Next Article in Journal
Long-Term Outcomes of Maxillary Alveolar Process Trauma and Primary Incisor Injury in Early Childhood: A Case Report
Previous Article in Journal
Diagnostic and Psychometric Properties of the Arabic Sensory Processing Measure—Second Edition, Adult Version
Previous Article in Special Issue
A Narrative Review on the Sperm Selection Methods in Assisted Reproductive Technology: Out with the New, the Old Is Better?
 
 
Search for Articles:
Title / Keyword
Author / Affiliation / Email
Journal
Article Type
 
 
Advanced Search
 
Section
Special Issue
Volume
Issue
Number
Page
 
Journals
JCM
Volume 14
Issue 10
10.3390/jcm14103284
jcm-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

Kisspeptins Regulating Fertility: Potential Future Therapeutic Approach in Infertility Treatment

by
Sonia Kotanidou
1,*,
Nikos Nikolettos
1,
Nektaria Kritsotaki
1,
Panagiotis Tsikouras
1,
Angeliki Tiptiri-Kourpeti
2 and
Konstantinos Nikolettos
3
1
Department of Obstetrics and Gynecology, Democritus University of Thrace, 68100 Alexandroupolis, Greece
2
Genesis Athens-Thrace Medically Assisted Reproduction Unit, Apalos, 68100 Alexandroupolis, Greece
3
Department of Gynaecological Oncology, Maidstone and Turnbridge Wells NHS Trust, Maidstone ME14 1FZ, UK
*
Author to whom correspondence should be addressed.
J. Clin. Med. 2025, 14(10), 3284; https://doi.org/10.3390/jcm14103284
Submission received: 27 March 2025 / Revised: 24 April 2025 / Accepted: 2 May 2025 / Published: 8 May 2025
(This article belongs to the Special Issue Assisted Reproductive Technology and Infertility Treatment: Current Updates and Perspectives)
Versions Notes

Abstract

:
Kisspeptins play a crucial role in the normal functioning of the reproductive axis in both humans and animals by stimulating the secretion of gonadotropin-releasing hormone (GnRH) from the hypothalamus. Recent studies have investigated the association of kisspeptins to infertility of diverse causes and the therapeutic potential of kisspeptins in infertility. Exogenous administration of kisspeptins appears to hold significant promise in restoring fertility, with ongoing studies in their application in ovarian stimulation protocols and as cryoprotectants during vitrification. This review provides a comprehensive analysis of the role of kisspeptins in reproductive physiology and their potential as therapeutic agents for infertility, highlighting their advantages over conventional treatments and their future prospects in clinical practice.

1. Introduction

Infertility is defined as the inability to achieve pregnancy after one year of unprotected intercourse [1]. Worldwide, it presents in 8–12% of reproductive-age couples and can result from factors related to either the female and/or male partner [2]. The pathophysiology of some conditions leading to infertility appears to be associated with a group of peptides known as kisspeptins [3,4,5]. Kisspeptins are considered the most potent stimulators of gonadotropin-releasing hormone (GnRH) secretion from the hypothalamus and their action is essential for normal reproductive function in both humans and animals [6,7].
Recently, the clinical efficacy of kisspeptin administration in individuals facing infertility has been investigated. Exogenous administration of kisspeptins in infertile patients exhibiting reduced kisspeptin expression may restore their fertility [8,9,10]. Furthermore, studies investigate their use in ovarian stimulation protocols or as cryoprotectants during vitrification [11,12]. However, therapeutic protocols utilizing kisspeptins for individuals with infertility have not yet been established, nor has their application been integrated into IVF protocols, as their therapeutic use is currently in its experimental stage and is being investigated for safety and efficacy. The use of kisspeptins may become widespread in the future due to the advantages they offer compared to currently utilized agents [13,14].
The purpose of this review was to present a thorough overview of the involvement of kisspeptins in the reproductive axis, and the potential use of kisspeptin analogs as a therapeutic approach to infertility in the future.

2. Kisspeptins System

Kisspeptins (Kp) are a group of structurally similar peptides synthesized by the KISS1 gene in humans and the Kiss1 gene in non-human species, respectively [15]. Kisspeptins are formed through the proteolytic processing of 145 amino acids precursor, which is proteolyzed further to four biologically active peptides consisting of 54, 14, 13, and 10 amino acids (kisspeptin-54, -14, -13, -10) [15,16]. KISS1, and its derived products, were initially known as suppressors of metastasis in multiple malignancies, such as melanoma, breast cancer, ovarian carcinoma, pancreatic carcinoma, and papillary thyroid carcinoma [15,17,18,19].
Despite the identification of KISS1 products in 2001, the reproductive aspect of the kisspeptin system remained undiscovered until 2003, when two independent studies found an association between mutations of their receptor (Gpr54) and idiopathic hypogonadotropic hypogonadism (iHH) [3,20]. This discovery revealed the correlation of kisspeptin system with the hypothalamic–pituitary–gonadal (HPG) axis, along with the crucial function in puberty onset and fertility. Kisspeptins function as strong stimulators of gonadotropin-releasing hormone (GnRH) secretion by attaching to their receptor—KISS1R [21]. The receptor is common for all the biologically active forms of kisspeptins [22].
The location of kisspeptin synthesis varies among species, as does their expression. In mammals, kisspeptin production is conducted in the arcuate nucleus (ARC) and the preoptic area (POA), whereas in rodents, it occurs in the arcuate nucleus (ARC) and the anteroventral periventricular nucleus (AVPV) [21,23]. The ARC population is responsible for the pulsatile secretion of GnRH and gonadotropins, while the POA population is responsible for generating the preovulatory surge of LH in individuals [21,23,24]. The ARC contains greater KISS1 neurons count compared to POA in mammals [25].
It is important to note that gonadal steroids regulate GnRH secretion through the kisspeptin system [26]. In particular, it has been observed that testosterone and estrogen can reduce the expression of Kiss1 mRNA in the ARC, whereas it increases the expression of Kiss1 mRNA in the anteroventral periventricular nucleus (AVPV), especially at the preovulatory phase across various species [26].

3. KNDy Neurons

Except kisspeptins, within the ARC, another two distinct neuropeptides are co-expressed that have been strongly associated with the feedback regulation of GnRH in POA [27]. The neuropeptides neurokinin B (NKB) and dynorphin (Dyn), along with kisspeptins, collectively define a subpopulation of neurons in ARC referred to as KNDy neurons [27]. NKB has a stimulatory effect, while Dyn an inhibitory effect on KNDy neurons; both function as co-transmitters and auto-regulators of KNDy neurons and control the secretory activity of kisspeptins. When secreted, kisspeptins bind to KISS1R expressed on GnRH neurons of POA and stimulate the secretion of GnRH [22]. A study by Topaloglu et al. showed that mutations in the gene encoding the NKB receptor (TACR3) are associated with idiopathic hypogonadotropic hypogonadism and infertility, confirming the correlation of KNDy neurons with gonadotropin secretion [28].

4. Association of Kisspeptins to Infertility

A defect in the kisspeptin signaling pathway appears to be linked to infertility [3,4,5,29]. Infertility is diagnosed as a failure to conceive after a year of regular unprotected coitus [30] and affects around one in six individuals globally, as reported by the World Health Organization (WHO) [2]. The kisspeptin system plays a critical role in the gonadal axis and has been strongly implicated in numerous causes of infertility, including among others idiopathic hypogonadotropic hypogonadism (iHH), hyperprolactinemia, primary ovarian insufficiency (POI), and polycystic ovarian syndrome (PCOS) [3,4,5,14,29].

4.1. Idiopathic Hypogonadotropic Hypogonadism (iHH)

Mutations or deletion of the Kiss1r gene, which encodes the kisspeptin receptor, lead to iHH in mammals and rodents, as studied initially by Seminara et al. and de Roux et al. in 2003 [3,20]. Differences between mice with the Gpr54 gene and Kiss1r-/- knockout mice have been reported in several studies, including observations of azoospermia, reduced testosterone levels, and smaller testicular size in male rodents [3,20]. In female rodents, findings include smaller ovaries, predominantly containing primary and secondary follicles; lower levels of 17β-estradiol; and an absence of mammary gland enlargement [3,20]. Additionally, both sexes showed a significant reduction in FSH and LH levels compared to the control group. [31,32]. The haploinsufficient Kiss1r mice (Kiss1r+/-) presented with a substantial reduction in the expression of ovarian Kiss1r and expedited primary ovarian insufficiency (POI) [33].
Studies have demonstrated that kisspeptins are necessary for the onset of puberty and specifically for the expansion of GnRH neuron activity [34]. Exogenous administration of kisspeptins in studies induces the production and secretion of GnRH from the pituitary gland, resulting in activation of the reproductive axis [34]. On the other hand, suppression of GnRH secretion, resulting in delayed onset of puberty, was observed by the administration of a kisspeptin antagonist (peptide 234) to female rodents [35,36].

