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The AAA team: related ATPases with diverse functions.AAA团队:具有多种功能的相关ATP酶。
Trends Cell Biol. 1998 Feb;8(2):65-71.
2
Mutational analysis of Csc1/Vps4p: involvement of endosome in regulation of autophagy in yeast.Csc1/Vps4p的突变分析:内体参与酵母自噬的调控
Cell Struct Funct. 1997 Oct;22(5):501-9. doi: 10.1247/csf.22.501.
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Inhibition of endosome function in CHO cells bearing a temperature-sensitive defect in the coatomer (COPI) component epsilon-COP.在衣被蛋白(COPI)组分ε-COP中存在温度敏感缺陷的CHO细胞中内体功能的抑制。
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NSF is required for transport from early to late endosomes.从早期内体到晚期内体的运输需要 NSF。
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Domain structure and intramolecular regulation of dynamin GTPase.发动蛋白GTP酶的结构域结构与分子内调节
EMBO J. 1997 Nov 17;16(22):6676-83. doi: 10.1093/emboj/16.22.6676.
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Sequence analysis of the AAA protein family.AAA蛋白家族的序列分析。
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Structure and conformational changes in NSF and its membrane receptor complexes visualized by quick-freeze/deep-etch electron microscopy.通过快速冷冻/深度蚀刻电子显微镜观察到的 NSF 及其膜受体复合物的结构和构象变化。
Cell. 1997 Aug 8;90(3):523-35. doi: 10.1016/s0092-8674(00)80512-7.
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The diversity of Rab proteins in vesicle transport.Rab蛋白在囊泡运输中的多样性。
Curr Opin Cell Biol. 1997 Aug;9(4):496-504. doi: 10.1016/s0955-0674(97)80025-7.
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SNAREs and NSF in targeted membrane fusion.靶向膜融合中的SNARE蛋白和N-乙基马来酰胺敏感因子
Curr Opin Cell Biol. 1997 Aug;9(4):505-12. doi: 10.1016/s0955-0674(97)80026-9.
10
Hrs, a tyrosine kinase substrate with a conserved double zinc finger domain, is localized to the cytoplasmic surface of early endosomes.Hrs是一种具有保守双锌指结构域的酪氨酸激酶底物,定位于早期内体的细胞质表面。
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Vps4p AAA型ATP酶调节正常内体功能所需的Vps蛋白复合物的膜结合。

The Vps4p AAA ATPase regulates membrane association of a Vps protein complex required for normal endosome function.

作者信息

Babst M, Wendland B, Estepa E J, Emr S D

机构信息

Division of Cellular Molecular Medicine and Howard Hughes Medical Institute, University of California at San Diego, School of Medicine La Jolla, CA 92093-0668, USA.

出版信息

EMBO J. 1998 Jun 1;17(11):2982-93. doi: 10.1093/emboj/17.11.2982.

DOI:10.1093/emboj/17.11.2982
PMID:9606181
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1170638/
Abstract

Vps4p is an AAA-type ATPase required for efficient transport of biosynthetic and endocytic cargo from an endosome to the lysosome-like vacuole of Saccharomyces cerevisiae. Vps4p mutants that do not bind ATP or are defective in ATP hydrolysis were characterized both in vivo and in vitro. The nucleotide-free or ADP-bound form of Vps4p existed as a dimer, whereas in the ATP-locked state, Vps4p dimers assembled into a decameric complex. This suggests that ATP hydrolysis drives a cycle of association and dissociation of Vps4p dimers/decamers. Nucleotide binding also regulated the association of Vps4p with an endosomal compartment in vivo. This membrane association required the N-terminal coiled-coil motif of Vps4p, but deletion of the coiled-coil domain did not affect ATPase activity or oligomeric assembly of the protein. Membrane association of two previously uncharacterized class E Vps proteins, Vps24p and Vps32p/Snf7p, was also affected by mutations in VPS4. Upon inactivation of a temperature-conditional vps4 mutant, Vps24p and Vps32p/Snf7p rapidly accumulated in a large membrane-bound complex. Immunofluorescence indicated that both proteins function with Vps4p at a common endosomal compartment. Together, the data suggest that the Vps4 ATPase catalyzes the release (uncoating) of an endosomal membrane-associated class E protein complex(es) required for normal morphology and sorting activity of the endosome.

摘要

Vps4p是一种AAA型ATP酶,对于酿酒酵母中生物合成和内吞货物从内体高效运输到溶酶体样液泡是必需的。对不结合ATP或ATP水解有缺陷的Vps4p突变体进行了体内和体外表征。Vps4p的无核苷酸或ADP结合形式以二聚体形式存在,而在ATP锁定状态下,Vps4p二聚体组装成十聚体复合物。这表明ATP水解驱动Vps4p二聚体/十聚体的缔合和解离循环。核苷酸结合在体内也调节Vps4p与内体区室的缔合。这种膜缔合需要Vps4p的N端卷曲螺旋基序,但卷曲螺旋结构域的缺失不影响该蛋白的ATP酶活性或寡聚组装。另外两个未表征的E类Vps蛋白Vps24p和Vps32p/Snf7p的膜缔合也受到VPS4突变的影响。温度条件性vps4突变体失活后,Vps24p和Vps32p/Snf7p迅速积累在一个大的膜结合复合物中。免疫荧光表明这两种蛋白与Vps4p在内体的一个共同区室发挥作用。总之,数据表明Vps4 ATP酶催化内体膜相关的E类蛋白复合物的释放(脱衣),这是内体正常形态和分选活性所必需的。