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Phylogenetic profiles reveal structural/functional determinants of TRPC3 signal-sensing antennae

机译:系统发生谱揭示了TRPC3信号感应天线的结构/功能决定因素

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摘要

Biochemical assessment of channel structure/function is incredibly challenging. Developing computational tools that provide these data would enable translational research, accelerating mechanistic experimentation for the bench scientist studying ion channels. Starting with the premise that protein sequence encodes information about structure, function and evolution (SF&E), we developed a unified framework for inferring SF&E from sequence information using a knowledge-based approach. The Gestalt Domain Detection Algorithm-Basic Local Alignment Tool (GDDA-BLAST) provides phylogenetic profiles that can model, ab initio, SF&E relationships of biological sequences at the whole protein, single domain and single-amino acid level., In our recent paper, we have applied GDDA-BLAST analysis to study canonical TRP (TRPC) channels and empirically validated predicted lipid-binding and trafficking activities contained within the TRPC3 TRP_2 domain of unknown function. Overall, our in silico, in vitro, and in vivo experiments support a model in which TRPC3 has signal-sensing antennae which are adorned with lipid-binding, trafficking and calmodulin regulatory domains. In this Addendum, we correlate our functional domain analysis with the cryo-EM structure of TRPC3. In addition, we synthesize recent studies with our new findings to provide a refined model on the mechanism(s) of TRPC3 activation/deactivation.
机译:通道结构/功能的生化评估极具挑战性。开发提供这些数据的计算工具将使翻译研究成为可能,并加快了研究离子通道的台式科学家的机械实验速度。从蛋白质序列编码有关结构,功能和进化(SF&E)信息的前提开始,我们开发了一个统一的框架,用于使用基于知识的方法从序列信息推断SF&E。完形结构域检测算法-基本局部比对工具(GDDA-BLAST)提供了系统发育概况,可在整个蛋白质,单个域和单个氨基酸水平上模拟,从头算,生物学序列的SF&E关系。 在我们最近的论文中, 我们已经应用GDDA-BLAST分析来研究典型的TRP(TRPC)通道 并通过经验验证了未知功能的TRPC3 TRP_2域中包含的预测脂质结合和运输活动。总体而言,我们的计算机模拟,体外和体内实验均支持TRPC3具有信号感应触角的模型,该触角被脂质结合,运输和钙调蛋白调节域修饰。在此附录中,我们将功能域分析与TRPC3的cryo-EM结构相关联。 此外,我们将最新研究与新发现进行了综合,以提供关于TRPC3机理的精确模型。激活/停用。

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