4.2. Hyperprolactinemia

Clinical presentation of hyperprolactinemia in women consist of oligomenorrhea/amenorrhea, anovulatory cycles, galactorrhea, and infertility [37]. Elevated PRL levels inhibit the pulsatile secretion of FSH and LH, resulting in hypogonadotropic hypogonadism mediated via the kisspeptins system [5]. This is supported by the observation that PRL receptors are expressed in a low density on GnRH neurons, whereas KISS1R present PRL receptors in a higher density [5].
The presence of PRL receptors on KISS1 neurons and the suppression of mRNA KISS1 expression due to the elevated levels of PRL indicate the direct inhibitory effect of PRL on KISS1 neurons [8]. The pivotal role of kisspeptins in the pathogenesis of hyperprolactinemia-induced infertility was highlighted in a study by Sonigo et al., which demonstrated that exogenous administration of kisspeptins effectively restores gonadotropin secretion [8,9].
Another study presented the reversal of hyperprolactinemia-induced amenorrhea in two premenopausal women by the exogenous administration of kisspeptin-10 (KP10) [38]. The treatment led to an increase in estradiol and gonadotropin levels, accompanied by follicular growth in the ovaries [38]. Τhis response to the exogenous administration of KΡ10 supports the view that higher PRL levels act by directly suppressing KISS1 neurons. KP10 has the potential for use as a treatment in women who do not respond to therapy with cabergoline (a dopamine agonist) or in women undergoing neuroleptic treatment who wish to conceive [38].

4.3. Primary Ovarian Insufficiency (POI)

Studies conducted in animal models have demonstrated the association between the kisspeptin signaling pathway in the gonads and primary ovarian insufficiency (POI) [33]. Mice with Kiss1r haploinsufficiency exhibited progressive loss of oocytes/follicles, decreased numbers of preantral follicles, and infertility [33]. Additionally, the ovarian tissue displayed an atrophic appearance, with no mature follicles or corpus luteum present during the lifespan of the mice, along with reduced expression of Kiss1r mRNA [33]. Hormonal replacement with gonadotropins in cases of Kiss1r haploinsufficiency, where follicular development and ovulation do not occur, is ineffective [33].
Kisspeptins and their receptor are expressed in the gonads of rodents and mammals, playing a crucial role in ovarian reserves, steroidogenesis, the onset of puberty, and follicular ovulation [39]. The expression of KISS1/KISS1R is generally increased in granulosa cells and theca cells and varies depending on the day of the cycle [33,40]. The expression of KISS1/KISS1R in women increases with follicular development, reaching peak levels during the pre-ovulatory phase due to the increased secretory action of gonadotropins [41,42]. Furthermore, the ovarian expression of kisspeptins prevents follicular atresia and contributes to ovulation during the reproductive years [39].

4.4. Polycystic Ovary Syndrome (PCOS)

Panidis et al. [4] were the first to report that females with PCOS and normal body mass index (BMI) have elevated plasma levels of kisspeptin. Multiple studies later confirmed that women with PCOS, independently of BMI, exhibited augmented kisspeptin levels [43,44,45]. However, the observation is not confirmed when the population sample is statistically small, due to the wide phenotypic spectrum of PCOS [46,47,48]. A recent study also observed a correlation between kisspeptin levels and the age of women with PCOS, but further investigation with more samples is required to confirm this correlation and establish its clinical significance [49].
In women with PCOS, elevated levels of kisspeptins lead to hyperfunction of the HPG axis, resulting in dysregulation of the menstrual cycle. As previously mentioned, kisspeptins are the strongest stimulators of GnRH secretion, which has a significant impact on the secretion of LH [6,7]. Therefore, it is expected that women with PCOS will simultaneously exhibit elevated LH levels, a finding that is not substantiated by studies due to insufficient data. Nyagolova et al. [50] and Jeon et al. [51] confirmed the elevated levels of kisspeptins in women with PCOS; however, they noted that these levels did not exhibit a positive linear correlation with LH levels. The explanation for this phenomenon is provided in the study by Katulski et al., who observed that the secretion of kisspeptins and LH occurs simultaneously only in women with PCOS and normal menstrual cycles [52]. In women with PCOS and oligomenorrhea, the secretion pulses are not synchronized, suggesting that, in addition to menstrual irregularities, there is a disturbance throughout the entire reproductive axis [52].

4.5. Endometriosis

Matrix metalloproteinases (MMPs) play a significant role in the development of endometriosis, as they are responsible for the degradation of extracellular matrix proteins, cell migration, and infiltration. Studies have shown increased activity of MMP-2 and MMP-9 in the endometrial tissue of women with endometriosis compared to that of women without endometriosis [53,54,55]. The action of metalloproteinases appears to be inhibited by kisspeptins [56,57]. An immunohistochemical study by Abdelkareem et al. [58] demonstrated that the endometrium of women with endometriosis exhibited lower levels of KISS1 and KISS1R compared to women without endometriosis. This finding supports the hypothesis regarding the involvement of kisspeptins in the pathophysiology of endometriosis, as their increased expression in the endometrium inhibits the activity of metalloproteinases and cellular infiltration.
The expression of the KISS1 gene in ectopic endometrial tissue is elevated compared to that in the endometrium [59]. This supports the antimetastatic action of kisspeptins and the implantation theory, which posits that reduced KISS1 expression in the endometrium allows for the migration and implantation of ectopic tissue [59]. In contrast, a study by Makri et al. [56] did not detect KISS1 expression in any of the 17 samples from women with endometriosis, which may be attributable to the different methodology used in the studies. Regarding serum kisspeptin levels, women with endometriosis exhibit higher levels compared to the control group [60,61].
Kisspeptins play a significant role in the inhibition of ectopic endometrial migration and implantation. The difference in the expression of KISS1/KISS1R in ectopically implanted endometrial tissue compared to the endometrium of women with and without endometriosis suggests their potential future use as biomarkers for early diagnosis of endometriosis.

4.6. Unexplained Infertility

A review of the literature identified two studies that compared KISS1 levels in infertile couples based on the causative factor. The categorization included male factor infertility, female factor infertility, and unexplained infertility. Women with unexplained infertility had lower levels of kisspeptins compared to women with infertility of other etiologies. The researchers hypothesize that the reduced levels of kisspeptins may be due to mutations in the KISS1 gene, which affect the HPG axis in women [62,63].

4.7. Functional Hypothalamic Amenorrhea (FHA)

Kisspeptin levels in women with FHA and normal body mass index (BMI) in follicular phase are presented lower than in healthy women [64]. Jayasena et al. conducted a study where women with functional hypothalamic amenorrhea received exogenous kisspeptins, exhibiting a fourfold increase in LH levels compared to healthy women during the follicular phase [65]. This finding aligns with a study in rodents with hypothalamic amenorrhea, where reduced Kiss1 expression in the hypothalamus was noted, along with increased expression of its receptor (Kiss1r) [66]. Therefore, hypothalamic amenorrhea appears to be due to a deficiency of kisspeptins in the hypothalamus, and treatment with exogenous kisspeptins restores normal hormone secretion from the HPG axis [65].
Eating disorders are a cause of hypothalamic amenorrhea, and studies have shown an association between kisspeptins and energy reserves [67]. Specifically, food deprivation in rats led to a reduction in KISS1, KISS1 mRNA, and GnRH levels, which was reversed with food intake. KISS1 and KISS1 mRNA are expressed in various brain regions, including those that regulate food intake, though kisspeptin administration has no direct effect on appetite [66]. To maintain energy balance, energy intake must be equal to or exceed energy expenditure. Chronic negative energy balance (intake lower than expenditure) leads to infertility, as observed in animal models [68].
Administration of KP54 (37 µg/kg) subcutaneously twice daily for two weeks was studied in five women with hypothalamic amenorrhea. After the first dose of KP54, gonadotropin levels significantly increased, but by the 14th day of KP54 administration, the increase was noticeably diminished [65]. This observation is attributed to desensitization of the hypothalamus with daily KP54 administration. Estrogen levels remained consistent, and ultrasound findings did not indicate folliculogenesis. Based on these findings, the possibility of long-term kisspeptin administration was considered as a potential treatment for hormone-dependent tumors, due to its ability to suppress sex steroid hormone secretion [69], and for metastatic tumors [70].
In 2010, Jayasena et al. investigated the response and the degree of desensitization in women with hypothalamic amenorrhea to KP54 (37 µg/kg) when administered subcutaneously, twice weekly, for 8 weeks [10]. In this case, women exhibited an increase in gonadotropins from the first dose, with a comparable increase observed by the 14th day. The response to KP54 and gonadotropin levels remained consistent after 8 weeks. KP54 administration twice weekly resulted in a lower degree of desensitization compared to twice-daily administration, but it did not restore menstruation in women with hypothalamic amenorrhea.

