/MPP-based therapy. Recently, a study demonstrated that the expression of Ventx robustly increased in normal myeloid cells and in AML patients [32]. The overexpressed Ventx in myeloid cells reduced the expression of myeloid-terminal-differentiation-related genes in healthy CD34+ stem and progenitor cells. Moreover, the transplantation of retrovirally-engineered Ventx-expressed bone marrow progenitor cells increased the population of primitive erythroid cells to trigger acute erythroid leukemia in transplanted mice. Furthermore, the concomitant expression of AML1-ETO (AML1-ETO, a fusion product of the chromosomal translocation t(8;21)(q22;q22)) usually occurs in acute myeloid leukemia (AML) with granulocytic differentiation, FAB M2 subtype [113], and Ventx induced the expression of the erythroid markers, leading to AML in all transplanted mice. In addition, high levels of Ventx in human erythroleukemia patients significantly inhibited cell proliferation and tumor growth. However, Ventx acted as a tumor activator and triggered leukemogenesis, but some studies demonstrated its tumor-suppressant role in humans. A study reported its reduced expression in peripheral blood of chronic lymphocytic leukemia (CLL) cells and that it acted as a tumor suppressant [99]. Ventx interacted with LEF/TCFs and inhibited the canonical Wnt/β-cat signaling (a positive regulator of cell proliferation) in CLL cells. Ventx and LEF/TCF interaction abrogates β-cat and LEF/TCFs complex formation and suppresss the proliferation-marker cyclin D1’s expression in CLL cells. Ventx-LEF/TCF interaction reduced the LEF/TCF-targeted oncogene, cyclin D1, to inhibit cyclin D1-mediated cell proliferation. The reduced level of Ventx in CLL cells promoted Wnt/β-cat and LEF/TCFs interaction, and in turn, induced cyclin D1 expression, leading to cell proliferation and cancer progression. Recently, it was reported that the differential methylation level of Ventx was significantly implicated in sarcoma progression in humans [114]. A genome-wide methylation-profiling study in metastatic and recurrent sarcomas showed that Ventx was hypermethylated in metastasis pleomorphic rhabdomyosarcoma (Ple-RMS, a rare, aggressive sarcoma with poor prognosis), as compared to primary Ple-RMS. This study hypothesized that due to its involvement in tumor microenvironment and acting as an Wnt antagonist, Ventx may have strong therapeutic potential for sarcomas associated with immune cell content. A study showed that Ventx might also act as a negative regulator of tumor progression. Ventx activated both p16ink4a-Rb and p53–p21 tumor-suppression pathways [54]. Overexpressing Ventx led to a cell-senescence-like phenotype, followed by an irreversible cell-cycle arrest. Strikingly, the RNAi-mediated inhibition of Ventx enhanced cell senescence and ameliorated the camptothecin (CPT) resistance in lymphocytic leukemia cells. Ventx-associated chemotherapeutic resistance and its involvement in the cell-senescence process suggested that Ventx could be a novel, potential target for cancer prevention. A recent study confirmed the anticancer role of Ventx and showed that Ventx triggered apoptosis in a p53-independent manner in cancer cells (HCT116 p53KO) but not in healthy cells, in vitro [115]. In addition, Ventx activated the executioner caspase-3 in p53−/− knockout cells, leading to the suppression of tumor growth.
Furthermore, the treatment of doxorubicin increased the level of Ventx in both p53 (WT) and p53−/− knockout cells. Ventx’s involvement in hematopoiesis, leukemogenesis, cell senescence, and macrophage differentiation is illustrated in Figure 4. These studies suggested a tumor-suppressant function of Ventx in both p53+/+ and p53−/− cells, and Ventx might be a novel therapeutic target for certain human cancers, working in a p53-independent manner. In summary, Ventx is deeply involved in hematopoiesis and leukemogenesis in humans, and it could be a future therapeutic target for combating tumorigenesis.

Nanog (Ventx-like) Is Considered an Oncogene in Humans

Nanog is a well-established stem-cell pluripotent marker and homeobox transcription factor which creates stem-cell-like properties in cancer cells [92]. Earlier, we discussed the functional and homologic similarities between Ventx2.2 and Nanog and their roles in maintaining cell pluripotency and inhibiting differentiation. Cancer stem cells (CSCs) and normal stem cells can self-differentiate and self-renew. CSCs are immortal in nature, persistent in tumors, and provide nourishment for tumor maintenance, metastasize, and relapses [116]. Similarly to Ventx, aberrant expression of Nanog was detected in a small subset of AML patients and an AML cell line, Namo-1 (serves as a model for AML) [117]. Loss and gain of function studies have shown that Ventx, KLF4, Myb, and anti-apoptosis-factor MIR17HG are Nanog-targeted genes [116]. These factors are widely involved in generating oncogenic properties and leading to leukemogenesis in humans. Nanog inhibited p53 in a Gli-MDM2-dependent manner in glioma tumors [118,119]. Nanog induced the expression of Gli1/2 (glioma-associated oncogenes) that is required for MDM2 activation, and inhibited p53 activity. The tumor suppressant p53 directly reduced the promoter activity of Nanog (p53 is a direct inhibitor of Nanog). Nanog and p53 mutually inhibit each other expression in glioma tumors (for a review, see Grubelnik et al., 2020). However, p53 promoted Notch1 expression in early-stage oral squamous cell carcinoma. Notch1 is a positive regulator of Nanog [120]. The Nanog-mediated inhibition of p53 indicated that Nanog was involved in cancer cell proliferation and tumor development in humans. Additionally, the p53-mediated inhibition of Nanog suggested that Nanog had oncogenic abilities and may promote the stem-cell-like nature of cancer cells, leading to cancer self-differentiation and self-renewal [116,120]. Meanwhile, the p53-mediated activation of Nanog in a Notch1-dependent manner indicated the importance of Nanog during embryonic development.
Although, Ventx synteny is absent in rodent, but a recent study has been demonstrated that Nanog acts like a Ventx ortholog in rodents [121]. It showed that IGF2/IGF1R/Nanog signaling cascade regulates the proliferation of leukemia stem cells (LSCs) in mice. The overexpressed level of Nanog has been reported in CD34+ acute myeloid leukemia (AML) cells of patients and LSCs cells. Additionally, the knockdown of Nanog notably inhibits cell proliferation and induces cell cycle arrest and apoptosis. The si-mRNA-mediated silencing of Nanog suppresses the leukemogenesis of LSCs in mice. This report indicates that Nanog acts as a downstream target of IGF2/IGF1R signaling pathways that might positively regulate the Nanog transcription in LSCs. The overexpressed Nanog rescue colony formation ability of LSCs treated with IGF1R inhibitor (picropodophyllin). The knockdown of Nanog diminishes the colony formation ability of LSCs led by insulin-like growth factor 2 (IGF2) [121]. These findings suggested that IGF2/IGF1R/Nanog signaling cascade plays a critical role in regulating the LSCs proliferation while the overexpressed levels of Nanog trigger AML proliferation in mice and leukemogenesis in mice LSCs. This study supports that Nanog may be a possible candidate for leukemogenesis in rodents and might act like a Ventx ortholog.
These studies showed that Nanog and Ventx not only share functional similarities in maintaining cell pluripotency to delay cell-lineage commitments during embryonic development, but they are also similarly involved in cancer progression and leukemogenesis in humans.

