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自毁的食欲:在非洲-亚洲眼镜蛇属蛇毒中探测猎物选择性结合的 α-神经毒素。

An Appetite for Destruction: Detecting Prey-Selective Binding of α-Neurotoxins in the Venom of Afro-Asian Elapids.

机构信息

Venom Evolution Lab, School of Biological Sciences, University of Queensland, St Lucia, QLD 4072, Australia.

QIMR Berghofer, Royal Brisbane Hospital, Brisbane, QLD 4029, Australia.

出版信息

Toxins (Basel). 2020 Mar 23;12(3):205. doi: 10.3390/toxins12030205.

Abstract

Prey-selective venoms and toxins have been documented across only a few species of snakes. The lack of research in this area has been due to the absence of suitably flexible testing platforms. In order to test more species for prey specificity of their venom, we used an innovative taxonomically flexible, high-throughput biolayer interferometry approach to ascertain the relative binding of 29 α-neurotoxic venoms from African and Asian elapid representatives (26 spp., , and four locales of ) to the alpha-1 nicotinic acetylcholine receptor orthosteric (active) site for amphibian, lizard, snake, bird, and rodent targets. Our results detected prey-selective, intraspecific, and geographical differences of α-neurotoxic binding. The results also suggest that crude venom that shows prey selectivity is likely driven by the proportions of prey-specific α-neurotoxins with differential selectivity within the crude venom. Our results also suggest that since the α-neurotoxic prey targeting does not always account for the full dietary breadth of a species, other toxin classes with a different pathophysiological function likely play an equally important role in prey immobilisation of the crude venom depending on the prey type envenomated. The use of this innovative and taxonomically flexible diverse assay in functional venom testing can be key in attempting to understanding the evolution and ecology of α-neurotoxic snake venoms, as well as opening up biochemical and pharmacological avenues to explore other venom effects.

摘要

猎物选择性毒液和毒素仅在少数几种蛇中得到记录。由于缺乏合适的灵活测试平台,该领域的研究一直很少。为了测试更多物种毒液对猎物的特异性,我们使用了一种创新的、分类学上灵活的高通量生物层干涉测量方法,以确定来自非洲和亚洲眼镜蛇代表(26 种,和四个地方)的 29 种α-神经毒素毒液对蛙类、蜥蜴、蛇、鸟类和啮齿动物靶标的α-1 烟碱型乙酰胆碱受体正位(活性)位点的相对结合。我们的研究结果检测到α-神经毒素结合的猎物选择性、种内和地理差异。研究结果还表明,表现出猎物选择性的粗毒液可能是由猎物特异性α-神经毒素的比例驱动的,这些毒素在粗毒液中具有不同的选择性。我们的研究结果还表明,由于α-神经毒素对猎物的靶向作用并不总是反映出一个物种的全部饮食范围,因此其他具有不同病理生理功能的毒素类可能在根据中毒的猎物类型,在粗毒液对猎物的固定中发挥同样重要的作用。这种创新的、分类学上灵活的多样化 assay 在功能毒液测试中的使用,可以帮助我们理解α-神经毒素蛇毒的进化和生态学,并为探索其他毒液作用开辟生化和药理学途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/349d/7150784/1e8d7a015c42/toxins-12-00205-g001.jpg

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