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高度易变的连接区调节 HIV-1 Rev 功能和稳定性。

Highly Mutable Linker Regions Regulate HIV-1 Rev Function and Stability.

机构信息

Department of Biochemistry and Biophysics, University of California San Francisco, San Francisco, CA, 94158, USA.

UCSC Genomics Institute/Howard Hughes Medical Institute, University of Santa Cruz, Santa Cruz, CA, 95060, USA.

出版信息

Sci Rep. 2019 Mar 26;9(1):5139. doi: 10.1038/s41598-019-41582-7.

Abstract

HIV-1 Rev is an essential viral regulatory protein that facilitates the nuclear export of intron-containing viral mRNAs. It is organized into structured, functionally well-characterized motifs joined by less understood linker regions. Our recent competitive deep mutational scanning study confirmed many known constraints in Rev's established motifs, but also identified positions of mutational plasticity, most notably in surrounding linker regions. Here, we probe the mutational limits of these linkers by testing the activities of multiple truncation and mass substitution mutations. We find that these regions possess previously unknown structural, functional or regulatory roles, not apparent from systematic point mutational approaches. Specifically, the N- and C-termini of Rev contribute to protein stability; mutations in a turn that connects the two main helices of Rev have different effects in different contexts; and a linker region which connects the second helix of Rev to its nuclear export sequence has structural requirements for function. Thus, Rev function extends beyond its characterized motifs, and is tuned by determinants within seemingly plastic portions of its sequence. Additionally, Rev's ability to tolerate many of these massive truncations and substitutions illustrates the overall mutational and functional robustness inherent in this viral protein.

摘要

HIV-1 Rev 是一种重要的病毒调节蛋白,可促进包含内含子的病毒 mRNA 的核输出。它由结构上组织良好、功能特征明确的基序组成,由不太了解的连接区连接。我们最近的竞争性深度突变扫描研究证实了 Rev 已建立基序中的许多已知约束,但也确定了突变可塑性的位置,尤其是在周围的连接区。在这里,我们通过测试多个截断和质量取代突变的活性来探测这些接头的突变极限。我们发现,这些区域具有以前未知的结构、功能或调节作用,这在系统的点突变方法中并不明显。具体来说,Rev 的 N 端和 C 端有助于蛋白质稳定性;连接 Rev 两个主要螺旋的转角中的突变在不同的上下文中具有不同的影响;连接 Rev 第二螺旋与其核输出序列的连接区具有结构要求的功能。因此,Rev 的功能超出了其特征性基序的范围,并由其序列中看似具有可塑性的部分中的决定因素进行调整。此外,Rev 能够耐受许多这些大规模的截断和取代,说明了该病毒蛋白固有的整体突变和功能稳健性。

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