5. Discussion and Conclusions

The Ventx and Vega families function downstream of BMP4/Smad1/5/8 signaling in vertebrates. BMP4/Smad1 upregulates the expression of Ventx and Vega families in the ventral regions of Xenopus and zebrafish embryos, respectively. The Ventx family is known for its transcriptional repressor activity, which drives the proper axial formation during embryonic development. The Ventx family not only inhibited dorsally expressed genes but also activated the transcription of ventral specific genes, leading to axial patterning and cell-fate determination in zebrafish and Xenopus [12,13,14,22,34,38,45,47,71,72,83,121]. Additionally, Ventx2.2 acted as a pluripotency regulator and maintained pluripotency in the VMZ. It could delay the blastula–gastrula transition during embryonic development of Xenopus [48,49]. Additionally, the inhibition of Ventx2.2 may trigger multiple cell-lineage commitments and gastrulation in Xenopus embryos.
In the Ventx family, the transactivation domain (TAD) of Ventx2.2 transactivated the Ventx genes, including ventx1.1 and ventx1.2, in a LEF1/TCF-dependent manner in Xenopus [14,22,24,87]. The ectopic expression of Ventx2.2 inhibited β-cat levels, causing the induction of gsk3β mRNA, leading to embryonic ventralization in Xenopus [105]. However, a study reported that Ventx2.2 was phosphorylated and degraded in a GSK3β-independent manner during gastrulation in Xenopus [86]. Ventx2.2 might be involved in GSK3b-mediated cranial neural-crest-cell (CNC) migration rather than β-cat-dependent CNC migration in Xenopus. In humans, Ventx boosted cell proliferation and hematopoietic cell-terminal differentiation, including myeloid cell differentiation [18,32]. Studies have shown that Ventx also participated in monocyte–macrophage cell differentiation [50,51]. Ventx modulated TAM plasticity in TME to suppress the immune actions and macrophage differentiation against tumorigenesis [109]. An elevated level of retrovirally-engineered Ventx caused erythroleukemia and expanded the abnormal primitive erythroid cells in bone marrow progenitor cells, leading to leukemic progression in transplanted mice [32]. On the contrary, recent studies have revealed that Ventx may also act as an anti-cancer agent [54,115]. Ventx triggers apoptosis in p53−/− knockout cell lines and activates cell senescence, which is followed by the activation of caspase-3, p53-p21, and p16ink4-Rb pathways. In p53−/− cells, doxorubicin augmented the Ventx level to trigger apoptosis in a caspase-3-dependent manner. Therefore, the Ventx family acts as a key player in dorsoventral axial patterning, pluripotency, cell-fate determination, hematopoiesis, apoptosis, and CNC migration. Additionally, the inhibition of Ventx family members suppresses cell proliferation and tumor growth in humans.

6. Future Prospective for Targeting the GATA2- and Ventx-Associated Cancers

A study has shown that Ventx2 interacted with GATA2 to promote the functions of ventx1.2 and bmp4 in Xenopus [22]. Moreover, Ventx family members were highly expressed in VBIs during the development of Xenopus embryos. The expression of GATA2 was also directly controlled by BMP4/Smad1 signaling and remained high in VBIs to induce differentiation of the hematopoietic mesoderm in Xenopus laevis [41,122,123]. Elevated levels of GATA2 were also reported in AML cell lines, patients’ samples, and tumors [124,125,126]. Cbfb-MYH11 is a chimeric product of core-binding-factor subunit-β (CBFB) and muscles myosin heavy chain 11 (MYH11). It was strongly associated with AML progression and triggered AML in humans. Elevated levels of GATA2 led to a poor prognosis and low survival in child AML, preleukemic Cbfb-MYH11 knock-in mice, and human inv(16) AML [124,125]. The RNAi- and K1717 (GATA2 inhibitor)-mediated inhibition of GATA2 notably diminished the expression of GATA2 targets—namely, Enah/Vasp-like AML markers, stem-like leukemia markers, and WT1 (Wilms tumor1, implicated in AML)—in KG1a cells and in clinical patients’ AML cells, triggering apoptosis. The heterozygous knockout of GATA2+/− in mice caused the inhibition of abnormal myeloid-progenitor-cell proliferation and differentiation and leukemia inhibition in Cbfb-MYH11 transgenic mice. Interestingly, transplanted leukemic cells drove leukemogenesis more aggressively in Cbfb-MYH11 and GATA2+/− mice, but not in normal mice. GATA2 inhibition minimized the mutation frequency of genes associated with leukemogenesis and delayed the onset of leukemogenesis in Cbfb-MYH11 knock-in mice. Collectively, the knockdown of GATA2 and Ventx attenuated cell proliferation and tumor growth, improved patient survival, and boosted the immunosuppression by drugs in tumor samples. Kumar et al. (2019) have reported that Ventx1.1 repressed the expression of ventx2.2 and ventx1.2 in a BMP4-independent manner in Xenopus embryos [80]. This inhibition was directly led by Ventx1.1 binding with the upstream region of ventx2.2, leading to ventx2.2 inhibition in Xenopus embryos (unpublished data). A previous study has reported that overexpressing Ventx1.1 suppressed GATA2 mRNA levels in the VMZ during hematopoiesis of Xenopus embryos [42]. A study demonstrated that Ventx1.1 interacted with Ventx2.2 during gastrulation of Xenopus embryos. However, the physiological outcome of this interaction remains unknown [127]. Since Ventx1.1 could interact with Ventx2.2 in Xenopus, it might be that the ectopic expression of Ventx1.1 inhibits the Ventx–GATA2 complex in humans and blocks GATA2- and Ventx2.1-induced leukemogenesis. Based on the collective evidence in Xenopus and humans, we concluded that Ventx1.1 may also inhibit the transcription of Ventx and GATA2, leading to the inhibition of human leukemogenesis. Xenopus Ventx1.1 could be a novel therapeutic pathway to target Ventx- and GATA2-associated cancers.

Author Contributions

Conceptualization, S.K. and W.L.; writing—original draft preparation, S.K.; writing—review and editing, S.K., W.L. and V.K.; supervision, S.K., W.L. and J.K.; project administration, J.K. and W.L.; funding acquisition, J.K. and W.L. All authors have read and agreed to the published version of the manuscript.

Funding

This study was supported by Biotechnology and Biological Sciences Research Council-BBSRC-UK (BB/T003146/1) and the Basic Science Research Program through the National Research Foundation of Korea (NRF), which is funded by the Ministry of Education, Science, and Technology of Korea (2016R1D1A1B02008770 and 2021M3H9A1097557).

Institutional Review Board Statement

Not applicable.

Informed Consent Statement

Not applicable.

Data Availability Statement

Not applicable.

Conflicts of Interest

The authors have no conflicting interest.