4.8. Male Factor Infertility

Although the central role of kisspeptins in the hypothalamus is well established, their peripheral role in the testes remains unclear. Several studies have confirmed the expression of KISS1/KISS1R and Kiss1/Kiss1r in the male reproductive system in both human and animal models [19,71]. Specifically, they are expressed in Sertoli cells, spermatocytes, spermatids, and spermatozoa, indicating a potential autocrine or paracrine role in spermatogenesis in animal models [72]. In humans, the presence of KISS1/KISS1R has been identified in the tail, head, and neck of spermatozoa, suggesting a possible direct role in male fertility [73].
Men with infertility issues have been found to exhibit reduced kisspeptin levels in serum, likely due to dysregulation of the HPG axis. Sperm quality does not demonstrate a correlation with serum kisspeptin levels, whereas a correlation is observed with kisspeptin levels in semen [74]. A large cohort study conducted in China observed that kisspeptin levels in semen were 60,000 times higher than in serum, with a positive correlation between semen quality and kisspeptin levels in semen [75]. Due to this positive correlation with total sperm count and motility, it has been suggested that kisspeptins may contribute to spermatogenesis. In fact, a study on a fish species demonstrated that subcutaneous administration of kisspeptins accelerated spermatogenesis as a result of stimulating GnRH secretion [76]. Although the action of kisspeptins appears to mediate through the HPG axis, the expression of KISS1/KISS1R in the testes cannot exclude a direct effect on the testes [77].
Leydig cells in the testes are stimulated by LH to produce testosterone. Various studies have evaluated testosterone production in the testes following exogenous administration of kisspeptins and, despite the fact that male gonads express the KISS1R receptor, steroidogenesis appears unaffected. In contrast, a recent study provided in vivo evidence of increased testosterone levels following exogenous kisspeptin administration, after prior treatment with a GnRH antagonist (Acyline) in primates to exclude pituitary influence [78]. The GnRH antagonist inhibits LH secretion from the pituitary, indicating a direct action of kisspeptin on the male gonads.

5. Therapeutic Use of Kisspeptins

The most commonly used forms of kisspeptins in studies are KP10 and KP54. Their clinical utility is limited by their short duration of action and the need for parenteral administration. The half-life of KP10 is approximately 4 min in humans, while KP54 has a longer half-life of around 28 min. Bolus infusion of KP54 stimulates gonadotropin secretion in healthy women during the follicular phase, an effect not observed with bolus infusion of KP10 [79]. Additionally, intravenous administration of KP54 leads to a higher increase in LH levels compared to KP10 in healthy men [80,81]. KP10, due to its shorter amino acid sequence, is less expensive to produce than KP54 but exhibits greater biological instability [82].
Numerous studies have been conducted aiming to explore the potential therapeutic use of kisspeptins in patients with infertility. The pivotal role of kisspeptins in the onset of puberty and ovulation has led to the consideration of stimulating the HPG axis by exogenous kisspeptin administration. Although many factors have the ability to stimulate the HPG axis, kisspeptins appear to have advantages over these alternatives. The ability of kisspeptins to directly stimulate GnRH secretion from the hypothalamus enables their use for assessing hypothalamic function. Patients with iHH show a weaker response to kisspeptin administration compared to healthy individuals, as confirmed by two separate studies. In one study, patients with congenital hypogonadotropic hypogonadism exhibited a weaker response to KP54 administration compared to healthy men, and in another study, patients with iHH also showed a reduced response to KP10 compared to the control group [80,83]. The hypothalamic function test with KP10/KP54 can be used for the differential diagnosis between hypogonadotropic hypogonadism and delayed puberty [84].
One therapeutic application of kisspeptins is in functional gonadal disorders such as hypothalamic amenorrhea, hyperprolactinemia, and obesity-related hypogonadism. These clinical conditions are associated with kisspeptin deficiency. Age-related hypogonadism also appears to respond to the therapeutic use of KP54 [85].
A second therapeutic indication for the administration of kisspeptins is the pulsatile release of GnRH that they induce. Subcutaneous bolus administration of KP54 in healthy women during the follicular phase causes pulsatile LH secretion [86]. It is possible that women suffering from infertility due to insufficient GnRH secretion may be able to restore pulsatile LH secretion through kisspeptin therapy, thereby regaining their fertility.
Finally, due to the important role that kisspeptins play in the process of ovulation, their potential use for inducing ovulation in women undergoing IVF cycles has been studied. This application is particularly promising for women at high risk for OHSS. For this reason, more studies are being conducted to assess the safety and efficacy of ovulation induction with kisspeptins, compared to the currently used ovulation stimulants.
The first study involving the administration of kisspeptins in humans was conducted to investigate their potential therapeutic ability in infertile individuals and the effects of chronic administration [69,87]. The results showed an increase in gonadotropin levels in short-term therapeutic protocols, while repeated doses led to the phenomenon of tachyphylaxis (desensitization), making their therapeutic use ambiguous [87]. Chronic administration of kisspeptins, whether continuous or in repeated doses, may lead to reduced gonadotropin and sex steroid hormone levels [87]. This phenomenon has been observed in humans and animal models, regardless of the route of administration (intravenous, subcutaneous) [87]. While desensitization is undesirable in women with infertility, chronic use to suppress the HPG axis may be used therapeutically in hormone-dependent tumors, such as prostate cancer [87].

5.1. Triggering Ovulation

Healthy women participated in a study that observed a dose-dependent increase in LH levels after administration of KP54 [88]. The LH surge varied depending on the day of the cycle when KP54 was administered [88]. Specifically, higher LH levels were observed pre-ovulatory, sparking interest in investigating its potential use as an ovulation trigger [88].
The first trial of KP54 for ovulation induction was conducted in 2014 in women undergoing IVF [89]. The LH peak reached its maximum approximately 5 h after KP54 administration and lasted for 12–15 h, with most women having at least one mature oocyte retrieved [89]. This study demonstrated the effective use of KP54 for triggering ovulation [89].
LH levels after KP54 administration rise to levels observed in a natural mid-cycle LH surge (approximately 45 IU/L and 56.5 IU/L, respectively) [82,89], in contrast to the very high levels observed after GnRH agonist stimulation (approximately 140 IU/L) [90]. Notably, although KP54 induces a smaller increase in LH than the GnRH agonist, it achieves the same result in oocyte maturation [90]. This is attributed to the direct action of kisspeptins on KISS1R, which are expressed in the ovaries [39,91].
Due to the shorter duration of the LH surge following KP54 administration [92], a study was conducted in which a second dose of KP54 was administered 10 h after the first dose to examine whether a longer-lasting LH surge could be achieved. It was found that the group receiving two doses of KP54 had more mature oocytes retrieved compared to the group receiving a single dose [93].
Recently, MVT-602 (also known as TAK-448), a kisspeptin receptor agonist derived from the modification of KP10, has been studied. It exhibits a stronger pharmacodynamic effect than natural KP54 and increases LH levels, with a prolonged duration of action (21–22 h vs. 4.7 h, respectively) [13].
In 2024, a study including two randomized clinical trials was published investigating the endocrine profile of MVT-602 in healthy premenopausal women in follicular phase with and without ovarian stimulation [94]. The trials were placebo-controlled, parallel-group, and dose-ranging, showing that the LH surge induced by MVT-602 more accurately reflects the physiological midcycle LH surge that any current trigger agents. More precisely, intermediate dose of MVT-602 (1.0mg) produced the highest levels of LH concentrations with longer duration in comparison to native KP54, despite having similar elimination of half-lives, closely resembling the triphasic pattern of the physiological midcycle LH surge.

5.2. Ovarian Hyperstimulation Syndrome (OHSS)

A randomized controlled trial (RCT) investigated the possibility of preventing OHSS in women at high risk for the syndrome during ovulation induction with KP54 [92,95]. No women exhibited symptoms of moderate or severe OHSS, even in the study where a second dose of KP54 was administered [92,93]. The use of KP54 for ovulation induction is associated with a 33.6-fold reduced risk of severe OHSS compared to induction with rhCG [95]. Kisspeptin’s ability to prevent the onset of OHSS seems to be due to its short duration of action, and it is hypothesized that its direct action on ovarian KISS1R inhibits VEGF secretion, thereby reducing the incidence of OHSS [70,92].
In a retrospective study conducted in the United Kingdom, data were presented on OHSS cases in high-risk women following ovulation induction with rhCG, GnRH agonist, and kisspeptins [96]. OHSS was more significantly associated with the use of rhCG and GnRH agonist as ovulation triggers, in comparison to kisspeptin [96]. Additionally, the symptoms of OHSS caused by kisspeptin administration were milder than those caused by the other agents [96]. Finally, ovarian volume increased twentyfold compared to pre-induction volume in cases induced with synthetic hCG, eightfold with GnRH agonist, and fivefold with kisspeptin [96].

5.3. In Vitro Maturation (IVM)

For oocyte maturation, various growth factors are essential, such as GDF9, BMP15, and Kit, which are responsible for folliculogenesis, ovulation, and luteinization of the follicle [97]. The administration of KP10 has been shown to increase the expression of these growth factors. Studies have been conducted on the IVM of oocytes with KP10 administration in animal models but not yet in human oocytes [90,97].
In a recent study, the action of MVT-602, an agonist of the KISS1R receptor, was examined in cell lines, and signaling similar to that of KP54 in humans was observed [13]. There are future prospects for the use of KP54 and MVT-602 in the IVM of human oocytes but more studies are needed to establish safety of usage [13].

