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Cwc23,一种必需的 J 蛋白,对于前体 mRNA 剪接至关重要,但具有非必需的 J 结构域。

Cwc23, an essential J protein critical for pre-mRNA splicing with a dispensable J domain.

机构信息

Department of Biochemistry, 433 Babcock Dr., University of Wisconsin-Madison, Madison, WI 53706, USA.

出版信息

Mol Cell Biol. 2010 Jan;30(1):33-42. doi: 10.1128/MCB.00842-09.

Abstract

J proteins are structurally diverse, obligatory cochaperones of Hsp70s, each with a highly conserved J domain that plays a critical role in the stimulation of Hsp70's ATPase activity. The essential protein, Cwc23, is one of 13 J proteins found in the cytosol and/or nucleus of Saccharomyces cerevisiae. We report that a partial loss-of-function CWC23 mutant has severe, global defects in pre-mRNA splicing. This mutation leads to accumulation of the excised, lariat form of the intron, as well as unspliced pre-mRNA, suggesting a role for Cwc23 in spliceosome disassembly. Such a role is further supported by the observation that this mutation results in reduced interaction between Cwc23 and Ntr1 (SPP382), a known component of the disassembly pathway. However, Cwc23 is a very atypical J protein. Its J domain, although functional, is dispensable for both cell viability and pre-mRNA splicing. Nevertheless, strong genetic interactions were uncovered between point mutations encoding alterations in Cwc23's J domain and either Ntr1 or Prp43, a DExD/H-box helicase essential for spliceosome disassembly. These genetic interactions suggest that Hsp70-based chaperone machinery does play a role in the disassembly process. Cwc23 provides a unique example of a J protein; its partnership with Hsp70 plays an auxiliary, rather than a central, role in its essential cellular function.

摘要

J 蛋白结构多样,是 Hsp70 的必需共伴侣,每个 J 蛋白都有一个高度保守的 J 结构域,在刺激 Hsp70 的 ATP 酶活性方面发挥着关键作用。必需蛋白 Cwc23 是酿酒酵母细胞质和/或核中发现的 13 种 J 蛋白之一。我们报告说,部分功能丧失的 CWC23 突变体在前体 mRNA 剪接中存在严重的、全局性缺陷。这种突变导致内含子被切除的套索形式以及未剪接的前体 mRNA 积累,表明 Cwc23 在剪接体解体中发挥作用。这种作用进一步得到以下观察结果的支持:这种突变导致 Cwc23 与 Ntr1(SPP382)之间的相互作用减少,Ntr1 是解体途径的已知组成部分。然而,Cwc23 是一种非常非典型的 J 蛋白。尽管其 J 结构域具有功能,但对细胞活力和前体 mRNA 剪接都不是必需的。然而,在编码 Cwc23 的 J 结构域改变的点突变与 Ntr1 或 Prp43(一种对剪接体解体至关重要的 DExD/H 盒解旋酶)之间发现了强烈的遗传相互作用。这些遗传相互作用表明,基于 Hsp70 的伴侣机制确实在解体过程中发挥作用。Cwc23 提供了 J 蛋白的一个独特例子;它与 Hsp70 的伙伴关系在其基本细胞功能中发挥辅助作用,而不是核心作用。

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