References

  1. Grainger, R.M. Xenopus tropicalis as a model organism for genetics and genomics: Past, present, and future. Methods Mol. Biol. 2012, 917, 3–15. [Google Scholar] [CrossRef] [PubMed]
  2. Blum, M.; Ott, T. Xenopus: An Undervalued Model Organism to Study and Model Human Genetic Disease. Cells Tissues Organs 2018, 205, 303–313. [Google Scholar] [CrossRef] [PubMed]
  3. Jia, Y.; Liu, X. Polyploidization and pseudogenization in allotetraploid frog Xenopus laevis promote the evolution of aquaporin family in higher vertebrates. BMC Genom. 2020, 21, 525. [Google Scholar] [CrossRef] [PubMed]
  4. Hellsten, U.; Khokha, M.K.; Grammer, T.C.; Harland, R.M.; Richardson, P.; Rokhsar, D.S. Accelerated gene evolution and subfunctionalization in the pseudotetraploid frog Xenopus laevis. BMC Biol. 2007, 5, 31. [Google Scholar] [CrossRef] [PubMed]
  5. Elurbe, D.M.; Paranjpe, S.S.; Georgiou, G.; van Kruijsbergen, I.; Bogdanovic, O.; Gibeaux, R.; Heald, R.; Lister, R.; Huynen, M.A.; van Heeringen, S.J.; et al. Regulatory remodeling in the allo-tetraploid frog Xenopus laevis. Genome Biol. 2017, 18, 198. [Google Scholar] [CrossRef]
  6. Session, A.M.; Uno, Y.; Kwon, T.; Chapman, J.A.; Toyoda, A.; Takahashi, S.; Fukui, A.; Hikosaka, A.; Suzuki, A.; Kondo, M.; et al. Genome evolution in the allotetraploid frog Xenopus laevis. Nature 2016, 538, 336–343. [Google Scholar] [CrossRef]
  7. Pollet, N.; Mazabraud, A. Insights from Xenopus genomes. Genome Dyn. 2006, 2, 138–153. [Google Scholar] [CrossRef]
  8. Gehring, W.J.; Affolter, M.; Burglin, T. Homeodomain proteins. Annu. Rev. Biochem. 1994, 63, 487–526. [Google Scholar] [CrossRef]
  9. Burglin, T.R.; Affolter, M. Homeodomain proteins: An update. Chromosoma 2016, 125, 497–521. [Google Scholar] [CrossRef]
  10. Burglin, T.R. Homeodomain subtypes and functional diversity. Subcell Biochem. 2011, 52, 95–122. [Google Scholar] [CrossRef]
  11. Holland, P.W.; Booth, H.A.; Bruford, E.A. Classification and nomenclature of all human homeobox genes. BMC Biol. 2007, 5, 47. [Google Scholar] [CrossRef] [PubMed]
  12. Henningfeld, K.A.; Friedle, H.; Rastegar, S.; Knochel, W. Autoregulation of Xvent-2B; direct interaction and functional cooperation of Xvent-2 and Smad1. J. Biol. Chem. 2002, 277, 2097–2103. [Google Scholar] [CrossRef] [PubMed]
  13. Kumar, S.; Umair, Z.; Yoon, J.; Lee, U.; Kim, S.C.; Park, J.B.; Lee, J.Y.; Kim, J. Xbra and Smad-1 cooperate to activate the transcription of neural repressor ventx1.1 in Xenopus embryos. Sci. Rep. 2018, 8, 11391. [Google Scholar] [CrossRef] [PubMed]
  14. Lee, H.S.; Lee, S.Y.; Lee, H.; Hwang, Y.S.; Cha, S.W.; Park, S.; Lee, J.Y.; Park, J.B.; Kim, S.; Park, M.J.; et al. Direct response elements of BMP within the PV.1A promoter are essential for its transcriptional regulation during early Xenopus development. PLoS ONE 2011, 6, e22621. [Google Scholar] [CrossRef] [PubMed]
  15. Lee, H.S.; Park, M.J.; Lee, S.Y.; Hwang, Y.S.; Lee, H.; Roh, D.H.; Kim, J.I.; Park, J.B.; Lee, J.Y.; Kung, H.F.; et al. Transcriptional regulation of Xbr-1a/Xvent-2 homeobox gene: Analysis of its promoter region. Biochem. Biophys. Res. Commun. 2002, 298, 815–823. [Google Scholar] [CrossRef]
  16. Faial, T.; Bernardo, A.S.; Mendjan, S.; Diamanti, E.; Ortmann, D.; Gentsch, G.E.; Mascetti, V.L.; Trotter, M.W.; Smith, J.C.; Pedersen, R.A. Brachyury and SMAD signalling collaboratively orchestrate distinct mesoderm and endoderm gene regulatory networks in differentiating human embryonic stem cells. Development 2015, 142, 2121–2135. [Google Scholar] [CrossRef]
  17. Moretti, P.A.; Davidson, A.J.; Baker, E.; Lilley, B.; Zon, L.I.; D’Andrea, R.J. Molecular cloning of a human Vent-like homeobox gene. Genomics 2001, 76, 21–29. [Google Scholar] [CrossRef]
  18. Rawat, V.P.; Arseni, N.; Ahmed, F.; Mulaw, M.A.; Thoene, S.; Heilmeier, B.; Sadlon, T.; D’Andrea, R.J.; Hiddemann, W.; Bohlander, S.K.; et al. The vent-like homeobox gene VENTX promotes human myeloid differentiation and is highly expressed in acute myeloid leukemia. Proc. Natl. Acad. Sci. USA 2010, 107, 16946–16951. [Google Scholar] [CrossRef]
  19. Genthe, J.R.; Min, J.; Farmer, D.M.; Shelat, A.A.; Grenet, J.A.; Lin, W.; Finkelstein, D.; Vrijens, K.; Chen, T.; Guy, R.K.; et al. Ventromorphins: A New Class of Small Molecule Activators of the Canonical BMP Signaling Pathway. ACS Chem. Biol. 2017, 12, 2436–2447. [Google Scholar] [CrossRef]
  20. Little, S.C.; Mullins, M.C. Extracellular modulation of BMP activity in patterning the dorsoventral axis. Birth Defects Res. C Embryo Today 2006, 78, 224–242. [Google Scholar] [CrossRef]
  21. Stickney, H.L.; Imai, Y.; Draper, B.; Moens, C.; Talbot, W.S. Zebrafish bmp4 functions during late gastrulation to specify ventroposterior cell fates. Dev. Biol. 2007, 310, 71–84. [Google Scholar] [CrossRef] [PubMed]
  22. Friedle, H.; Knochel, W. Cooperative interaction of Xvent-2 and GATA-2 in the activation of the ventral homeobox gene Xvent-1B. J. Biol. Chem. 2002, 277, 23872–23881. [Google Scholar] [CrossRef] [PubMed]
  23. Messenger, N.J.; Kabitschke, C.; Andrews, R.; Grimmer, D.; Nunez Miguel, R.; Blundell, T.L.; Smith, J.C.; Wardle, F.C. Functional specificity of the Xenopus T-domain protein Brachyury is conferred by its ability to interact with Smad1. Dev. Cell 2005, 8, 599–610. [Google Scholar] [CrossRef] [PubMed]
  24. Onichtchouk, D.; Gawantka, V.; Dosch, R.; Delius, H.; Hirschfeld, K.; Blumenstock, C.; Niehrs, C. The Xvent-2 homeobox gene is part of the BMP-4 signalling pathway controlling [correction of controling] dorsoventral patterning of Xenopus mesoderm. Development 1996, 122, 3045–3053. [Google Scholar] [CrossRef] [PubMed]
  25. Schuler-Metz, A.; Knochel, S.; Kaufmann, E.; Knochel, W. The homeodomain transcription factor Xvent-2 mediates autocatalytic regulation of BMP-4 expression in Xenopus embryos. J. Biol. Chem. 2000, 275, 34365–34374. [Google Scholar] [CrossRef] [PubMed]
  26. Trindade, M.; Tada, M.; Smith, J.C. DNA-binding specificity and embryological function of Xom (Xvent-2). Dev. Biol. 1999, 216, 442–456. [Google Scholar] [CrossRef]
  27. Ladher, R.; Mohun, T.J.; Smith, J.C.; Snape, A.M. Xom: A Xenopus homeobox gene that mediates the early effects of BMP-4. Development 1996, 122, 2385–2394. [Google Scholar] [CrossRef]
  28. Papalopulu, N.; Kintner, C. A Xenopus gene, Xbr-1, defines a novel class of homeobox genes and is expressed in the dorsal ciliary margin of the eye. Dev. Biol. 1996, 174, 104–114. [Google Scholar] [CrossRef]
  29. Zhong, Y.F.; Holland, P.W. The dynamics of vertebrate homeobox gene evolution: Gain and loss of genes in mouse and human lineages. BMC Evol. Biol. 2011, 11, 169. [Google Scholar] [CrossRef]
  30. Ault, K.T.; Dirksen, M.L.; Jamrich, M. A novel homeobox gene PV.1 mediates induction of ventral mesoderm in Xenopus embryos. Proc. Natl. Acad. Sci. USA 1996, 93, 6415–6420. [Google Scholar] [CrossRef]
  31. Dale, L.; Wardle, F.C. A gradient of BMP activity specifies dorsal-ventral fates in early Xenopus embryos. Semin. Cell Dev. Biol. 1999, 10, 319–326. [Google Scholar] [CrossRef] [PubMed]
  32. Gentner, E.; Vegi, N.M.; Mulaw, M.A.; Mandal, T.; Bamezai, S.; Claus, R.; Tasdogan, A.; Quintanilla-Martinez, L.; Grunenberg, A.; Dohner, K.; et al. VENTX induces expansion of primitive erythroid cells and contributes to the development of acute myeloid leukemia in mice. Oncotarget 2016, 7, 86889–86901. [Google Scholar] [CrossRef] [PubMed]
