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Ypt1 GTP酶介导的蛋白质转运对核苷酸交换因子的需求。

Requirement of nucleotide exchange factor for Ypt1 GTPase mediated protein transport.

作者信息

Jones S, Litt R J, Richardson C J, Segev N

机构信息

Department of Pharmacological, University of Chicago, Illinois 60637, USA.

出版信息

J Cell Biol. 1995 Sep;130(5):1051-61. doi: 10.1083/jcb.130.5.1051.

DOI:10.1083/jcb.130.5.1051
PMID:7657691
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2120555/
Abstract

Small GTPases of the rab family are involved in the regulation of vesicular transport. It is believed that cycling between the GTP- and GDP-bound forms, and accessory factors regulating this cycling are crucial for rab function. However, an essential role for rab nucleotide exchange factors has not yet been demonstrated. In this report we show the requirement of nucleotide exchange factor activity for Ypt1 GTPase mediated protein transport. The Ypt1 protein, a member of the rab family, plays a role in targeting vesicles to the acceptor compartment and is essential for the first two steps of the yeast secretory pathway. We use two YPT1 dominant mutations that contain alterations in a highly conserved GTP-binding domain, N121I and D124N. YPT1-D124N is a novel mutation that encodes a protein with nucleotide specificity modified from guanine to xanthine. This provides a tool for the study of an individual rab GTPase in crude extracts: a xanthosine triphosphate (XTP)-dependent conditional dominant mutation. Both mutations confer growth inhibition and a block in protein secretion when expressed in vivo. The purified mutant proteins do not bind either GDP or GTP. Moreover, they completely inhibit the ability of the exchange factor to stimulate nucleotide exchange for wild type Ypt1 protein, and are potent inhibitors of ER to Golgi transport in vitro at the vesicle targeting step. The inhibitory effects of the Ypt1-D124N mutant protein on both nucleotide exchange activity and protein transport in vitro can be relieved by XTP, indicating that it is the nucleotide-free form of the mutant protein that is inhibitory. These results suggest that the dominant mutant proteins inhibit protein transport by sequestering the exchange factor from the wild type Ypt1 protein, and that this factor has an essential role in vesicular transport.

摘要

Rab家族的小GTP酶参与囊泡运输的调控。人们认为,在结合GTP和GDP的形式之间循环,以及调节这种循环的辅助因子对Rab功能至关重要。然而,Rab核苷酸交换因子的重要作用尚未得到证实。在本报告中,我们展示了Ypt1 GTP酶介导的蛋白质运输对核苷酸交换因子活性的需求。Ypt1蛋白是Rab家族的成员,在将囊泡靶向受体区室中发挥作用,并且对酵母分泌途径的前两个步骤至关重要。我们使用了两个YPT1显性突变,它们在高度保守的GTP结合结构域中含有改变,即N121I和D124N。YPT1-D124N是一种新的突变,编码一种核苷酸特异性从鸟嘌呤改变为黄嘌呤的蛋白质。这为在粗提物中研究单个Rab GTP酶提供了一种工具:一种依赖于三磷酸黄苷(XTP)的条件显性突变。当在体内表达时,这两种突变都会导致生长抑制和蛋白质分泌受阻。纯化的突变蛋白既不结合GDP也不结合GTP。此外,它们完全抑制交换因子刺激野生型Ypt1蛋白核苷酸交换的能力,并且在体外囊泡靶向步骤中是内质网到高尔基体运输的有效抑制剂。Ypt1-D124N突变蛋白对体外核苷酸交换活性和蛋白质运输的抑制作用可以被XTP缓解,这表明是突变蛋白的无核苷酸形式具有抑制作用。这些结果表明,显性突变蛋白通过将交换因子与野生型Ypt1蛋白隔离来抑制蛋白质运输,并且该因子在囊泡运输中具有重要作用。