5.4. Cryopreservation

In recent years, the use of kisspeptins as antioxidant agents has been studied, as well as their effect on the expression of factors related to normal ovarian development. A study observed that the number of primary and secondary follicles in the group that underwent vitrification of ovarian tissue with kisspeptins was greater than that found in the group vitrified with other cryoprotective agents [11].
Furthermore, the level of apoptosis, the total antioxidant capacity (TAC) of the plasma, and the levels of superoxide dismutase (SOD) were examined in a further study by the same research group [12]. It was found that tissues that underwent vitrification with kisspeptins had the level of cell apoptosis reduced, while TAC and SOD were increased compared to the control group [12].
Various growth factors from the TGF-β family, specifically GDF9 and BMP15, are involved in paracrine signaling between the oocyte and the surrounding granulosa cells and play a significant role in oocyte maturation [98,99]. Several studies in the literature have investigated the expression of these factors in the ovaries of experimental animals and presented data showing reduced expression of GDF9 and BMP15 after cryopreservation and subsequent warming [98,99]. In a later study comparing classical vitrification with vitrification using kisspeptins, increased expression of GDF9 and BMP15 was observed in the vitrified samples with kisspeptins compared to the control group [97].
Based on studies in the literature, it appears that cryopreservation using the vitrification method and the use of kisspeptins as cryoprotectants may reduce the negative effects of cryopreservation by decreasing the generation of oxidative stress and apoptotic processes in the cell [11,12].

6. Conclusions

The literature review demonstrates the crucial role of kisspeptins in the onset of puberty, regulation of ovarian reserve, steroidogenesis, and ovulation. Mutations in the gene encoding kisspeptins or their receptor led to infertility. The kisspeptin system with the HPG axis in females has been elucidated, while their precise contribution to the male reproductive system remains unclear [22,74]. Further research is needed to clarify their role in steroidogenesis and their effect on male sperm quality [74].
The future use of kisspeptins may support differential diagnosis of delayed puberty [86], as well as offer treatment options for reversible infertility linked to their signaling pathways. For example, cases of central etiology infertility appear to respond to the administration of kisspeptin agonists, activating the HPG axis [65]. Although the physiology and pharmacokinetics of kisspeptins have been studied in recent years, the necessary therapeutic dosage and appropriate administration frequency are being tested in experimental studies and have not been established yet [65].
Additionally, kisspeptins are expressed in multiple tissues, including the endometrium. In women with endometriosis, the expression of the KISS1 gene in the endometrium is lower compared to that in ectopically implanted tissue [59]. However, one study disagreed with this observation, as KISS1 expression was not detected in any samples from women with or without endometriosis, likely due to methodological differences between the studies [56].
The hormonal response to the exogenous administration of kisspeptins in infertile women resembles the response observed in fertile women, due to endogenous kisspeptins and their signaling [90]. The administration of KP54 during the ovarian phase induces the pulsatile secretion of GnRH, resulting in an LH peak that reaches levels comparable to the mid-cycle peak seen in women with normal menstruation and ovulation [86,89]. Cases of infertility resulting from dysfunction in the kisspeptin system may potentially be treated in the future with kisspeptin analogs, which are considered safe for administration, and their use is being studied in central etiology infertility [80].
However, chronic administration of kisspeptins, as reported by Jayasena et al. [65], leads to desensitization of the axis, thus necessitating further research to determine therapeutic dosages. While desensitization of the gonadal axis is not desirable in infertility contexts, it may be therapeutic in hormone-dependent pathological entities or metastatic tumors, as it inhibits the production and secretion of sex steroid hormones [69,70].
Kisspeptins have potential applications in inducing ovulation, cryopreservation, and IVM of oocytes during IVF, as mentioned above [14]. The primary advantage of kisspeptin analogs is their short action on LH receptors, making them safer for inducing ovulation compared to rhCG, which is currently used [96]. Studies suggest that replacing rhCG with kisspeptins could reduce the incidence of OHSS [95]. However, their use remains experimental, with phase 1–2 trials currently underway examining the safety and efficacy of kisspeptin administration.
Considering the potential advantages of therapies including kisspeptins, it is important to study the benefits over current treatment options. Kisspeptins seem to stimulate a more physiological release of gonadotropins due to the endogenous pituitary release of GnRH they exert. As a result, kisspeptins may induce a more natural pattern of hormonal secretion rather than exogenous administration, reducing the possibilities of OHSS as revealed by clinical trials so far [100].
In conclusion, elucidating the action of kisspeptins provides a novel approach to regulating the HPG axis using kisspeptin analogs. Research conducted so far indicates that their administration is safe; however, further studies are necessary to determine their safety, side effects, and long-term effects in humans.

Author Contributions

Conceptualization, S.K. and N.N.; writing—original draft preparation, S.K.; writing—review and editing, N.K., P.T. and A.T.-K.; supervision, K.N. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

Not applicable.

Informed Consent Statement

This is a review, so no subjects were involved in the study.

Data Availability Statement

This is a review, and all the data are published and cited in the text.

Conflicts of Interest

The authors declare no conflicts of interest.