  33. Hwang, Y.S.; Seo, J.J.; Cha, S.W.; Lee, H.S.; Lee, S.Y.; Roh, D.H.; Kung Hf, H.F.; Kim, J.; Ja Park, M. Antimorphic PV.1 causes secondary axis by inducing ectopic organizer. Biochem. Biophys. Res. Commun. 2002, 292, 1081–1086. [Google Scholar] [CrossRef] [PubMed]
  34. Kawahara, A.; Wilm, T.; Solnica-Krezel, L.; Dawid, I.B. Antagonistic role of vega1 and bozozok/dharma homeobox genes in organizer formation. Proc. Natl. Acad. Sci. USA 2000, 97, 12121–12126. [Google Scholar] [CrossRef] [PubMed]
  35. Lee, S.Y.; Lim, S.K.; Cha, S.W.; Yoon, J.; Lee, S.H.; Lee, H.S.; Park, J.B.; Lee, J.Y.; Kim, S.C.; Kim, J. Inhibition of FGF signaling converts dorsal mesoderm to ventral mesoderm in early Xenopus embryos. Differentiation 2011, 82, 99–107. [Google Scholar] [CrossRef]
  36. Lee, S.Y.; Yoon, J.; Lee, M.H.; Jung, S.K.; Kim, D.J.; Bode, A.M.; Kim, J.; Dong, Z. The role of heterodimeric AP-1 protein comprised of JunD and c-Fos proteins in hematopoiesis. J. Biol. Chem. 2012, 287, 31342–31348. [Google Scholar] [CrossRef]
  37. Shapira, E.; Marom, K.; Yelin, R.; Levy, A.; Fainsod, A. A role for the homeobox gene Xvex-1 as part of the BMP-4 ventral signaling pathway. Mech. Dev. 1999, 86, 99–111. [Google Scholar] [CrossRef]
  38. Shimizu, T.; Yamanaka, Y.; Nojima, H.; Yabe, T.; Hibi, M.; Hirano, T. A novel repressor-type homeobox gene, ved, is involved in dharma/bozozok-mediated dorsal organizer formation in zebrafish. Mech. Dev. 2002, 118, 125–138. [Google Scholar] [CrossRef]
  39. De Robertis, E.M.; Kuroda, H. Dorsal-ventral patterning and neural induction in Xenopus embryos. Annu. Rev. Cell Dev. Biol. 2004, 20, 285–308. [Google Scholar] [CrossRef]
  40. Hemmati-Brivanlou, A.; Thomsen, G.H. Ventral mesodermal patterning in Xenopus embryos: Expression patterns and activities of BMP-2 and BMP-4. Dev. Genet. 1995, 17, 78–89. [Google Scholar] [CrossRef]
  41. Maeno, M.; Mead, P.E.; Kelley, C.; Xu, R.H.; Kung, H.F.; Suzuki, A.; Ueno, N.; Zon, L.I. The role of BMP-4 and GATA-2 in the induction and differentiation of hematopoietic mesoderm in Xenopus laevis. Blood 1996, 88, 1965–1972. [Google Scholar] [CrossRef] [PubMed]
  42. Xu, R.H.; Ault, K.T.; Kim, J.; Park, M.J.; Hwang, Y.S.; Peng, Y.; Sredni, D.; Kung, H. Opposite effects of FGF and BMP-4 on embryonic blood formation: Roles of PV.1 and GATA-2. Dev. Biol. 1999, 208, 352–361. [Google Scholar] [CrossRef] [PubMed]
  43. Friedle, H.; Rastegar, S.; Paul, H.; Kaufmann, E.; Knochel, W. Xvent-1 mediates BMP-4-induced suppression of the dorsal-lip-specific early response gene XFD-1’ in Xenopus embryos. EMBO J. 1998, 17, 2298–2307. [Google Scholar] [CrossRef] [PubMed][Green Version]
  44. Imai, Y.; Gates, M.A.; Melby, A.E.; Kimelman, D.; Schier, A.F.; Talbot, W.S. The homeobox genes vox and vent are redundant repressors of dorsal fates in zebrafish. Development 2001, 128, 2407–2420. [Google Scholar] [CrossRef] [PubMed]
  45. Kawahara, A.; Wilm, T.; Solnica-Krezel, L.; Dawid, I.B. Functional interaction of vega2 and goosecoid homeobox genes in zebrafish. Genesis 2000, 28, 58–67. [Google Scholar] [CrossRef]
  46. Gawantka, V.; Delius, H.; Hirschfeld, K.; Blumenstock, C.; Niehrs, C. Antagonizing the Spemann organizer: Role of the homeobox gene Xvent-1. EMBO J. 1995, 14, 6268–6279. [Google Scholar] [CrossRef] [PubMed]
  47. Onichtchouk, D.; Glinka, A.; Niehrs, C. Requirement for Xvent-1 and Xvent-2 gene function in dorsoventral patterning of Xenopus mesoderm. Development 1998, 125, 1447–1456. [Google Scholar] [CrossRef]
  48. Scerbo, P.; Girardot, F.; Vivien, C.; Markov, G.V.; Luxardi, G.; Demeneix, B.; Kodjabachian, L.; Coen, L. Ventx factors function as Nanog-like guardians of developmental potential in Xenopus. PLoS ONE 2012, 7, e36855. [Google Scholar] [CrossRef]
  49. Scerbo, P.; Marchal, L.; Kodjabachian, L. Lineage commitment of embryonic cells involves MEK1-dependent clearance of pluripotency regulator Ventx2. eLife 2017, 6, e21526. [Google Scholar] [CrossRef]
  50. Wu, X.; Gao, H.; Bleday, R.; Zhu, Z. Homeobox transcription factor VentX regulates differentiation and maturation of human dendritic cells. J. Biol. Chem. 2014, 289, 14633–14643. [Google Scholar] [CrossRef]
  51. Wu, X.; Gao, H.; Ke, W.; Giese, R.W.; Zhu, Z. The homeobox transcription factor VentX controls human macrophage terminal differentiation and proinflammatory activation. J. Clin. Investig. 2011, 121, 2599–2613. [Google Scholar] [CrossRef] [PubMed][Green Version]
  52. Gartel, A.L.; Radhakrishnan, S.K. Lost in transcription: p21 repression, mechanisms, and consequences. Cancer Res. 2005, 65, 3980–3985. [Google Scholar] [CrossRef] [PubMed]
  53. Deng, C.; Zhang, P.; Harper, J.W.; Elledge, S.J.; Leder, P. Mice lacking p21CIP1/WAF1 undergo normal development, but are defective in G1 checkpoint control. Cell 1995, 82, 675–684. [Google Scholar] [CrossRef]
  54. Wu, X.; Gao, H.; Ke, W.; Hager, M.; Xiao, S.; Freeman, M.R.; Zhu, Z. VentX trans-activates p53 and p16ink4a to regulate cellular senescence. J. Biol. Chem. 2011, 286, 12693–12701. [Google Scholar] [CrossRef] [PubMed]
  55. Schmid, M.; Evans, B.J.; Bogart, J.P. Polyploidy in Amphibia. Cytogenet. Genome Res. 2015, 145, 315–330. [Google Scholar] [CrossRef] [PubMed]
  56. Becak, M.L. Polyploidy and epigenetic events in the evolution of Anura. Genet. Mol. Res. 2014, 13, 5995–6014. [Google Scholar] [CrossRef]
  57. Burgess, S. Genomics: A matched set of frog sequences. Nature 2016, 538, 320–321. [Google Scholar] [CrossRef][Green Version]
  58. Xie, J.; Nachabe, A.; Hathaway, L.J.; Farah, B.; Berbari, B.; Li, Y.; Brown, T.C.; Schmid, J.L.; Socola, F.; Saba, N.S.; et al. The prognostic implications of tetraploidy/near-Tetraploidy in acute myeloid leukemia: A case series and systematic review of the literature. Leuk Lymphoma 2021, 62, 203–210. [Google Scholar] [CrossRef]
  59. Singh, M.D.; Jensen, M.; Lasser, M.; Huber, E.; Yusuff, T.; Pizzo, L.; Lifschutz, B.; Desai, I.; Kubina, A.; Yennawar, S.; et al. NCBP2 modulates neurodevelopmental defects of the 3q29 deletion in Drosophila and Xenopus laevis models. PLoS Genet. 2020, 16, e1008590. [Google Scholar] [CrossRef]
  60. Yaguchi, K.; Yamamoto, T.; Matsui, R.; Shimada, M.; Shibanuma, A.; Kamimura, K.; Koda, T.; Uehara, R. Tetraploidy-associated centrosome overduplication in mouse early embryos. Commun. Integr. Biol. 2018, 11, e1526605. [Google Scholar] [CrossRef]
  61. Tanaka, K.; Goto, H.; Nishimura, Y.; Kasahara, K.; Mizoguchi, A.; Inagaki, M. Tetraploidy in cancer and its possible link to aging. Cancer Sci. 2018, 109, 2632–2640. [Google Scholar] [CrossRef] [PubMed]
  62. Frade, J.M.; Lopez-Sanchez, N. Neuronal tetraploidy in Alzheimer and aging. Aging 2017, 9, 2014–2015. [Google Scholar] [CrossRef] [PubMed]
  63. Tandon, P.; Conlon, F.; Furlow, J.D.; Horb, M.E. Expanding the genetic toolkit in Xenopus: Approaches and opportunities for human disease modeling. Dev. Biol. 2017, 426, 325–335. [Google Scholar] [CrossRef] [PubMed]
  64. Jonsdottir, A.B.; Stefansson, O.A.; Bjornsson, J.; Jonasson, J.G.; Ogmundsdottir, H.M.; Eyfjord, J.E. Tetraploidy in BRCA2 breast tumours. Eur. J. Cancer 2012, 48, 305–310. [Google Scholar] [CrossRef]
  65. Takeuchi, M.; Takeuchi, K.; Ozawa, Y.; Kohara, A.; Mizusawa, H. Aneuploidy in immortalized human mesenchymal stem cells with non-random loss of chromosome 13 in culture. Vitr. Cell Dev. Biol. Anim. 2009, 45, 290–299. [Google Scholar] [CrossRef]
