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内质网相关 SNARE 蛋白和 Sey1p 在酵母交配过程中核融合的两个不同步骤中发挥作用。

ER-associated SNAREs and Sey1p mediate nuclear fusion at two distinct steps during yeast mating.

机构信息

Department of Molecular Biology, Princeton University, Princeton, NJ 08544-1014.

出版信息

Mol Biol Cell. 2013 Dec;24(24):3896-908. doi: 10.1091/mbc.E13-08-0441. Epub 2013 Oct 23.

Abstract

During yeast mating, two haploid nuclei fuse membranes to form a single diploid nucleus. However, the known proteins required for nuclear fusion are unlikely to function as direct fusogens (i.e., they are unlikely to directly catalyze lipid bilayer fusion) based on their predicted structure and localization. Therefore we screened known fusogens from vesicle trafficking (soluble N-ethylmaleimide-sensitive factor attachment protein receptors [SNAREs]) and homotypic endoplasmic reticulum (ER) fusion (Sey1p) for additional roles in nuclear fusion. Here we demonstrate that the ER-localized SNAREs Sec20p, Ufe1p, Use1p, and Bos1p are required for efficient nuclear fusion. In contrast, Sey1p is required indirectly for nuclear fusion; sey1Δ zygotes accumulate ER at the zone of cell fusion, causing a block in nuclear congression. However, double mutants of Sey1p and Sec20p, Ufe1p, or Use1p, but not Bos1p, display extreme ER morphology defects, worse than either single mutant, suggesting that retrograde SNAREs fuse ER in the absence of Sey1p. Together these data demonstrate that SNAREs mediate nuclear fusion, ER fusion after cell fusion is necessary to complete nuclear congression, and there exists a SNARE-mediated, Sey1p-independent ER fusion pathway.

摘要

在酵母交配过程中,两个单倍体核融合膜形成一个单倍体核。然而,根据已知的蛋白质预测结构和定位,用于核融合的已知蛋白质不太可能作为直接融合蛋白(即,它们不太可能直接催化脂质双层融合)。因此,我们从囊泡运输(可溶性 N-乙基马来酰亚胺敏感因子附着蛋白受体 [SNAREs])和同源内质网(ER)融合(Sey1p)中筛选了已知的融合蛋白,以寻找其在核融合中的其他作用。在这里,我们证明了内质网定位的 SNAREs Sec20p、Ufe1p、Use1p 和 Bos1p 是核融合所必需的。相比之下,Sey1p 间接参与核融合;sey1Δ 合子在细胞融合区积累 ER,导致核汇聚受阻。然而,sey1Δ 和 Sec20p、Ufe1p 或 Use1p 的双突变体,但不是 Bos1p,显示出极端的 ER 形态缺陷,比任何单突变体都严重,这表明逆行 SNAREs 在没有 Sey1p 的情况下融合 ER。这些数据共同表明 SNAREs 介导核融合,细胞融合后 ER 融合对于完成核汇聚是必要的,并且存在 SNARE 介导的、Sey1p 独立的 ER 融合途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2e2a/3861085/22ddcdb17d1a/3896fig1.jpg

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