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GAD65靶向高尔基体复合体区域需要位于其1-27位氨基酸内的信号。

A signal located within amino acids 1-27 of GAD65 is required for its targeting to the Golgi complex region.

作者信息

Solimena M, Dirkx R, Radzynski M, Mundigl O, De Camilli P

机构信息

Department of Cell Biology, Yale University School of Medicine, New Haven, Connecticut 06510.

出版信息

J Cell Biol. 1994 Jul;126(2):331-41. doi: 10.1083/jcb.126.2.331.

Abstract

The mechanisms involved in the targeting of proteins to different cytosolic compartments are still largely unknown. In this study we have investigated the targeting signal of the 65-kD isoform of glutamic acid decarboxylase (GAD65), a major autoantigen in two autoimmune diseases: Stiff-Man syndrome and insulin-dependent diabetes mellitus. GAD65 is expressed in neurons and in pancreatic beta-cells, where it is concentrated in the Golgi complex region and in proximity to GABA-containing vesicles. GAD65, but not the similar isoform GAD67 which has a more diffuse cytosolic distribution, is palmitoylated within its first 100 amino acids (a.a.). We have previously demonstrated that the domain corresponding to a.a. 1-83 of GAD65 is required for the targeting of GAD65 to the Golgi complex region. Here we show that this domain is sufficient to target an unrelated protein, beta-galactosidase, to the same region. Site-directed mutagenesis of all the putative acceptor sites for thiopalmitoylation within this domain did not abolish targeting of GAD65 to the Golgi complex region. The replacement of a.a. 1-29 of GAD67 with the corresponding a.a. 1-27 of GAD65 was sufficient to target the otherwise soluble GAD67 to the Golgi complex region. Conversely, the replacement of a.a. 1-27 of GAD65 with a.a. 1-29 of GAD67 resulted in a GAD65 protein that had a diffuse cytosolic distribution and was primarily hydrophilic, suggesting that targeting to the Golgi complex region is required for palmitoylation of GAD65. We propose that the domain corresponding to a.a. 1-27 of GAD65, contains a signal required for the targeting of GAD65 to the Golgi complex region.

摘要

蛋白质靶向不同胞质区室的机制在很大程度上仍不清楚。在本研究中,我们研究了谷氨酸脱羧酶65-kD同工型(GAD65)的靶向信号,GAD65是两种自身免疫性疾病——僵人综合征和胰岛素依赖型糖尿病中的主要自身抗原。GAD65在神经元和胰腺β细胞中表达,在这些细胞中它集中在高尔基体复合体区域以及含γ-氨基丁酸(GABA)的囊泡附近。GAD65,而非具有更弥散胞质分布的类似同工型GAD67,在其前100个氨基酸(a.a.)内发生了棕榈酰化。我们之前已经证明,GAD65对应于a.a. 1-83的结构域是GAD65靶向高尔基体复合体区域所必需的。在此我们表明,该结构域足以将无关蛋白β-半乳糖苷酶靶向到同一区域。对该结构域内所有假定的硫代棕榈酰化受体位点进行定点诱变,并未消除GAD65靶向高尔基体复合体区域的能力。用GAD65相应的a.a. 1-27替换GAD67的a.a. 1-29足以将原本可溶的GAD67靶向到高尔基体复合体区域。相反,用GAD67的a.a. 1-29替换GAD65的a.a. 1-27导致GAD65蛋白具有弥散的胞质分布且主要为亲水性,这表明靶向高尔基体复合体区域是GAD65棕榈酰化所必需的。我们提出,GAD65对应于a.a. 1-27的结构域包含将GAD65靶向高尔基体复合体区域所需的信号。

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