  66. Nguyen, H.G.; Ravid, K. Tetraploidy/aneuploidy and stem cells in cancer promotion: The role of chromosome passenger proteins. J. Cell Physiol. 2006, 208, 12–22. [Google Scholar] [CrossRef]
  67. Burglin, T.R. The PBC domain contains a MEINOX domain: Coevolution of Hox and TALE homeobox genes? Dev. Genes. Evol. 1998, 208, 113–116. [Google Scholar] [CrossRef]
  68. Yoon, J.; Kim, J.H.; Lee, S.Y.; Kim, S.; Park, J.B.; Lee, J.Y.; Kim, J. PV.1 induced by FGF-Xbra functions as a repressor of neurogenesis in Xenopus embryos. BMB Rep. 2014, 47, 673. [Google Scholar] [CrossRef]
  69. Zhong, Y.F.; Holland, P.W. HomeoDB2: Functional expansion of a comparative homeobox gene database for evolutionary developmental biology. Evol. Dev. 2011, 13, 567–568. [Google Scholar] [CrossRef]
  70. Zhong, Y.F.; Butts, T.; Holland, P.W. HomeoDB: A database of homeobox gene diversity. Evol. Dev. 2008, 10, 516–518. [Google Scholar] [CrossRef]
  71. Ault, K.T.; Xu, R.H.; Kung, H.F.; Jamrich, M. The homeobox gene PV.1 mediates specification of the prospective neural ectoderm in Xenopus embryos. Dev. Biol. 1997, 192, 162–171. [Google Scholar] [CrossRef] [PubMed]
  72. Hwang, Y.S.; Lee, H.S.; Roh, D.H.; Cha, S.; Lee, S.Y.; Seo, J.J.; Kim, J.; Park, M.J. Active repression of organizer genes by C-terminal domain of PV.1. Biochem. Biophys. Res. Commun. 2003, 308, 79–86. [Google Scholar] [CrossRef]
  73. Kumar, V.; Park, S.; Lee, U.; Kim, J. The Organizer and Its Signaling in Embryonic Development. J. Dev. Biol. 2021, 9, 47. [Google Scholar] [CrossRef]
  74. Kumar, V.; Goutam, R.S.; Park, S.; Lee, U.; Kim, J. Functional Roles of FGF Signaling in Early Development of Vertebrate Embryos. Cells 2021, 10, 2148. [Google Scholar] [CrossRef]
  75. Kumar, V.; Umair, Z.; Kumar, S.; Lee, U.; Kim, J. Smad2 and Smad3 differentially modulate chordin transcription via direct binding on the distal elements in gastrula Xenopus embryos. Biochem. Biophys. Res. Commun. 2021, 559, 168–175. [Google Scholar] [CrossRef]
  76. Umair, Z.; Kumar, S.; Kim, D.H.; Rafiq, K.; Kumar, V.; Kim, S.; Park, J.B.; Lee, J.Y.; Lee, U.; Kim, J. Ventx1.1 as a Direct Repressor of Early Neural Gene zic3 in Xenopus laevis. Mol. Cells 2018, 41, 1061–1071. [Google Scholar] [CrossRef] [PubMed]
  77. Yoon, J.; Kim, J.H.; Kim, S.C.; Park, J.B.; Lee, J.Y.; Kim, J. PV.1 suppresses the expression of FoxD5b during neural induction in Xenopus embryos. Mol. Cells 2014, 37, 220–225. [Google Scholar] [CrossRef]
  78. Kumar, V.; Goutam, R.S.; Umair, Z.; Park, S.; Lee, U.; Kim, J. Foxd4l1.1 Negatively Regulates Chordin Transcription in Neuroectoderm of Xenopus Gastrula. Cells 2021, 10, 2779. [Google Scholar] [CrossRef]
  79. Kumar, S.; Umair, Z.; Kumar, V.; Kumar, S.; Lee, U.; Kim, J. Foxd4l1.1 negatively regulates transcription of neural repressor ventx1.1 during neuroectoderm formation in Xenopus embryos. Sci. Rep. 2020, 10, 16780. [Google Scholar] [CrossRef]
  80. Kumar, S.; Umair, Z.; Kumar, V.; Lee, U.; Choi, S.C.; Kim, J. Ventx1.1 competes with a transcriptional activator Xcad2 to regulate negatively its own expression. BMB Rep. 2019, 52, 403–408. [Google Scholar] [CrossRef]
  81. Pillemer, G.; Yelin, R.; Epstein, M.; Gont, L.; Frumkin, Y.; Yisraeli, J.K.; Steinbeisser, H.; Fainsod, A. The Xcad-2 gene can provide a ventral signal independent of BMP-4. Mech. Dev. 1998, 74, 133–143. [Google Scholar] [CrossRef]
  82. Kumano, G.; Belluzzi, L.; Smith, W.C. Spatial and temporal properties of ventral blood island induction in Xenopus laevis. Development 1999, 126, 5327–5337. [Google Scholar] [CrossRef] [PubMed]
  83. Sander, V.; Reversade, B.; De Robertis, E.M. The opposing homeobox genes Goosecoid and Vent1/2 self-regulate Xenopus patterning. EMBO J. 2007, 26, 2955–2965. [Google Scholar] [CrossRef] [PubMed]
  84. Rogers, C.D.; Archer, T.C.; Cunningham, D.D.; Grammer, T.C.; Casey, E.M. Sox3 expression is maintained by FGF signaling and restricted to the neural plate by Vent proteins in the Xenopus embryo. Dev. Biol. 2008, 313, 307–319. [Google Scholar] [CrossRef] [PubMed]
  85. Miyazaki, A.; Ishii, K.; Yamashita, S.; Nejigane, S.; Matsukawa, S.; Ito, Y.; Onuma, Y.; Asashima, M.; Michiue, T. mNanog possesses dorsal mesoderm-inducing ability by modulating both BMP and Activin/nodal signaling in Xenopus ectodermal cells. PLoS ONE 2012, 7, e46630. [Google Scholar] [CrossRef] [PubMed]
  86. Zhu, Z.; Kirschner, M. Regulated proteolysis of Xom mediates dorsoventral pattern formation during early Xenopus development. Dev. Cell 2002, 3, 557–568. [Google Scholar] [CrossRef]
  87. Gao, H.; Wu, B.; Giese, R.; Zhu, Z. Xom interacts with and stimulates transcriptional activity of LEF1/TCFs: Implications for ventral cell fate determination during vertebrate embryogenesis. Cell Res. 2007, 17, 345–356. [Google Scholar] [CrossRef]
  88. Wroble, B.N.; Finkielstein, C.V.; Sible, J.C. Wee1 kinase alters cyclin E/Cdk2 and promotes apoptosis during the early embryonic development of Xenopus laevis. BMC Dev. Biol. 2007, 7, 119. [Google Scholar] [CrossRef]
  89. Trindade, M.; Messenger, N.; Papin, C.; Grimmer, D.; Fairclough, L.; Tada, M.; Smith, J.C. Regulation of apoptosis in the Xenopus embryo by Bix3. Development 2003, 130, 4611–4622. [Google Scholar] [CrossRef]
  90. Wu, B.; Gao, H.; Le, Y.; Wu, X.; Zhu, Z. Xom induces proteolysis of beta-catenin through GSK3beta-mediated pathway. FEBS Lett. 2018, 592, 299–309. [Google Scholar] [CrossRef]
  91. Schuff, M.; Siegel, D.; Philipp, M.; Bundschu, K.; Heymann, N.; Donow, C.; Knochel, W. Characterization of Danio rerio Nanog and functional comparison to Xenopus Vents. Stem. Cells Dev. 2012, 21, 1225–1238. [Google Scholar] [CrossRef] [PubMed]
  92. Chambers, I.; Silva, J.; Colby, D.; Nichols, J.; Nijmeijer, B.; Robertson, M.; Vrana, J.; Jones, K.; Grotewold, L.; Smith, A. Nanog safeguards pluripotency and mediates germline development. Nature 2007, 450, 1230–1234. [Google Scholar] [CrossRef] [PubMed]
  93. Scerbo, P.; Monsoro-Burq, A.H. The vertebrate-specific VENTX/NANOG gene empowers neural crest with ectomesenchyme potential. Sci. Adv. 2020, 6, eaaz1469. [Google Scholar] [CrossRef] [PubMed]
  94. Shakhova, O.; Sommer, L. Neural crest-derived stem cells. In StemBook; Harvard Stem Cell Institute: Cambridge, MA, USA, 2008. [Google Scholar] [CrossRef]
  95. Fraser, G.J.; Hulsey, C.D.; Bloomquist, R.F.; Uyesugi, K.; Manley, N.R.; Streelman, J.T. An ancient gene network is co-opted for teeth on old and new jaws. PLoS Biol. 2009, 7, e31. [Google Scholar] [CrossRef]
  96. Miletich, I.; Yu, W.Y.; Zhang, R.; Yang, K.; Caixeta de Andrade, S.; Pereira, S.F.; Ohazama, A.; Mock, O.B.; Buchner, G.; Sealby, J.; et al. Developmental stalling and organ-autonomous regulation of morphogenesis. Proc. Natl. Acad. Sci. USA 2011, 108, 19270–19275. [Google Scholar] [CrossRef]
  97. Nichols, J.T.; Pan, L.; Moens, C.B.; Kimmel, C.B. barx1 represses joints and promotes cartilage in the craniofacial skeleton. Development 2013, 140, 2765–2775. [Google Scholar] [CrossRef]
  98. Sperber, S.M.; Dawid, I.B. barx1 is necessary for ectomesenchyme proliferation and osteochondroprogenitor condensation in the zebrafish pharyngeal arches. Dev. Biol. 2008, 321, 101–110. [Google Scholar] [CrossRef]
