Department of Genetics and Cell Physiology, Faculty of Biological Sciences, University of Wroclaw, 50-328 Wroclaw, Poland.
Institute of Genetics and Development of Rennes, CNRS UMR 6290, University of Rennes 1, 35000 Rennes, France.
Cells. 2023 Jan 27;12(3):419. doi: 10.3390/cells12030419.
Up-frameshift protein 1 (UPF1) plays the role of a vital controller for transcripts, ready to react in the event of an incorrect translation mechanism. It is well known as one of the key elements involved in mRNA decay pathways and participates in transcript and protein quality control in several different aspects. Firstly, UPF1 specifically degrades premature termination codon (PTC)-containing products in a nonsense-mediated mRNA decay (NMD)-coupled manner. Additionally, UPF1 can potentially act as an E3 ligase and degrade target proteins independently from mRNA decay pathways. Thus, UPF1 protects cells against the accumulation of misfolded polypeptides. However, this multitasking protein may still hide many of its functions and abilities. In this article, we summarize important discoveries in the context of UPF1, its involvement in various cellular pathways, as well as its structural importance and mutational changes related to the emergence of various pathologies and disease states. Even though the state of knowledge about this protein has significantly increased over the years, there are still many intriguing aspects that remain unresolved.
上移框移蛋白 1(UPF1)在转录物中起着至关重要的控制器的作用,随时准备在翻译机制出错时做出反应。它是参与 mRNA 衰变途径的关键因素之一,并在多个不同方面参与转录物和蛋白质的质量控制。首先,UPF1 特异性地降解含有提前终止密码子(PTC)的产物,以非终止介导的 mRNA 衰变(NMD)偶联方式。此外,UPF1 可以作为 E3 连接酶,独立于 mRNA 衰变途径降解靶蛋白。因此,UPF1 可防止细胞中错误折叠的多肽积累。然而,这种多功能蛋白可能仍隐藏着许多其功能和能力。在本文中,我们总结了 UPF1 背景下的重要发现,包括其在各种细胞途径中的参与,以及其结构重要性和与各种病理和疾病状态出现相关的突变变化。尽管多年来对这种蛋白质的了解有了显著提高,但仍有许多有趣的方面尚未解决。
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