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RNA 伴侣蛋白 Hfq 的 C 端结构域具有多种体内功能。

Multiple in vivo roles for the C-terminal domain of the RNA chaperone Hfq.

机构信息

Laboratory of Molecular Biology, National Cancer Institute, Bethesda, MD, USA.

Cell Biology and Metabolism Program, Eunice Kennedy Shriver National Institute of Child Health and Human Development, Bethesda, MD, USA.

出版信息

Nucleic Acids Res. 2022 Feb 22;50(3):1718-1733. doi: 10.1093/nar/gkac017.

Abstract

Hfq, a bacterial RNA chaperone, stabilizes small regulatory RNAs (sRNAs) and facilitates sRNA base-pairing with target mRNAs. Hfq has a conserved N-terminal domain and a poorly conserved disordered C-terminal domain (CTD). In a transcriptome-wide examination of the effects of a chromosomal CTD deletion (Hfq1-65), the Escherichia coli mutant was most defective for the accumulation of sRNAs that bind the proximal and distal faces of Hfq (Class II sRNAs), but other sRNAs also were affected. There were only modest effects on the levels of mRNAs, suggesting little disruption of sRNA-dependent regulation. However, cells expressing Hfq lacking the CTD in combination with a weak distal face mutation were defective for the function of the Class II sRNA ChiX and repression of mutS, both dependent upon distal face RNA binding. Loss of the region between amino acids 66-72 was critical for this defect. The CTD region beyond amino acid 72 was not necessary for distal face-dependent regulation, but was needed for functions associated with the Hfq rim, seen most clearly in combination with a rim mutant. Our results suggest that the C-terminus collaborates in various ways with different binding faces of Hfq, leading to distinct outcomes for individual sRNAs.

摘要

Hfq 是一种细菌 RNA 伴侣,可稳定小调控 RNA(sRNA)并促进 sRNA 与靶 mRNA 碱基配对。Hfq 具有保守的 N 端结构域和较差保守的无规卷曲 C 端结构域(CTD)。在对染色体 CTD 缺失(Hfq1-65)的全转录组影响进行检查时,大肠杆菌突变体在积累与 Hfq 近端和远端结合的 sRNA(II 类 sRNA)方面缺陷最大,但其他 sRNA 也受到影响。mRNA 水平的影响仅适度,表明 sRNA 依赖性调节的破坏很小。然而,表达缺乏 CTD 的 Hfq 与弱远端面突变的细胞在 ChiX 类 II sRNA 的功能和 mutS 的抑制方面存在缺陷,这两者都依赖于远端面 RNA 结合。缺失氨基酸 66-72 之间的区域对于该缺陷至关重要。氨基酸 72 以后的 CTD 区域对于远端面依赖性调节不是必需的,但对于与 Hfq 边缘相关的功能是必需的,在与边缘突变体结合时最为明显。我们的结果表明,C 端以各种方式与 Hfq 的不同结合面协作,导致不同的 sRNA 产生不同的结果。

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