  99. Gao, H.; Le, Y.; Wu, X.; Silberstein, L.E.; Giese, R.W.; Zhu, Z. VentX, a novel lymphoid-enhancing factor/T-cell factor-associated transcription repressor, is a putative tumor suppressor. Cancer Res. 2010, 70, 202–211. [Google Scholar] [CrossRef][Green Version]
  100. Kim, B.M.; Buchner, G.; Miletich, I.; Sharpe, P.T.; Shivdasani, R.A. The stomach mesenchymal transcription factor Barx1 specifies gastric epithelial identity through inhibition of transient Wnt signaling. Dev. Cell 2005, 8, 611–622. [Google Scholar] [CrossRef]
  101. Kim, B.M.; Miletich, I.; Mao, J.; McMahon, A.P.; Sharpe, P.A.; Shivdasani, R.A. Independent functions and mechanisms for homeobox gene Barx1 in patterning mouse stomach and spleen. Development 2007, 134, 3603–3613. [Google Scholar] [CrossRef]
  102. Shapira, E.; Marom, K.; Levy, V.; Yelin, R.; Fainsod, A. The Xvex-1 antimorph reveals the temporal competence for organizer formation and an early role for ventral homeobox genes. Mech. Dev. 2000, 90, 77–87. [Google Scholar] [CrossRef]
  103. Gilardelli, C.N.; Pozzoli, O.; Sordino, P.; Matassi, G.; Cotelli, F. Functional and hierarchical interactions among zebrafish vox/vent homeobox genes. Dev. Dyn. 2004, 230, 494–508. [Google Scholar] [CrossRef] [PubMed]
  104. Melby, A.E.; Clements, W.K.; Kimelman, D. Regulation of dorsal gene expression in Xenopus by the ventralizing homeodomain gene Vox. Dev. Biol. 1999, 211, 293–305. [Google Scholar] [CrossRef] [PubMed]
  105. Xie, Y.; Liu, C. Xom, a ventralizing factor, regulates beta-catenin levels and cell fate. FEBS Lett. 2018, 592, 297–298. [Google Scholar] [CrossRef]
  106. Leibovich, A.; Kot-Leibovich, H.; Ben-Zvi, D.; Fainsod, A. ADMP controls the size of Spemann’s organizer through a network of self-regulating expansion-restriction signals. BMC Biol. 2018, 16, 13. [Google Scholar] [CrossRef]
  107. Watanabe, M.; Yasuoka, Y.; Mawaribuchi, S.; Kuretani, A.; Ito, M.; Kondo, M.; Ochi, H.; Ogino, H.; Fukui, A.; Taira, M.; et al. Conservatism and variability of gene expression profiles among homeologous transcription factors in Xenopus laevis. Dev. Biol. 2017, 426, 301–324. [Google Scholar] [CrossRef]
  108. Trompouki, E.; Bowman, T.V.; Lawton, L.N.; Fan, Z.P.; Wu, D.C.; DiBiase, A.; Martin, C.S.; Cech, J.N.; Sessa, A.K.; Leblanc, J.L.; et al. Lineage regulators direct BMP and Wnt pathways to cell-specific programs during differentiation and regeneration. Cell 2011, 147, 577–589. [Google Scholar] [CrossRef]
  109. Le, Y.; Gao, H.; Bleday, R.; Zhu, Z. The homeobox protein VentX reverts immune suppression in the tumor microenvironment. Nat. Commun. 2018, 9, 2175. [Google Scholar] [CrossRef]
  110. Le, Y.; Gao, H.; Richards, W.; Zhao, L.; Bleday, R.; Clancy, T.; Zhu, Z. VentX expression in tumor-associated macrophages promotes phagocytosis and immunity against pancreatic cancers. JCI Insight 2020, 5, e137088. [Google Scholar] [CrossRef]
  111. Ino, Y.; Yamazaki-Itoh, R.; Shimada, K.; Iwasaki, M.; Kosuge, T.; Kanai, Y.; Hiraoka, N. Immune cell infiltration as an indicator of the immune microenvironment of pancreatic cancer. Br. J. Cancer 2013, 108, 914–923. [Google Scholar] [CrossRef]
  112. Gao, H.; Wu, X.; Sun, Y.; Zhou, S.; Silberstein, L.E.; Zhu, Z. Suppression of homeobox transcription factor VentX promotes expansion of human hematopoietic stem/multipotent progenitor cells. J. Biol. Chem. 2012, 287, 29979–29987. [Google Scholar] [CrossRef] [PubMed]
  113. Elagib, K.E.; Goldfarb, A.N. Oncogenic pathways of AML1-ETO in acute myeloid leukemia: Multifaceted manipulation of marrow maturation. Cancer Lett. 2007, 251, 179–186. [Google Scholar] [CrossRef] [PubMed]
  114. Vargas, A.C.; Gray, L.A.; White, C.L.; Maclean, F.M.; Grimison, P.; Ardakani, N.M.; Bonar, F.; Algar, E.M.; Cheah, A.L.; Russell, P.; et al. Genome wide methylation profiling of selected matched soft tissue sarcomas identifies methylation changes in metastatic and recurrent disease. Sci. Rep. 2021, 11, 667. [Google Scholar] [CrossRef]
  115. Gao, H.; Wu, B.; Le, Y.; Zhu, Z. Homeobox protein VentX induces p53-independent apoptosis in cancer cells. Oncotarget 2016, 7, 39719–39729. [Google Scholar] [CrossRef] [PubMed][Green Version]
  116. Grubelnik, G.; Bostjancic, E.; Pavlic, A.; Kos, M.; Zidar, N. NANOG expression in human development and cancerogenesis. Exp Biol. Med. 2020, 245, 456–464. [Google Scholar] [CrossRef] [PubMed]
  117. Nagel, S.; Scherr, M.; MacLeod, R.A.F.; Pommerenke, C.; Koeppel, M.; Meyer, C.; Kaufmann, M.; Dallmann, I.; Drexler, H.G. NKL homeobox gene activities in normal and malignant myeloid cells. PLoS ONE 2019, 14, e0226212. [Google Scholar] [CrossRef] [PubMed]
  118. Brandner, S. Nanog, Gli, and p53: A new network of stemness in development and cancer. EMBO J. 2010, 29, 2475–2476. [Google Scholar] [CrossRef]
  119. Zbinden, M.; Duquet, A.; Lorente-Trigos, A.; Ngwabyt, S.N.; Borges, I.; Ruiz i Altaba, A. NANOG regulates glioma stem cells and is essential in vivo acting in a cross-functional network with GLI1 and p53. EMBO J. 2010, 29, 2659–2674. [Google Scholar] [CrossRef]
  120. Wang, S.; Fan, H.; Xu, J.; Zhao, E. Prognostic implication of NOTCH1 in early stage oral squamous cell cancer with occult metastases. Clin. Oral Investig. 2018, 22, 1131–1138. [Google Scholar] [CrossRef]
  121. Schier, A.F. Axis formation and patterning in zebrafish. Curr. Opin. Genet. Dev. 2001, 11, 393–404. [Google Scholar] [CrossRef]
  122. Mimoto, M.S.; Kwon, S.; Green, Y.S.; Goldman, D.; Christian, J.L. GATA2 regulates Wnt signaling to promote primitive red blood cell fate. Dev. Biol. 2015, 407, 1–11. [Google Scholar] [CrossRef] [PubMed]
  123. Kelley, C.; Yee, K.; Harland, R.; Zon, L.I. Ventral expression of GATA-1 and GATA-2 in the Xenopus embryo defines induction of hematopoietic mesoderm. Dev. Biol. 1994, 165, 193–205. [Google Scholar] [CrossRef] [PubMed]
  124. Yang, L.; Sun, H.; Cao, Y.; Xuan, B.; Fan, Y.; Sheng, H.; Zhuang, W. GATA2 Inhibition Sensitizes Acute Myeloid Leukemia Cells to Chemotherapy. PLoS ONE 2017, 12, e0170630. [Google Scholar] [CrossRef]
  125. Saida, S.; Zhen, T.; Kim, E.; Yu, K.; Lopez, G.; McReynolds, L.J.; Liu, P.P. Gata2 deficiency delays leukemogenesis while contributing to aggressive leukemia phenotype in Cbfb-MYH11 knockin mice. Leukemia 2020, 34, 759–770. [Google Scholar] [CrossRef] [PubMed]
  126. Luesink, M.; Hollink, I.H.; van der Velden, V.H.; Knops, R.H.; Boezeman, J.B.; de Haas, V.; Trka, J.; Baruchel, A.; Reinhardt, D.; van der Reijden, B.A.; et al. High GATA2 expression is a poor prognostic marker in pediatric acute myeloid leukemia. Blood 2012, 120, 2064–2075. [Google Scholar] [CrossRef] [PubMed]
  127. Hwang, Y.S.; Chae, J.P.; Kim, D.S.; Park, K.M.; Bae, Y.C.; Park, M.J. Screening of Interacting Proteins with PV. 1 as Downstream Factors of BMP Signal. Korean J. Anat. 2007, 40, 203–210. [Google Scholar]
Ijms 23 02741 g001
Figure 1. Chromosomal localization of Ventx gene synteny in humans and other animal species relative to adjacent genes (color-coded).
Figure 1. Chromosomal localization of Ventx gene synteny in humans and other animal species relative to adjacent genes (color-coded).
Ijms 23 02741 g001
Ijms 23 02741 g002
Figure 2. Schematic representation of conserved domains and motifs associated with different classes of HD proteins in animals. This figure was adapted from Burglin et al. (2016) [9].
Figure 2. Schematic representation of conserved domains and motifs associated with different classes of HD proteins in animals. This figure was adapted from Burglin et al. (2016) [9].
