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Replacement and Parallel Simplification of Nonhomologous Proteinases Maintain Venom Phenotypes in Rear-Fanged Snakes

机译:非同源蛋白酶的替代和平行简化维持了后牙蛇的毒液表型

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Novel phenotypes are commonly associated with gene duplications and neofunctionalization, less documented are the cases of phenotypic maintenance through the recruitment of novel genes. Proteolysis is the primary toxic character of many snake venoms, and ADAM metalloproteinases, named snake venom metalloproteinases (SVMPs), are largely recognized as the major effectors of this phenotype. However, by investigating original transcriptomes from 58 species of advanced snakes (Caenophidia) across their phylogeny, we discovered that a different enzyme, matrix metalloproteinase (MMP), is actually the dominant venom component in three tribes (Tachymenini, Xenodontini, and Conophiini) of rear-fanged snakes (Dipsadidae). Proteomic and functional analyses of these venoms further indicate that MMPs are likely playing an “SVMP-like” function in the proteolytic phenotype. A detailed look into the venom-specific sequences revealed a new highly expressed MMP subtype, named snake venom MMP (svMMP), which originated independently on at least three occasions from an endogenous MMP-9. We further show that by losing ancillary noncatalytic domains present in its ancestors, svMMPs followed an evolutionary path toward a simplified structure during their expansion in the genomes, thus paralleling what has been proposed for the evolution of their Viperidae counterparts, the SVMPs. Moreover, we inferred an inverse relationship between the expression of svMMPs and SVMPs along the evolutionary history of Xenodontinae, pointing out that one type of enzyme may be substituting for the other, whereas the general (metallo)proteolytic phenotype is maintained. These results provide rare evidence on how relevant phenotypic traits can be optimized via natural selection on nonhomologous genes, yielding alternate biochemical components.
机译:新表型通常与基因复制和新功能化有关,较少记录通过募集新基因来维持表型的情况。蛋白水解是许多蛇毒的主要毒性特征,而ADAM金属蛋白酶,称为蛇毒金属蛋白酶(SVMPs),在很大程度上被认为是这种表型的主要效应因子。然而,通过研究 58 种高级蛇 (Caenophidia) 在其系统发育中的原始转录组,我们发现一种不同的酶,基质金属蛋白酶 (MMP),实际上是后牙蛇 (Dipsadidae) 的三个部落(Tachymenini、Xenodontini 和 Conophiini)的主要毒液成分。这些毒液的蛋白质组学和功能分析进一步表明,MMP可能在蛋白水解表型中发挥“SVMP样”功能。对毒液特异性序列的详细研究揭示了一种新的高度表达的MMP亚型,称为蛇毒MMP(svMMP),它至少三次独立起源于内源性MMP-9。我们进一步表明,通过失去其祖先中存在的辅助非催化结构域,svMMPs在基因组中的扩展过程中遵循了一条简化结构的进化路径,从而与它们的Viperidae对应物SVMPs的进化提出了平行。此外,我们推断了svMMPs和SVMPs在异齿科进化史上的表达呈反比关系,指出一种酶可能取代了另一种酶,而一般的(金属)蛋白水解表型保持不变。这些结果提供了罕见的证据,说明如何通过对非同源基因的自然选择来优化相关表型性状,从而产生替代的生化成分。

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