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端粒长度调控和端粒染色质需要无义介导的mRNA降解途径。

Telomere length regulation and telomeric chromatin require the nonsense-mediated mRNA decay pathway.

作者信息

Lew J E, Enomoto S, Berman J

机构信息

Department of Plant Biology and Plant Molecular Genetics Institute, University of Minnesota, St. Paul, Minnesota 55108, USA.

出版信息

Mol Cell Biol. 1998 Oct;18(10):6121-30. doi: 10.1128/MCB.18.10.6121.

Abstract

Rap1p localization factor 4 (RLF4) is a Saccharomyces cerevisiae gene that was identified in a screen for mutants that affect telomere function and alter the localization of the telomere binding protein Rap1p. In rlf4 mutants, telomeric silencing is reduced and telomere DNA tracts are shorter, indicating that RLF4 is required for both the establishment and/or maintenance of telomeric chromatin and for the control of telomere length. In this paper, we demonstrate that RLF4 is allelic to NMD2/UPF2, a gene required for the nonsense-mediated mRNA decay (NMD) pathway (Y. Cui, K. W. Hagan, S. Zhang, and S. W. Peltz, Mol. Cell. Biol. 9:423-436, 1995, and F. He and A. Jacobson, Genes Dev. 9:437-454, 1995). The NMD pathway, which requires Nmd2p/Rlf4p together with two other proteins, (Upf1p and Upf3p), targets nonsense messages for degradation in the cytoplasm by the exoribonuclease Xrn1p. Deletion of UPF1 and UPF3 caused telomere-associated defects like those caused by rlf4 mutations, implying that the NMD pathway, rather than an NMD-independent function of Nmd2p/Rlf4p, is required for telomere functions. In addition, telomere length regulation required Xrn1p but not Rat1p, a nuclear exoribonuclease with functional similarity to Xrn1p (A. W. Johnson, Mol. Cell. Biol. 17:6122-6130, 1997). In contrast, telomere-associated defects were not observed in pan2, pan3, or pan2 pan3 strains, which are defective in the intrinsic deadenylation-dependent decay of normal (as opposed to nonsense) mRNAs. Thus, loss of the NMD pathway specifically causes defects at telomeres, demonstrating a physiological requirement for the NMD pathway in normal cell functions. We propose a model in which the NMD pathway regulates the levels of specific mRNAs that are important for telomere functions.

摘要

Rap1p定位因子4(RLF4)是酿酒酵母中的一个基因,它是在一项针对影响端粒功能并改变端粒结合蛋白Rap1p定位的突变体筛选中被鉴定出来的。在rlf4突变体中,端粒沉默作用减弱,端粒DNA序列变短,这表明RLF4对于端粒染色质的建立和/或维持以及端粒长度的控制都是必需的。在本文中,我们证明RLF4与NMD2/UPF2等位,NMD2/UPF2是无义介导的mRNA降解(NMD)途径所必需的一个基因(Y. Cui、K. W. Hagan、S. Zhang和S. W. Peltz,《分子细胞生物学》9:423 - 436,1995年;以及F. He和A. Jacobson,《基因与发育》9:437 - 454,1995年)。NMD途径需要Nmd2p/Rlf4p以及另外两种蛋白质(Upf1p和Upf3p),它通过外切核糖核酸酶Xrn1p将无义信息靶向到细胞质中进行降解。UPF1和UPF3的缺失会导致与rlf4突变所引起的类似的端粒相关缺陷,这意味着端粒功能需要NMD途径,而不是Nmd2p/Rlf4p的不依赖NMD的功能。此外,端粒长度调控需要Xrn1p而不是Rat1p,Rat1p是一种与Xrn1p功能相似的核外切核糖核酸酶(A. W. Johnson,《分子细胞生物学》17:6122 - 6130,1997年)。相比之下,在pan2、pan3或pan2 pan3菌株中未观察到端粒相关缺陷,这些菌株在正常(而非无义)mRNA的内在依赖去腺苷酸化的降解过程中存在缺陷。因此,NMD途径的缺失会特异性地导致端粒缺陷,这表明NMD途径在正常细胞功能中具有生理需求。我们提出了一个模型,其中NMD途径调节对端粒功能很重要的特定mRNA的水平。

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