Ijms 23 02741 g002
Ijms 23 02741 g003
Figure 3. Schematic representations of Ventx domains in Xenopus laevis, zebrafish, and humans. (A) All Ventx members contain a transactivation domain (green), a highly conserved homeobox DNA-binding domain (HD, 60 aa, pink), and a repressor domain (grey), which inhibits the expression of dorsal-specific genes such as gsc, chordin, and boz/dha. The N-terminal domain (ND) of the Ventx family acts as a transactivation domain (TAD) to activate ventral-specific genes such as bmp4, ventx1.1, ventx1.2, Ventx2.2, and Ventx2.2. (B) An evolutionary phylogenetic tree of the Ventx gene cluster in Xenopus laevis. (C) An evolutionary phylogenetic tree of the vega/ventx gene cluster in zebrafish. (B’,C’) The percentage-identity matrix of Ventx family members in Xenopus and zebrafish.
Figure 3. Schematic representations of Ventx domains in Xenopus laevis, zebrafish, and humans. (A) All Ventx members contain a transactivation domain (green), a highly conserved homeobox DNA-binding domain (HD, 60 aa, pink), and a repressor domain (grey), which inhibits the expression of dorsal-specific genes such as gsc, chordin, and boz/dha. The N-terminal domain (ND) of the Ventx family acts as a transactivation domain (TAD) to activate ventral-specific genes such as bmp4, ventx1.1, ventx1.2, Ventx2.2, and Ventx2.2. (B) An evolutionary phylogenetic tree of the Ventx gene cluster in Xenopus laevis. (C) An evolutionary phylogenetic tree of the vega/ventx gene cluster in zebrafish. (B’,C’) The percentage-identity matrix of Ventx family members in Xenopus and zebrafish.
Ijms 23 02741 g003
Ijms 23 02741 g004
Figure 4. Upstream and downstream regulatory pathways for Ventx members during Xenopus laevis and zebrafish embryonic development and the potential functions of Ventx in human hematopoiesis, cell differentiation, and leukemogenesis. Lines with arrows indicate promoting and those with bars suppressing (functions of) the targets. Indirect targets of Ventx family members are in red. Sign (?) indicates unknown factors.
Figure 4. Upstream and downstream regulatory pathways for Ventx members during Xenopus laevis and zebrafish embryonic development and the potential functions of Ventx in human hematopoiesis, cell differentiation, and leukemogenesis. Lines with arrows indicate promoting and those with bars suppressing (functions of) the targets. Indirect targets of Ventx family members are in red. Sign (?) indicates unknown factors.
Ijms 23 02741 g004
Table 1. Summary of all HD proteins based on additional domains and conserved amino acid (AA) locations in DNA-binding homeobox domain. The sign (-) indicates the absence of glutamine residue at N + 1 position.
Table 1. Summary of all HD proteins based on additional domains and conserved amino acid (AA) locations in DNA-binding homeobox domain. The sign (-) indicates the absence of glutamine residue at N + 1 position.
SuperclassClassSubclassAA Position in HDAA in HD
ANTPHoxLN = 5N + 1X = 50X + 1
Arginine-GlutamineLysine60
NKLArginineGlutamineGlutamine-60
PRDPaxArginine-Serine-60
PRD-likePaxLArginine-Glutamine(X + 3) Lysine60
LIM Arginine-Glutamine-60
ZF Arginine-GlutamineArginine60
POU Arginine-Cysteine-60
HNF Arginine-Alanine-60
CUTCuxArginine-Histidine-60
ONECUTArginine-Methionine-60
CMPArginine-Lysine 60
SATBArginine-Glutamine-60
PROS Serine-Serine-60
CERS Serine-Arginine 60
SIX/SO Serine, threonine, valine-lysine-60
TALEPBC Arginine-Glycine-63
MEIS Arginine-Isoleucine-63
TGIF Arginine-Isoleucine-63
IRO Arginine-Alanine-63
MKX Lysine-Alanine-63
Table 2. Numbers of all HD proteins identified in humans, Xenopus, and zebrafish distributed across homeobox classes, subclasses, and families based on HD and additional domains.
Table 2. Numbers of all HD proteins identified in humans, Xenopus, and zebrafish distributed across homeobox classes, subclasses, and families based on HD and additional domains.
Homeobox ClassSubclassNumber of Families of Different ClassesNumber of GenesReferences
HumanXenopusZebrafishHumanXenopusZebrafish[68,69]
http://homeodb.zoo.ox.ac.uk/ (accessed on 27 December 2021)
ANTPHoxL141414525368
NKL232222676064
PRDPax333759
PRD-likePaxL281818913244
LIM 666121220
POU 766241919
HNF 222336
SINE 3336613
TALE 666301629
CUT 3331079
PROS 111223
ZF 555151417
CERS 111523
Others 33191918
Total1059391333250322
Table 3. The chromosomal localization and developmental roles of Ventx/Vega family members in Xenopus, zebrafish, and humans. * Some consider Ventx2.1 Xom/Xbr-1a, whereas others document Ventx2.2 as Xom/Xbr-1a. The genomic locations of a given gene were collected from the following genome browsers: Xenopus (http://www.xenbase.org) genome assembly version V.9.1 jbrowse, Zebrafish (http://www.zfin.org) genome assembly version GRCz11, and human (https://genome.ucsc.edu) genome assembly version GRCh38/hg38. NA indicates not known yet. All datasets are accessed on the 27 December 2021.
Table 3. The chromosomal localization and developmental roles of Ventx/Vega family members in Xenopus, zebrafish, and humans. * Some consider Ventx2.1 Xom/Xbr-1a, whereas others document Ventx2.2 as Xom/Xbr-1a. The genomic locations of a given gene were collected from the following genome browsers: Xenopus (http://www.xenbase.org) genome assembly version V.9.1 jbrowse, Zebrafish (http://www.zfin.org) genome assembly version GRCz11, and human (https://genome.ucsc.edu) genome assembly version GRCh38/hg38. NA indicates not known yet. All datasets are accessed on the 27 December 2021.
NamesChromosomal
Localization		Similarity with Human Ventx (%)Developmental RolesReferences
Xenopus laevis
Venxt1.1/PV.1/Ventx1.1a/Ventx1.1bChr7L:21,842,291–21,845,156
Chr7S:16,920,567–16,923,476		59.02Neural repressor, Spemann-organizer inhibitor, embryonic ventralization, hematopoiesis, axial patterning[30,33,72]
Ventx1.2/Xvent1/Vent1/Vent-1/Xvent-1Chr7L:21,802,386–21,807,247
Chr7S:16,883,662–16,887,492		44.95Neural repressor, Spemann-organizer inhibitor, embryonic ventralization, axial patterning[46,47,83]
Ventx2.1a/Ventx2.1b, Vox1, Vox, Xvent2Chr7L:21,859,318–21,861,104
Chr7S:16,932,131–16,933,936		66.67Neural repressor, Spemann-organizer inhibitor, embryonic ventralization, Ventx1.2 and ventx1.1 activator, hematopoiesis, axial patterning[12,15,104]
Ventx2.2/Xom */Xvent-2/Xbr-1Chr7L:21,830,246–21,832,823
Chr7S:16,908,607–16,911,052		66.67Neural repressor, VMZ activator, induce GSK3β expression, axial patterning, pluripotency marker, neural crest migration[27,28,87,90,105]
Ventx3.1/vent3Chr7L-NA
Chr7S:16,889,505–16,895,419		39.1NA[106,107]
Ventx3.2/Vex1Chr7L:21,784,572–21,787,885
Chr7S:16,870,294–16,873,640		51.32Neural repressor, VMZ activator, axial patterning[37,102]
Zebrafish
Vega1/VoxChr13:50,621,929–50,624,15455Neural repressor, VMZ, activator, axial patterning[34]
Vega2/Vent1Chr13:50,609,716–50,614,71855Neural repressor, VMZ activator, axial patterning[45]
VedChr10:44,997,062–45,002,19649.12Neural repressor, VMZ activator, axial patterning[38]
Human
VentxChr10:133,237,855–133,241,928100Acute myeloid leukemia, cellular senescence, myeloid and macrophage differentiation, dendritic cell differentiation, immunosuppressor, apoptotic activator[17,18]
Publisher’s Note: MDPI stays neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Share and Cite

