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细胞质蛋白酶体对于酿酒酵母的细胞生长并非不可或缺。

Cytoplasmic proteasomes are not indispensable for cell growth in Saccharomyces cerevisiae.

机构信息

Laboratory of Protein Metabolism, Tokyo Metropolitan Institute of Medical Science, Tokyo, Japan.

出版信息

Biochem Biophys Res Commun. 2013 Jul 5;436(3):372-6. doi: 10.1016/j.bbrc.2013.05.105. Epub 2013 Jun 4.

Abstract

The 26S proteasome is an essential protease complex responsible for the degradation of ubiquitinated proteins in eukaryotic cells. In rapidly proliferating yeast cells, proteasomes are mainly localized in the nucleus, but the biological significance of the proteasome localization is still unclear. In this study, we investigated the relationship between the proteasome localization and the functions by the anchor-away technique, a ligand-dependent sequestration of a target protein into specific compartment(s). Anchoring of the proteasome to the plasma membrane or the ribosome resulted in conditional depletion of the nuclear proteasomes, whereas anchoring to histone resulted in the proteasome sequestration into the nucleus. We observed that the accumulation of ubiquitinated proteins in all the proteasome-targeted cells, suggesting that both the nuclear and cytoplasmic proteasomes have proteolytic functions and that the ubiquitinated proteins are produced and degraded in each compartment. Consistent with previous studies, the nuclear proteasome-depleted cells exhibited a lethal phenotype. In contrast, the nuclear sequestration of the proteasome resulted only in a mild growth defect, suggesting that the cytoplasmic proteasomes are not basically indispensable for cell growth in rapidly growing yeast cells.

摘要

26S 蛋白酶体是一种负责降解真核细胞中泛素化蛋白的必需蛋白酶复合物。在快速增殖的酵母细胞中,蛋白酶体主要定位于细胞核,但蛋白酶体定位的生物学意义仍不清楚。在这项研究中,我们通过锚定技术(一种依赖配体将靶蛋白隔离到特定隔室的方法)研究了蛋白酶体定位与功能之间的关系。将蛋白酶体锚定到质膜或核糖体上会导致核蛋白酶体的条件性耗竭,而将蛋白酶体锚定到组蛋白上则会导致蛋白酶体被隔离到细胞核中。我们观察到所有靶向蛋白酶体的细胞中泛素化蛋白的积累,表明核蛋白酶体和细胞质蛋白酶体都具有蛋白水解功能,并且泛素化蛋白在每个隔室中产生和降解。与之前的研究一致,核蛋白酶体耗竭的细胞表现出致命表型。相比之下,蛋白酶体的核隔离仅导致轻微的生长缺陷,表明在快速生长的酵母细胞中,细胞质蛋白酶体对于细胞生长并非基本必需。

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