References

  1. Zegers-Hochschild, F.; Nygren, K.-G.; Adamson, G.D.; De Mouzon, J.; Lancaster, P.; Mansour, R.; Sullivan, E. The International Committee Monitoring Assisted Reproductive Technologies (ICMART) glossary on ART terminology. Fertil. Steril. 2006, 86, 16–19. [Google Scholar] [CrossRef] [PubMed]
  2. Njagi, P.; Groot, W.; Arsenijevic, J.; Dyer, S.; Mburu, G.; Kiarie, J. Financial costs of assisted reproductive technology for patients in low- and middle-income countries: A systematic review. Hum. Reprod. Open 2023, 2023, hoad007. [Google Scholar] [CrossRef] [PubMed]
  3. Seminara, S.B.; Messager, S.; Chatzidaki, E.E.; Thresher, R.R.; Acierno, J.S.; Shagoury, J.K.; Bo-Abbas, Y.; Kuohung, W.; Schwinof, K.M.; Hendrick, A.G.; et al. The GPR54 Gene as a Regulator of Puberty. N. Engl. J. Med. 2003, 349, 1614–1627. [Google Scholar] [CrossRef]
  4. Panidis, D.; Rousso, D.; Koliakos, G.; Kourtis, A.; Katsikis, I.; Farmakiotis, D.; Votsi, E.; Diamanti-Kandarakis, E. Plasma metastin levels are negatively correlated with insulin resistance and free androgens in women with polycystic ovary syndrome. Fertil. Steril. 2006, 85, 1778–1783. [Google Scholar] [CrossRef] [PubMed]
  5. Liu, X.; Brown, R.S.E.; Herbison, A.E.; Grattan, D.R. Lactational Anovulation in Mice Results From a Selective Loss of Kisspeptin Input to GnRH Neurons. Endocrinology 2014, 155, 193–203. [Google Scholar] [CrossRef]
  6. Irwig, M.S.; Fraley, G.S.; Smith, J.T.; Acohido, B.V.; Popa, S.M.; Cunningham, M.J.; Gottsch, M.L.; Clifton, D.K.; Steiner, R.A. Kisspeptin Activation of Gonadotropin Releasing Hormone Neurons and Regulation of KiSS-1 mRNA in the Male Rat. Neuroendocrinology 2004, 80, 264–272. [Google Scholar] [CrossRef]
  7. Lee, E.B.; Dilower, I.; Marsh, C.A.; Wolfe, M.W.; Masumi, S.; Upadhyaya, S.; Rumi, M.A.K. Sexual Dimorphism in Kisspeptin Signaling. Cells 2022, 11, 1146. [Google Scholar] [CrossRef]
  8. Sonigo, C.; Bouilly, J.; Carré, N.; Tolle, V.; Caraty, A.; Tello, J.; Simony-Conesa, F.-J.; Millar, R.; Young, J.; Binart, N. Hyperprolactinemia-induced ovarian acyclicity is reversed by kisspeptin administration. J. Clin. Investig. 2012, 122, 3791–3795. [Google Scholar] [CrossRef]
  9. Calik-Ksepka, A.; Stradczuk, M.; Czarnecka, K.; Grymowicz, M.; Smolarczyk, R. Lactational Amenorrhea: Neuroendocrine Pathways Controlling Fertility and Bone Turnover. Int. J. Mol. Sci. 2022, 23, 1633. [Google Scholar] [CrossRef]
  10. Jayasena, C.N.; Nijher, G.M.K.; Abbara, A.; Murphy, K.G.; Lim, A.; Patel, D.; Mehta, A.; Todd, C.; Donaldson, M.; Trew, G.H.; et al. Twice-Weekly Administration of Kisspeptin-54 for 8 Weeks Stimulates Release of Reproductive Hormones in Women With Hypothalamic Amenorrhea. Clin. Pharmacol. Ther. 2010, 88, 840–847. [Google Scholar] [CrossRef]
  11. Tavakoli, A.; Azar, A.T.; Taghizabet, N.; Rezaei-Tazangi, F.; Ardebili, S.N.; Mofarahe, Z.S.; Aliakbari, F.; Mehranjani, M.S. The effect of kisspeptin on the maturation of human ovarian follicles in culture following vitrification-thawing processes. JBRA Assist. Reprod. 2023, 27, 668–676. [Google Scholar] [CrossRef] [PubMed]
  12. Tavakoli, A.; Aliakbari, F.; Mehranjani, M.S. Kisspeptin decreases the adverse effects of human ovarian vitrification by regulating ROS-related apoptotic occurrences. Zygote 2023, 31, 537–543. [Google Scholar] [CrossRef] [PubMed]
  13. Abbara, A.; Eng, P.C.; Phylactou, M.; Clarke, S.A.; Richardson, R.; Sykes, C.M.; Phumsatitpong, C.; Mills, E.; Modi, M.; Izzi-Engbeaya, C.; et al. Kisspeptin receptor agonist has therapeutic potential for female reproductive disorders. J. Clin. Investig. 2020, 130, 6739–6753. [Google Scholar] [CrossRef] [PubMed]
  14. Patel, B.; Koysombat, K.; Mills, E.G.; Tsoutsouki, J.; Comninos, A.N.; Abbara, A.; Dhillo, W.S. The Emerging Therapeutic Potential of Kisspeptin and Neurokinin B. Endocr. Rev. 2023, 45, 30–68. [Google Scholar] [CrossRef]
  15. Roseweir, A.K.; Millar, R.P. The role of kisspeptin in the control of gonadotrophin secretion. Hum. Reprod. Update 2009, 15, 203–212. [Google Scholar] [CrossRef]
  16. Tng, E.L. Kisspeptin signalling and its roles in humans. Singapore Med. J. 2015, 56, 649–656. [Google Scholar] [CrossRef]
  17. Lee, J.H.; Welch, D.R. Suppression of metastasis in human breast carcinoma MDA-MB-435 cells after transfection with the metastasis suppressor gene, KiSS-1. Cancer Res. 1997, 57, 2384–2387. [Google Scholar]
  18. Masui, T.; Doi, R.; Mori, T.; Toyoda, E.; Koizumi, M.; Kami, K.; Ito, D.; Peiper, S.C.; Broach, J.R.; Oishi, S.; et al. Metastin and its variant forms suppress migration of pancreatic cancer cells. Biochem. Biophys. Res. Commun. 2004, 315, 85–92. [Google Scholar] [CrossRef]
  19. Ohtaki, T.; Shintani, Y.; Honda, S.; Matsumoto, H.; Hori, A.; Kanehashi, K.; Terao, Y.; Kumano, S.; Takatsu, Y.; Masuda, Y.; et al. Metastasis suppressor gene KiSS-1 encodes peptide ligand of a G-protein-coupled receptor. Nature 2001, 411, 613–617. [Google Scholar] [CrossRef]
  20. de Roux, N.; Genin, E.; Carel, J.-C.; Matsuda, F.; Chaussain, J.-L.; Milgrom, E. Hypogonadotropic hypogonadism due to loss of function of the KiSS1-derived peptide receptor GPR54. Proc. Natl. Acad. Sci. USA 2003, 100, 10972–10976. [Google Scholar] [CrossRef]
  21. Ruiz-Cruz, M.; Torres-Granados, C.; Tena-Sempere, M.; Roa, J. Central and peripheral mechanisms involved in the control of GnRH neuronal function by metabolic factors. Curr. Opin. Pharmacol. 2023, 71, 102382. [Google Scholar] [CrossRef] [PubMed]
  22. Pinilla, L.; Aguilar, E.; Dieguez, C.; Millar, R.P.; Tena-Sempere, M. Kisspeptins and Reproduction: Physiological Roles and Regulatory Mechanisms. Physiol. Rev. 2012, 92, 1235–1316. [Google Scholar] [CrossRef] [PubMed]
  23. Prashar, V.; Arora, T.; Singh, R.; Sharma, A.; Parkash, J. Hypothalamic Kisspeptin Neurons: Integral Elements of the GnRH System. Reprod. Sci. 2023, 30, 802–822. [Google Scholar] [CrossRef]
  24. Lin, X.-H.; Lass, G.; Kong, L.-S.; Wang, H.; Li, X.-F.; Huang, H.-F.; O’Byrne, K.T. Optogenetic Activation of Arcuate Kisspeptin Neurons Generates a Luteinizing Hormone Surge-Like Secretion in an Estradiol-Dependent Manner. Front. Endocrinol. 2021, 12, 775233. [Google Scholar] [CrossRef]
  25. Yeo, S.-H.; Colledge, W.H. The Role of Kiss1 Neurons As Integrators of Endocrine, Metabolic, and Environmental Factors in the Hypothalamic–Pituitary–Gonadal Axis. Front. Endocrinol. 2018, 9, 188. [Google Scholar] [CrossRef]
  26. Roa, J.; Castellano, J.M.; Navarro, V.M.; Handelsman, D.J.; Pinilla, L.; Tena-Sempere, M. Kisspeptins and the control of gonadotropin secretion in male and female rodents. Peptides 2009, 30, 57–66. [Google Scholar] [CrossRef]
  27. Lehman, M.N.; Coolen, L.M.; Goodman, R.L. Minireview: Kisspeptin/neurokinin B/dynorphin (KNDy) cells of the arcuate nucleus: A central node in the control of gonadotropin-releasing hormone secretion. Endocrinology 2010, 151, 3479–3489. [Google Scholar] [CrossRef]
  28. Topaloglu, A.K.; Reimann, F.; Guclu, M.; Yalin, A.S.; Kotan, L.D.; Porter, K.M.; Serin, A.; Mungan, N.O.; Cook, J.R.; Imamoglu, S.; et al. TAC3 and TACR3 Mutations in Familial Hypogonadotropic Hypogonadism Reveal a Key Role for Neurokinin B in the Central Control of Reproduction. Nat. Genet. 2009, 41, 354–358. [Google Scholar] [CrossRef]
  29. Merhi, Z.; Bazzi, A.A.; Bonney, E.A.; Buyuk, E. Role of adiponectin in ovarian follicular development and ovarian reserve. Biomed. Rep. 2019, 10, 337–342. [Google Scholar] [CrossRef]
  30. Zegers-Hochschild, F.; Adamson, G.D.; Dyer, S.; Racowsky, C.; de Mouzon, J.; Sokol, R.; Rienzi, L.; Sunde, A.; Schmidt, L.; Cooke, I.D.; et al. The International Glossary on Infertility and Fertility Care, 2017. Hum. Reprod. 2017, 32, 1786–1801. [Google Scholar] [CrossRef]
  31. Chan, Y.M.; Broder-Fingert, S.; Wong, K.M.; Seminara, S.B. Kisspeptin/Gpr54-independent gonadotrophin-releasing hormone activity in Kiss1 and Gpr54 mutant mice. J. Neuroendocrinol. 2009, 21, 1015–1023. [Google Scholar] [CrossRef] [PubMed]
  32. d’Anglemont de Tassigny, X.; Fagg, L.A.; Dixon, J.P.C.; Day, K.; Leitch, H.G.; Hendrick, A.G.; Zahn, D.; Franceschini, I.; Caraty, A.; Carlton, M.B.L.; et al. Hypogonadotropic hypogonadism in mice lacking a functional Kiss1 gene. Proc. Natl. Acad. Sci. USA 2007, 104, 10714–10719. [Google Scholar] [CrossRef] [PubMed]
  33. Hu, K.-L.; Zhao, H.; Chang, H.-M.; Yu, Y.; Qiao, J. Kisspeptin/Kisspeptin Receptor System in the Ovary. Front. Endocrinol. 2018, 8, 365. [Google Scholar] [CrossRef] [PubMed]
  34. Jayasena, C.N.; Dhillo, W.S. Kisspeptin offers a novel therapeutic target in reproduction. Curr. Opin. Investig. Drugs Lond. Engl. 2000 2009, 10, 311–318. [Google Scholar]
  35. Pineda, R.; Garcia-Galiano, D.; Roseweir, A.; Romero, M.; Sanchez-Garrido, M.A.; Ruiz-Pino, F.; Morgan, K.; Pinilla, L.; Millar, R.P.; Tena-Sempere, M. Critical Roles of Kisspeptins in Female Puberty and Preovulatory Gonadotropin Surges as Revealed by a Novel Antagonist. Endocrinology 2010, 151, 722–730. [Google Scholar] [CrossRef]
  36. Guerriero, K.A.; Keen, K.L.; Millar, R.P.; Terasawa, E. Developmental Changes in GnRH Release in Response to Kisspeptin Agonist and Antagonist in Female Rhesus Monkeys (Macaca mulatta): Implication for the Mechanism of Puberty. Endocrinology 2012, 153, 825–836. [Google Scholar] [CrossRef]
