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真核生物蛋白结构域作为细胞进化的功能单元。

Eukaryotic protein domains as functional units of cellular evolution.

机构信息

Centre for Systems Biology, Samuel Lunenfeld Research Institute, Mount Sinai Hospital, Ontario, Canada.

出版信息

Sci Signal. 2009 Nov 24;2(98):ra76. doi: 10.1126/scisignal.2000546.

Abstract

Modular protein domains are functional units that can be modified through the acquisition of new intrinsic activities or by the formation of novel domain combinations, thereby contributing to the evolution of proteins with new biological properties. Here, we assign proteins to groups with related domain compositions and functional properties, termed "domain clubs," which we use to compare multiple eukaryotic proteomes. This analysis shows that different domain types can take distinct evolutionary trajectories, which correlate with the conservation, gain, expansion, or decay of particular biological processes. Evolutionary jumps are associated with a domain that coordinately acquires a new intrinsic function and enters new domain clubs, thereby providing the modified domain with access to a new cellular microenvironment. We also coordinately analyzed the covalent and noncovalent interactions of different domain types to assess the molecular compartment occupied by each domain. This reveals that specific subsets of domains demarcate particular cellular processes, such as growth factor signaling, chromatin remodeling, apoptotic and inflammatory responses, or vesicular trafficking. We suggest that domains, and the proteins in which they reside, are selected during evolution through reciprocal interactions with protein domains in their local microenvironment. Based on this scheme, we propose a mechanism by which Tudor domains may have evolved to support different modes of epigenetic regulation and suggest a role for the germline group of mammalian Tudor domains in Piwi-regulated RNA biology.

摘要

模块化蛋白质结构域是具有内在活性的功能单元,可通过获得新的固有活性或形成新的结构域组合进行修饰,从而有助于具有新生物学特性的蛋白质的进化。在这里,我们将具有相关结构域组成和功能特性的蛋白质分配到称为“结构域俱乐部”的组中,并用其来比较多个真核生物的蛋白质组。该分析表明,不同的结构域类型可以采取不同的进化轨迹,这些轨迹与特定生物学过程的保守性、获得、扩展或衰减相关。进化跳跃与协调地获得新的内在功能并进入新的结构域俱乐部的结构域有关,从而为修饰后的结构域提供了进入新的细胞微环境的途径。我们还协调地分析了不同结构域类型的共价和非共价相互作用,以评估每个结构域占据的分子区室。这表明,特定的结构域子集标记了特定的细胞过程,如生长因子信号、染色质重塑、细胞凋亡和炎症反应或小泡运输。我们认为,在进化过程中,通过与局部微环境中的蛋白质结构域的相互作用,选择了结构域及其所在的蛋白质。基于该方案,我们提出了一种机制,说明 tudor 结构域可能是如何进化为支持不同的表观遗传调控模式的,并提出了哺乳动物 tudor 结构域的种系群在 piwi 调控的 RNA 生物学中的作用。

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