MDPI and ACS Style

Kumar, S.; Kumar, V.; Li, W.; Kim, J. Ventx Family and Its Functional Similarities with Nanog: Involvement in Embryonic Development and Cancer Progression. Int. J. Mol. Sci. 2022, 23, 2741. https://doi.org/10.3390/ijms23052741

AMA Style

Kumar S, Kumar V, Li W, Kim J. Ventx Family and Its Functional Similarities with Nanog: Involvement in Embryonic Development and Cancer Progression. International Journal of Molecular Sciences. 2022; 23(5):2741. https://doi.org/10.3390/ijms23052741

Chicago/Turabian Style

Kumar, Shiv, Vijay Kumar, Wenchang Li, and Jaebong Kim. 2022. "Ventx Family and Its Functional Similarities with Nanog: Involvement in Embryonic Development and Cancer Progression" International Journal of Molecular Sciences 23, no. 5: 2741. https://doi.org/10.3390/ijms23052741

APA Style

Kumar, S., Kumar, V., Li, W., & Kim, J. (2022). Ventx Family and Its Functional Similarities with Nanog: Involvement in Embryonic Development and Cancer Progression. International Journal of Molecular Sciences, 23(5), 2741. https://doi.org/10.3390/ijms23052741

Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.

Article Metrics

Back to TopTop