  37. Capozzi, A.; Scambia, G.; Pontecorvi, A.; Lello, S. Hyperprolactinemia: Pathophysiology and therapeutic approach. Gynecol. Endocrinol. 2015, 31, 506–510. [Google Scholar] [CrossRef]
  38. Millar, R.P.; Sonigo, C.; Anderson, R.A.; George, J.; Maione, L.; Brailly-Tabard, S.; Chanson, P.; Binart, N.; Young, J. Hypothalamic-Pituitary-Ovarian Axis Reactivation by Kisspeptin-10 in Hyperprolactinemic Women with Chronic Amenorrhea. J. Endocr. Soc. 2017, 1, 1362–1371. [Google Scholar] [CrossRef]
  39. Ruohonen, S.T.; Poutanen, M.; Tena-Sempere, M. Role of kisspeptins in the control of the hypothalamic-pituitary-ovarian axis: Old dogmas and new challenges. Fertil. Steril. 2020, 114, 465–474. [Google Scholar] [CrossRef]
  40. Ricu, M.A.; Ramirez, V.D.; Paredes, A.H.; Lara, H.E. Evidence for a Celiac Ganglion-Ovarian Kisspeptin Neural Network in the Rat: Intraovarian Anti-Kisspeptin Delays Vaginal Opening and Alters Estrous Cyclicity. Endocrinology 2012, 153, 4966–4977. [Google Scholar] [CrossRef]
  41. Mondal, M.; Baruah, K.K.; Prakash, B.S. Determination of plasma kisspeptin concentrations during reproductive cycle and different phases of pregnancy in crossbred cows using bovine specific enzyme immunoassay. Gen. Comp. Endocrinol. 2015, 224, 168–175. [Google Scholar] [CrossRef] [PubMed]
  42. Mondal, M.; Karunakaran, M.; Baruah, K.K. Development and Validation of a Sensitive Enzymeimmunoassay for Determination of Plasma Metastin in Mithun (Bos frontalis ). J. Immunoass. Immunochem. 2016, 37, 201–216. [Google Scholar] [CrossRef] [PubMed]
  43. Yilmaz, S.A.; Kerimoglu, O.S.; Pekin, A.T.; Incesu, F.; Dogan, N.U.; Celik, C.; Unlu, A. Metastin levels in relation with hormonal and metabolic profile in patients with polycystic ovary syndrome. Eur. J. Obstet. Gynecol. Reprod. Biol. 2014, 180, 56–60. [Google Scholar] [CrossRef] [PubMed]
  44. Chen, X.; Mo, Y.; Li, L.; Chen, Y.; Li, Y.; Yang, D. Increased plasma metastin levels in adolescent women with polycystic ovary syndrome. Eur. J. Obstet. Gynecol. Reprod. Biol. 2010, 149, 72–76. [Google Scholar] [CrossRef]
  45. Pérez-López, F.R.; Ornat, L.; López-Baena, M.T.; Santabárbara, J.; Savirón-Cornudella, R.; Pérez-Roncero, G.R. Circulating kisspeptin and anti-müllerian hormone levels, and insulin resistance in women with polycystic ovary syndrome: A systematic review, meta-analysis, and meta-regression. Eur. J. Obstet. Gynecol. Reprod. Biol. 2021, 260, 85–98. [Google Scholar] [CrossRef]
  46. Tang, R.; Ding, X.; Zhu, J. Kisspeptin and Polycystic Ovary Syndrome. Front. Endocrinol. 2019, 10, 298. [Google Scholar] [CrossRef]
  47. Albalawi, F.S.; Daghestani, M.H.; Daghestani, M.H.; Eldali, A.; Warsy, A.S. rs4889 polymorphism in KISS1 gene, its effect on polycystic ovary syndrome development and anthropometric and hormonal parameters in Saudi women. J. Biomed. Sci. 2018, 25, 50. [Google Scholar] [CrossRef]
  48. Emekci Ozay, O.; Ozay, A.C.; Acar, B.; Cagliyan, E.; Seçil, M.; Küme, T. Role of kisspeptin in polycystic ovary syndrome (PCOS). Gynecol. Endocrinol. 2016, 32, 718–722. [Google Scholar] [CrossRef]
  49. Nikolettos, K.; Vlahos, N.; Pagonopoulou, O.; Nikolettos, N.; Zikopoulos, K.; Tsikouras, P.; Kontomanolis, E.; Damaskos, C.; Garmpis, N.; Asimakopoulos, B. Is There an Association Between Circulating Kisspeptin Levels and Ovarian Reserve in Women of Reproductive Age? In Vivo 2023, 37, 2219–2223. [Google Scholar] [CrossRef]
  50. Nyagolova, P.V.; Mitkov, M.D.; Orbetzova, M.M.; Terzieva, D.D. Kisspeptin and Galanin-like Peptide (GALP) Levels in Women with Polycystic Ovary Syndrome. Int. J. Pharmaceut. Med. Res. 2016, 4, 7–12. [Google Scholar]
  51. Jeon, Y.E.; Lee, K.E.; Jung, J.A.; Yim, S.Y.; Kim, H.; Seo, S.K.; Cho, S.; Choi, Y.S.; Lee, B.S. Kisspeptin, Leptin, and Retinol-Binding Protein 4 in Women with Polycystic Ovary Syndrome. Gynecol. Obstet. Investig. 2013, 75, 268–274. [Google Scholar] [CrossRef] [PubMed]
  52. Katulski, K.; Podfigurna, A.; Czyzyk, A.; Meczekalski, B.; Genazzani, A.D. Kisspeptin and LH pulsatile temporal coupling in PCOS patients. Endocrine 2018, 61, 149–157. [Google Scholar] [CrossRef] [PubMed]
  53. Collette, T. Evidence for an increased release of proteolytic activity by the eutopic endometrial tissue in women with endometriosis and for involvement of matrix metalloproteinase-9. Hum. Reprod. 2004, 19, 1257–1264. [Google Scholar] [CrossRef]
  54. Collette, T.; Maheux, R.; Mailloux, J.; Akoum, A. Increased expression of matrix metalloproteinase-9 in the eutopic endometrial tissue of women with endometriosis. Hum. Reprod. 2006, 21, 3059–3067. [Google Scholar] [CrossRef]
  55. Di Carlo, C.; Bonifacio, M.; Tommaselli, G.A.; Bifulco, G.; Guerra, G.; Nappi, C. Metalloproteinases, vascular endothelial growth factor, and angiopoietin 1 and 2 in eutopic and ectopic endometrium. Fertil. Steril. 2009, 91, 2315–2323. [Google Scholar] [CrossRef]
  56. Makri, A.; Msaouel, P.; Petraki, C.; Milingos, D.; Protopapas, A.; Liapi, A.; Antsaklis, A.; Magkou, C.; Koutsilieris, M. KISS1/KISS1R Expression in Eutopic and Ectopic Endometrium of Women Suffering from Endometriosis. In Vivo 2012, 26, 119–127. [Google Scholar]
  57. Kleimenova, T.; Polyakova, V.; Linkova, N.; Drobintseva, A.; Medvedev, D.; Krasichkov, A. The Expression of Kisspeptins and Matrix Metalloproteinases in Extragenital Endometriosis. Biomedicines 2024, 12, 94. [Google Scholar] [CrossRef]
  58. Abdelkareem, A.O.; Alotaibi, F.T.; AlKusayer, G.M.; Ait-Allah, A.S.; Rasheed, S.M.; Helmy, Y.A.; Allaire, C.; Peng, B.; Yong, P.J.; Bedaiwy, M.A. Immunoreactivity of Kisspeptin and Kisspeptin Receptor in Eutopic and Ectopic Endometrial Tissue of Women With and Without Endometriosis. Reprod. Sci. 2020, 27, 1731–1741. [Google Scholar] [CrossRef]
  59. Timologou, A.; Zafrakas, M.; Grimbizis, G.; Miliaras, D.; Kotronis, K.; Stamatopoulos, P.; Tarlatzis, B.C. Immunohistochemical expression pattern of metastasis suppressors KAI1 and KISS1 in endometriosis and normal endometrium. Eur. J. Obstet. Gynecol. Reprod. Biol. 2016, 199, 110–115. [Google Scholar] [CrossRef]
  60. Önal, M.; Karli, P.; Özdemir, A.Z.; Kocaman, A.; Katirci, Y.; Çoban, G.; Nakişli, G.K.; Civil, Y.; Avci, B. Serum kisspeptin levels in deep-infiltrating, ovarian, and superficial endometriosis: A prospective observational study. Medicine 2022, 101, e31529. [Google Scholar] [CrossRef]
  61. Akad, M.; Socolov, D.; Akad, F.; Covali, R.; Crauciuc, E.; Stan, C.; Stan, C.; Socolov, R. Treatments in Patients with Polycystic Ovary Syndrome and Effects on Kisspeptin Serum Levels. Maedica 2022, 17, 799–804. [Google Scholar] [CrossRef] [PubMed]
  62. Kaya, C.; Alay, İ.; Babayeva, G.; Gedikbaşı, A.; Ertaş Kaya, S.; Ekin, M.; Yaşar, L. Serum Kisspeptin levels in unexplained infertility, polycystic ovary syndrome, and male factor infertility. Gynecol. Endocrinol. Off. J. Int. Soc. Gynecol. Endocrinol. 2019, 35, 228–232. [Google Scholar] [CrossRef] [PubMed]
  63. Mumtaz, A.; Khalid, A.; Jamil, Z.; Fatima, S.S.; Arif, S.; Rehman, R. Kisspeptin: A Potential Factor for Unexplained Infertility and Impaired Embryo Implantation. Int. J. Fertil. Steril. 2017, 11, 99–104. [Google Scholar] [CrossRef] [PubMed]
  64. Podfigurna, A.; Szeliga, A.; Meczekalski, B. Serum kisspeptin and corticotropin-releasing hormone levels in patients with functional hypothalamic amenorrhea. Gynecol. Reprod. Endocrinol. Metab. 2020, 1, 37–42. [Google Scholar]
  65. Jayasena, C.N.; Nijher, G.M.K.; Chaudhri, O.B.; Murphy, K.G.; Ranger, A.; Lim, A.; Patel, D.; Mehta, A.; Todd, C.; Ramachandran, R.; et al. Subcutaneous Injection of Kisspeptin-54 Acutely Stimulates Gonadotropin Secretion in Women with Hypothalamic Amenorrhea, But Chronic Administration Causes Tachyphylaxis. J. Clin. Endocrinol. Metab. 2009, 94, 4315–4323. [Google Scholar] [CrossRef]
  66. Castellano, J.M.; Navarro, V.M.; Fernández-Fernández, R.; Nogueiras, R.; Tovar, S.; Roa, J.; Vazquez, M.J.; Vigo, E.; Casanueva, F.F.; Aguilar, E.; et al. Changes in Hypothalamic KiSS-1 System and Restoration of Pubertal Activation of the Reproductive Axis by Kisspeptin in Undernutrition. Endocrinology 2005, 146, 3917–3925. [Google Scholar] [CrossRef]
  67. Hudson, A.D.; Kauffman, A.S. Metabolic actions of kisspeptin signaling: Effects on body weight, energy expenditure, and feeding. Pharmacol. Ther. 2022, 231, 107974. [Google Scholar] [CrossRef]
  68. Thomas, G.B.; Mercer, J.E.; Karalis, T.; Rao, A.; Cummins, J.T.; Clarke, I.J. Effect of Restricted Feeding on the Concentrations of Growth Hormone (GH), Gonadotropins, and Prolactin (PRL) in Plasma, and on the Amounts of Messenger Ribonucleic Acid for GH, Gonadotropin Subunits, and PRL in the Pituitary Glands of Adult Ovariectomized Ewes. Endocrinology 1990, 126, 1361–1367. [Google Scholar] [CrossRef]
  69. Seminara, S.B.; Dipietro, M.J.; Ramaswamy, S.; Crowley, W.F.; Plant, T.M. Continuous human metastin 45-54 infusion desensitizes G protein-coupled receptor 54-induced gonadotropin-releasing hormone release monitored indirectly in the juvenile male Rhesus monkey (Macaca mulatta): A finding with therapeutic implications. Endocrinology 2006, 147, 2122–2126. [Google Scholar] [CrossRef]
  70. Zhai, J.; Liu, J.; Zhao, S.; Zhao, H.; Chen, Z.-J.; Du, Y.; Li, W. Kisspeptin-10 inhibits OHSS by suppressing VEGF secretion. Reproduction 2017, 154, 355–362. [Google Scholar] [CrossRef]
