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Authors = Shunyi Zhu

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SHUNYI (6) , ZHU (1727)

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Open AccessArticle Exon Shuffling and Origin of Scorpion Venom Biodiversity
Toxins 2017, 9(1), 10; doi:10.3390/toxins9010010
Received: 26 July 2016 / Revised: 13 December 2016 / Accepted: 21 December 2016 / Published: 26 December 2016
Cited by 1 | Viewed by 621 | PDF Full-text (1760 KB) | HTML Full-text | XML Full-text | Supplementary Files
Abstract
Scorpion venom is a complex combinatorial library of peptides and proteins with multiple biological functions. A combination of transcriptomic and proteomic techniques has revealed its enormous molecular diversity, as identified by the presence of a large number of ion channel-targeted neurotoxins with different
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Scorpion venom is a complex combinatorial library of peptides and proteins with multiple biological functions. A combination of transcriptomic and proteomic techniques has revealed its enormous molecular diversity, as identified by the presence of a large number of ion channel-targeted neurotoxins with different folds, membrane-active antimicrobial peptides, proteases, and protease inhibitors. Although the biodiversity of scorpion venom has long been known, how it arises remains unsolved. In this work, we analyzed the exon-intron structures of an array of scorpion venom protein-encoding genes and unexpectedly found that nearly all of these genes possess a phase-1 intron (one intron located between the first and second nucleotides of a codon) near the cleavage site of a signal sequence despite their mature peptides remarkably differ. This observation matches a theory of exon shuffling in the origin of new genes and suggests that recruitment of different folds into scorpion venom might be achieved via shuffling between body protein-coding genes and ancestral venom gland-specific genes that presumably contributed tissue-specific regulatory elements and secretory signal sequences. Full article
(This article belongs to the collection Evolution of Venom Systems)
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Open AccessReview The Fungal Defensin Family Enlarged
Pharmaceuticals 2014, 7(8), 866-880; doi:10.3390/ph7080866
Received: 5 June 2014 / Revised: 5 August 2014 / Accepted: 8 August 2014 / Published: 18 August 2014
Cited by 5 | Viewed by 1724 | PDF Full-text (4030 KB) | HTML Full-text | XML Full-text | Supplementary Files
Abstract
Fungi are an emerging source of peptide antibiotics. With the availability of a large number of model fungal genome sequences, we can expect that more and more fungal defensin-like peptides (fDLPs) will be discovered by sequence similarity search. Here, we report a total
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Fungi are an emerging source of peptide antibiotics. With the availability of a large number of model fungal genome sequences, we can expect that more and more fungal defensin-like peptides (fDLPs) will be discovered by sequence similarity search. Here, we report a total of 69 new fDLPs encoded by 63 genes, in which a group of fDLPs derived from dermatophytes are defined as a new family (fDEF8) according to sequence and phylogenetic analyses. In the oleaginous fungus Mortierella alpine, fDLPs have undergone extensive gene expansion. Our work further enlarges the fungal defensin family and will help characterize new peptide antibiotics with therapeutic potential. Full article

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