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An overview of Phoneutria nigriventer spider venom using combined transcriptomic and proteomic approaches

机译:转录组学和蛋白质组学方法相结合的黑腹Phoneutria蜘蛛毒概述

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摘要

Phoneutria nigriventer is one of the largest existing true spiders and one of the few considered medically relevant. Its venom contains several neurotoxic peptides that act on different ion channels and chemical receptors of vertebrates and invertebrates. Some of these venom toxins have been shown as promising models for pharmaceutical or biotechnological use. However, the large diversity and the predominance of low molecular weight toxins in this venom have hampered the identification and deep investigation of the less abundant toxins and the proteins with high molecular weight. Here, we combined conventional and next-generation cDNA sequencing with Multidimensional Protein Identification Technology (MudPIT), to obtain an in-depth panorama of the composition of P. nigriventer spider venom. The results from these three approaches showed that cysteine-rich peptide toxins are the most abundant components in this venom and most of them contain the Inhibitor Cysteine Knot (ICK) structural motif. Ninety-eight sequences corresponding to cysteine-rich peptide toxins were identified by the three methodologies and many of them were considered as putative novel toxins, due to the low similarity to previously described toxins. Furthermore, using next-generation sequencing we identified families of several other classes of toxins, including CAPs (Cysteine Rich Secretory Protein—CRiSP, antigen 5 and Pathogenesis-Related 1—PR-1), serine proteinases, TCTPs (translationally controlled tumor proteins), proteinase inhibitors, metalloproteinases and hyaluronidases, which have been poorly described for this venom. This study provides an overview of the molecular diversity of P. nigriventer venom, revealing several novel components and providing a better basis to understand its toxicity and pharmacological activities.
机译:Phoneutria nigriventer是现存最大的真蜘蛛之一,也是少数被认为与医学相关的蜘蛛之一。它的毒液包含几种神经毒性肽,它们作用于脊椎动物和无脊椎动物的不同离子通道和化学受体。这些毒液毒素中的一些已被证明是用于药物或生物技术用途的有前途的模型。然而,这种毒液中低分子量毒素的广泛多样性和优势阻碍了对含量较低的毒素和高分子量蛋白的鉴定和深入研究。在这里,我们将常规和下一代cDNA测序与多维蛋白质识别技术(MudPIT)结合在一起,以深入了解黑腹果蝇蜘蛛毒液的组成。这三种方法的结果表明,富含半胱氨酸的肽毒素是该毒液中最丰富的成分,并且大多数含有抑制剂半胱氨酸结(ICK)结构基序。通过三种方法鉴定了与富含半胱氨酸的肽毒素相对应的九十八个序列,由于与前述毒素的相似性低,其中许多被认为是推定的新型毒素。此外,使用下一代测序技术,我们鉴定了其他几种毒素家族,包括CAP(半胱氨酸富含分泌蛋白CRiSP,抗原5和与发病相关的1-PR-1),丝氨酸蛋白酶,TCTP(翻译控制的肿瘤蛋白) ,蛋白酶抑制剂,金属蛋白酶和透明质酸酶,对此毒液的描述很少。这项研究概述了黑腹果蝇毒液的分子多样性,揭示了几种新型成分,并为了解其毒性和药理活性提供了更好的基础。

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