  71. Kotani, M.; Detheux, M.; Vandenbogaerde, A.; Communi, D.; Vanderwinden, J.-M.; Poul, E.L.; Brézillon, S.; Tyldesley, R.; Suarez-Huerta, N.; Vandeput, F.; et al. The Metastasis Suppressor Gene KiSS-1 Encodes Kisspeptins, the Natural Ligands of the Orphan G Protein-coupled Receptor GPR54. J. Biol. Chem. 2001, 276, 34631–34636. [Google Scholar] [CrossRef] [PubMed]
  72. Wahab, F.; Atika, B.; Shahab, M.; Behr, R. Kisspeptin signalling in the physiology and pathophysiology of the urogenital system. Nat. Rev. Urol. 2016, 13, 21–32. [Google Scholar] [CrossRef] [PubMed]
  73. Pinto, F.M.; Cejudo-Román, A.; Ravina, C.G.; Fernández-Sánchez, M.; Martín-Lozano, D.; Illanes, M.; Tena-Sempere, M.; Candenas, M.L. Characterization of the kisspeptin system in human spermatozoa. Int. J. Androl. 2012, 35, 63–73. [Google Scholar] [CrossRef]
  74. Ramzan, M.H.; Ramzan, M.; Ramzan, F.; Wahab, F.; Jelani, M.; Khan, M.A.; Shah, M. Insight into the serum kisspeptin levels in infertile males. Arch. Iran. Med. 2015, 18, 12–17. [Google Scholar]
  75. Zou, P.; Wang, X.; Chen, Q.; Yang, H.; Zhou, N.; Sun, L.; Chen, H.; Liu, J.; Ao, L.; Cui, Z.; et al. Kisspeptin Protein in Seminal Plasma Is Positively Associated with Semen Quality: Results from the MARHCS Study in Chongqing, China. BioMed Res. Int. 2019, 2019, 5129263. [Google Scholar] [CrossRef]
  76. Selvaraj, S.; Ohga, H.; Nyuji, M.; Kitano, H.; Nagano, N.; Yamaguchi, A.; Matsuyama, M. Subcutaneous administration of Kiss1 pentadecapeptide accelerates spermatogenesis in prepubertal male chub mackerel (Scomber japonicus). Comp. Biochem. Physiol. A. Mol. Integr. Physiol. 2013, 166, 228–236. [Google Scholar] [CrossRef]
  77. Mei, H.; Doran, J.; Kyle, V.; Yeo, S.-H.; Colledge, W.H. Does Kisspeptin Signaling have a Role in the Testes? Front. Endocrinol. 2013, 4, 198. [Google Scholar] [CrossRef]
  78. Irfan, S.; Ehmcke, J.; Wahab, F.; Shahab, M.; Schlatt, S. Intratesticular action of kisspeptin in rhesus monkey ( Macaca mulatta ). Andrologia 2014, 46, 610–617. [Google Scholar] [CrossRef]
  79. Jayasena, C.N.; Nijher, G.M.K.; Comninos, A.N.; Abbara, A.; Januszewki, A.; Vaal, M.L.; Sriskandarajah, L.; Murphy, K.G.; Farzad, Z.; Ghatei, M.A.; et al. The Effects of Kisspeptin-10 on Reproductive Hormone Release Show Sexual Dimorphism in Humans. J. Clin. Endocrinol. Metab. 2011, 96, E1963–E1972. [Google Scholar] [CrossRef]
  80. Abbara, A.; Eng, P.C.; Phylactou, M.; Clarke, S.A.; Mills, E.; Chia, G.; Yang, L.; Izzi-Engbeaya, C.; Smith, N.; Jayasena, C.N.; et al. Kisspeptin-54 Accurately Identifies Hypothalamic Gonadotropin-Releasing Hormone Neuronal Dysfunction in Men with Congenital Hypogonadotropic Hypogonadism. Neuroendocrinology 2021, 111, 1176–1186. [Google Scholar] [CrossRef]
  81. George, J.T.; Veldhuis, J.D.; Roseweir, A.K.; Newton, C.L.; Faccenda, E.; Millar, R.P.; Anderson, R.A. Kisspeptin-10 is a potent stimulator of LH and increases pulse frequency in men. J. Clin. Endocrinol. Metab. 2011, 96, E1228-36. [Google Scholar] [CrossRef] [PubMed]
  82. Cohlen, B.J.; te Velde, E.R.; Scheffer, G.; van Kooij, R.J.; Maria de Brouwer, C.P.; van Zonneveld, P. The pattern of the luteinizing hormone surge in spontaneous cycles is related to the probability of conception. Fertil. Steril. 1993, 60, 413–417. [Google Scholar] [CrossRef] [PubMed]
  83. Chan, Y.-M.; Lippincott, M.F.; Butler, J.P.; Sidhoum, V.F.; Li, C.X.; Plummer, L.; Seminara, S.B. Exogenous kisspeptin administration as a probe of GnRH neuronal function in patients with idiopathic hypogonadotropic hypogonadism. J. Clin. Endocrinol. Metab. 2014, 99, E2762–E2771. [Google Scholar] [CrossRef] [PubMed]
  84. Chan, Y.-M.; Lippincott, M.F.; Sales Barroso, P.; Alleyn, C.; Brodsky, J.; Granados, H.; Roberts, S.A.; Sandler, C.; Srivatsa, A.; Seminara, S.B. Using Kisspeptin to Predict Pubertal Outcomes for Youth With Pubertal Delay. J. Clin. Endocrinol. Metab. 2020, 105, e2717–e2725. [Google Scholar] [CrossRef]
  85. Abbara, A.; Narayanaswamy, S.; Izzi-Engbeaya, C.; Comninos, A.N.; Clarke, S.A.; Malik, Z.; Papadopoulou, D.; Clobentz, A.; Sarang, Z.; Bassett, P.; et al. Hypothalamic Response to Kisspeptin-54 and Pituitary Response to Gonadotropin-Releasing Hormone Are Preserved in Healthy Older Men. Neuroendocrinology 2018, 106, 401–410. [Google Scholar] [CrossRef]
  86. Jayasena, C.N.; Comninos, A.N.; Veldhuis, J.D.; Misra, S.; Abbara, A.; Izzi-Engbeaya, C.; Donaldson, M.; Ghatei, M.A.; Bloom, S.R.; Dhillo, W.S. A single injection of kisspeptin-54 temporarily increases luteinizing hormone pulsatility in healthy women. Clin. Endocrinol. 2013, 79, 558–563. [Google Scholar] [CrossRef]
  87. Abbara, A.; Ratnasabapathy, R.; Jayasena, C.N.; Dhillo, W.S. The effects of kisspeptin on gonadotropin release in non-human mammals. Adv. Exp. Med. Biol. 2013, 784, 63–87. [Google Scholar] [CrossRef]
  88. Dhillo, W.S.; Chaudhri, O.B.; Thompson, E.L.; Murphy, K.G.; Patterson, M.; Ramachandran, R.; Nijher, G.K.; Amber, V.; Kokkinos, A.; Donaldson, M.; et al. Kisspeptin-54 Stimulates Gonadotropin Release Most Potently during the Preovulatory Phase of the Menstrual Cycle in Women. J. Clin. Endocrinol. Metab. 2007, 92, 3958–3966. [Google Scholar] [CrossRef]
  89. Jayasena, C.N.; Abbara, A.; Comninos, A.N.; Nijher, G.M.K.; Christopoulos, G.; Narayanaswamy, S.; Izzi-Engbeaya, C.; Sridharan, M.; Mason, A.J.; Warwick, J.; et al. Kisspeptin-54 triggers egg maturation in women undergoing in vitro fertilization. J. Clin. Investig. 2014, 124, 3667–3677. [Google Scholar] [CrossRef]
  90. Abbara, A.; Clarke, S.A.; Dhillo, W.S. Novel Concepts for Inducing Final Oocyte Maturation in In Vitro Fertilization Treatment. Endocr. Rev. 2018, 39, 593–628. [Google Scholar] [CrossRef]
  91. Garcia-Ortega, J.; Pinto, F.M.; Fernandez-Sanchez, M.; Prados, N.; Cejudo-Roman, A.; Almeida, T.A.; Hernandez, M.; Romero, M.; Tena-Sempere, M.; Candenas, L. Expression of neurokinin B/NK3 receptor and kisspeptin/KISS1 receptor in human granulosa cells. Hum. Reprod. 2014, 29, 2736–2746. [Google Scholar] [CrossRef] [PubMed]
  92. Abbara, A.; Jayasena, C.N.; Christopoulos, G.; Narayanaswamy, S.; Izzi-Engbeaya, C.; Nijher, G.M.K.; Comninos, A.N.; Peters, D.; Buckley, A.; Ratnasabapathy, R.; et al. Efficacy of Kisspeptin-54 to Trigger Oocyte Maturation in Women at High Risk of Ovarian Hyperstimulation Syndrome (OHSS) During In Vitro Fertilization (IVF) Therapy. J. Clin. Endocrinol. Metab. 2015, 100, 3322–3331. [Google Scholar] [CrossRef]
  93. Abbara, A.; Clarke, S.; Islam, R.; Izzi-Engbeaya, C.; Ratnasabapathy, R.; Nesbitt, A.; Vimalesvaran, S.; Salim, R.; Lavery, S.A.; Bloom, S.R.; et al. A second dose of kisspeptin-54 improves oocyte maturation in women at high risk of ovarian hyperstimulation syndrome: A Phase 2 randomized controlled trial. Hum. Reprod. 2017, 32, 1915–1924. [Google Scholar] [CrossRef] [PubMed]
  94. Abbara, A.; Ufer, M.; Voors-Pette, C.; Berman, L.; Ezzati, M.; Wu, R.; Lee, T.-Y.; Ferreira, J.C.A.; Migoya, E.; Dhillo, W.S. Endocrine profile of the kisspeptin receptor agonist MVT-602 in healthy premenopausal women with and without ovarian stimulation: Results from 2 randomized, placebo-controlled clinical tricals. Fertil. Steril. 2024, 121, 95–106. [Google Scholar] [CrossRef] [PubMed]
  95. Abbara, A.; Islam, R.; Clarke, S.A.; Jeffers, L.; Christopoulos, G.; Comninos, A.N.; Salim, R.; Lavery, S.A.; Vuong, T.N.L.; Humaidan, P.; et al. Clinical parameters of ovarian hyperstimulation syndrome following different hormonal triggers of oocyte maturation in IVF treatment. Clin. Endocrinol. 2018, 88, 920–927. [Google Scholar] [CrossRef]
  96. Abbara, A.; Hunjan, T.; Ho, V.N.A.; Clarke, S.A.; Comninos, A.N.; Izzi-Engbeaya, C.; Ho, T.M.; Trew, G.H.; Hramyka, A.; Kelsey, T.; et al. Endocrine Requirements for Oocyte Maturation Following hCG, GnRH Agonist, and Kisspeptin During IVF Treatment. Front. Endocrinol. 2020, 11, 537205. [Google Scholar] [CrossRef]
  97. Saadeldin, I.M.; Koo, O.J.; Kang, J.T.; Kwon, D.K.; Park, S.J.; Kim, S.J.; Moon, J.H.; Oh, H.J.; Jang, G.; Lee, B.C. Paradoxical effects of kisspeptin: It enhances oocyte in vitro maturation but has an adverse impact on hatched blastocysts during in vitro culture. Reprod. Fertil. Dev. 2012, 24, 656–668. [Google Scholar] [CrossRef]
  98. Ebrahimi, B.; Valojerdi, M.R.; Eftekhari-Yazdi, P.; Baharvand, H.; Farrokhi, A. IVM and gene expression of sheep cumulus–oocyte complexes following different methods of vitrification. Reprod. Biomed. Online 2010, 20, 26–34. [Google Scholar] [CrossRef]
  99. Choi, J.; Lee, J.-Y.; Lee, E.; Yoon, B.-K.; Bae, D.; Choi, D. Cryopreservation of the mouse ovary inhibits the onset of primordial follicle development. Cryobiology 2007, 54, 55–62. [Google Scholar] [CrossRef]
  100. Hameed, S.; Jayasena, C.N.; Dhillo, W.S. Kisspeptin and fertility. J. Endocrinol. 2011, 208, 97–105. [Google Scholar] [CrossRef]
Disclaimer/Publisher’s Note: The statements, opinions and data contained in all publications are solely those of the individual author(s) and contributor(s) and not of MDPI and/or the editor(s). MDPI and/or the editor(s) disclaim responsibility for any injury to people or property resulting from any ideas, methods, instructions or products referred to in the content.

