Discovery of a Distinct Superfamily of Kunitz-Type Toxin (KTT) from Tarantulas

BACKGROUND: Kuntiz-type toxins (KTTs) have been found in the venom of animals such as snake, cone snail and sea anemone. The main ancestral function of Kunitz-type proteins was the inhibition of a diverse array of serine proteases, while toxic activities (such as ion-channel blocking) were developed...

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Autores principales: Yuan, Chun-Hua, He, Quan-Yuan, Peng, Kuan, Diao, Jian-Bo, Jiang, Li-Ping, Tang, Xing, Liang, Song-Ping
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2008
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2561067/
https://www.ncbi.nlm.nih.gov/pubmed/18923708
http://dx.doi.org/10.1371/journal.pone.0003414
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author Yuan, Chun-Hua
He, Quan-Yuan
Peng, Kuan
Diao, Jian-Bo
Jiang, Li-Ping
Tang, Xing
Liang, Song-Ping
author_facet Yuan, Chun-Hua
He, Quan-Yuan
Peng, Kuan
Diao, Jian-Bo
Jiang, Li-Ping
Tang, Xing
Liang, Song-Ping
author_sort Yuan, Chun-Hua
collection PubMed
description BACKGROUND: Kuntiz-type toxins (KTTs) have been found in the venom of animals such as snake, cone snail and sea anemone. The main ancestral function of Kunitz-type proteins was the inhibition of a diverse array of serine proteases, while toxic activities (such as ion-channel blocking) were developed under a variety of Darwinian selection pressures. How new functions were grafted onto an old protein scaffold and what effect Darwinian selection pressures had on KTT evolution remains a puzzle. PRINCIPAL FINDINGS: Here we report the presence of a new superfamily of KTTs in spiders (Tarantulas: Ornithoctonus huwena and Ornithoctonus hainana), which share low sequence similarity to known KTTs and is clustered in a distinct clade in the phylogenetic tree of KTT evolution. The representative molecule of spider KTTs, HWTX-XI, purified from the venom of O. huwena, is a bi-functional protein which is a very potent trypsin inhibitor (about 30-fold more strong than BPTI) as well as a weak Kv1.1 potassium channel blocker. Structural analysis of HWTX-XI in 3-D by NMR together with comparative function analysis of 18 expressed mutants of this toxin revealed two separate sites, corresponding to these two activities, located on the two ends of the cone-shape molecule of HWTX-XI. Comparison of non-synonymous/synonymous mutation ratios (ω) for each site in spider and snake KTTs, as well as PBTI like body Kunitz proteins revealed high Darwinian selection pressure on the binding sites for Kv channels and serine proteases in snake, while only on the proteases in spider and none detected in body proteins, suggesting different rates and patterns of evolution among them. The results also revealed a series of key events in the history of spider KTT evolution, including the formation of a novel KTT family (named sub-Kuntiz-type toxins) derived from the ancestral native KTTs with the loss of the second disulfide bridge accompanied by several dramatic sequence modifications. CONCLUSIONS/SIGNIFICANCE: These finding illustrate that the two activity sites of Kunitz-type toxins are functionally and evolutionally independent and provide new insights into effects of Darwinian selection pressures on KTT evolution, and mechanisms by which new functions can be grafted onto old protein scaffolds.
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spelling pubmed-25610672008-10-15 Discovery of a Distinct Superfamily of Kunitz-Type Toxin (KTT) from Tarantulas Yuan, Chun-Hua He, Quan-Yuan Peng, Kuan Diao, Jian-Bo Jiang, Li-Ping Tang, Xing Liang, Song-Ping PLoS One Research Article BACKGROUND: Kuntiz-type toxins (KTTs) have been found in the venom of animals such as snake, cone snail and sea anemone. The main ancestral function of Kunitz-type proteins was the inhibition of a diverse array of serine proteases, while toxic activities (such as ion-channel blocking) were developed under a variety of Darwinian selection pressures. How new functions were grafted onto an old protein scaffold and what effect Darwinian selection pressures had on KTT evolution remains a puzzle. PRINCIPAL FINDINGS: Here we report the presence of a new superfamily of KTTs in spiders (Tarantulas: Ornithoctonus huwena and Ornithoctonus hainana), which share low sequence similarity to known KTTs and is clustered in a distinct clade in the phylogenetic tree of KTT evolution. The representative molecule of spider KTTs, HWTX-XI, purified from the venom of O. huwena, is a bi-functional protein which is a very potent trypsin inhibitor (about 30-fold more strong than BPTI) as well as a weak Kv1.1 potassium channel blocker. Structural analysis of HWTX-XI in 3-D by NMR together with comparative function analysis of 18 expressed mutants of this toxin revealed two separate sites, corresponding to these two activities, located on the two ends of the cone-shape molecule of HWTX-XI. Comparison of non-synonymous/synonymous mutation ratios (ω) for each site in spider and snake KTTs, as well as PBTI like body Kunitz proteins revealed high Darwinian selection pressure on the binding sites for Kv channels and serine proteases in snake, while only on the proteases in spider and none detected in body proteins, suggesting different rates and patterns of evolution among them. The results also revealed a series of key events in the history of spider KTT evolution, including the formation of a novel KTT family (named sub-Kuntiz-type toxins) derived from the ancestral native KTTs with the loss of the second disulfide bridge accompanied by several dramatic sequence modifications. CONCLUSIONS/SIGNIFICANCE: These finding illustrate that the two activity sites of Kunitz-type toxins are functionally and evolutionally independent and provide new insights into effects of Darwinian selection pressures on KTT evolution, and mechanisms by which new functions can be grafted onto old protein scaffolds. Public Library of Science 2008-10-15 /pmc/articles/PMC2561067/ /pubmed/18923708 http://dx.doi.org/10.1371/journal.pone.0003414 Text en Yuan et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Yuan, Chun-Hua
He, Quan-Yuan
Peng, Kuan
Diao, Jian-Bo
Jiang, Li-Ping
Tang, Xing
Liang, Song-Ping
Discovery of a Distinct Superfamily of Kunitz-Type Toxin (KTT) from Tarantulas
title Discovery of a Distinct Superfamily of Kunitz-Type Toxin (KTT) from Tarantulas
title_full Discovery of a Distinct Superfamily of Kunitz-Type Toxin (KTT) from Tarantulas
title_fullStr Discovery of a Distinct Superfamily of Kunitz-Type Toxin (KTT) from Tarantulas
title_full_unstemmed Discovery of a Distinct Superfamily of Kunitz-Type Toxin (KTT) from Tarantulas
title_short Discovery of a Distinct Superfamily of Kunitz-Type Toxin (KTT) from Tarantulas
title_sort discovery of a distinct superfamily of kunitz-type toxin (ktt) from tarantulas
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2561067/
https://www.ncbi.nlm.nih.gov/pubmed/18923708
http://dx.doi.org/10.1371/journal.pone.0003414
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