Share and Cite

MDPI and ACS Style

Kotanidou, S.; Nikolettos, N.; Kritsotaki, N.; Tsikouras, P.; Tiptiri-Kourpeti, A.; Nikolettos, K. Kisspeptins Regulating Fertility: Potential Future Therapeutic Approach in Infertility Treatment. J. Clin. Med. 2025, 14, 3284. https://doi.org/10.3390/jcm14103284

AMA Style

Kotanidou S, Nikolettos N, Kritsotaki N, Tsikouras P, Tiptiri-Kourpeti A, Nikolettos K. Kisspeptins Regulating Fertility: Potential Future Therapeutic Approach in Infertility Treatment. Journal of Clinical Medicine. 2025; 14(10):3284. https://doi.org/10.3390/jcm14103284

Chicago/Turabian Style

Kotanidou, Sonia, Nikos Nikolettos, Nektaria Kritsotaki, Panagiotis Tsikouras, Angeliki Tiptiri-Kourpeti, and Konstantinos Nikolettos. 2025. "Kisspeptins Regulating Fertility: Potential Future Therapeutic Approach in Infertility Treatment" Journal of Clinical Medicine 14, no. 10: 3284. https://doi.org/10.3390/jcm14103284

APA Style

Kotanidou, S., Nikolettos, N., Kritsotaki, N., Tsikouras, P., Tiptiri-Kourpeti, A., & Nikolettos, K. (2025). Kisspeptins Regulating Fertility: Potential Future Therapeutic Approach in Infertility Treatment. Journal of Clinical Medicine, 14(10), 3284. https://doi.org/10.3390/jcm14103284

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