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通过弗林蛋白酶在分泌途径中进行蛋白质加工产生MHC I类肽抗原。

Generation of MHC class I peptide antigens by protein processing in the secretory route by furin.

作者信息

Gil-Torregrosa B C, Castaño A R, López D, Del Val M

机构信息

Centro Nacional de Biología Fundamental, Instituto de Salud Carlos III, 28220 Madrid, Spain.

出版信息

Traffic. 2000 Aug;1(8):641-51. doi: 10.1034/j.1600-0854.2000.010808.x.

DOI:10.1034/j.1600-0854.2000.010808.x
PMID:11208152
Abstract

Cytosolic degradation of endogenously synthesized proteins by the proteasome and translocation of processed peptides to the endoplasmic reticulum by the transporters associated with antigen presentation constitutes the classical route for antigen presentation by MHC class I proteins. We have previously defined an alternative pathway in the secretory route involving proteolytic maturation of precursor proproteins for chimeric hepatitis B virus secretory core protein HBe containing a class I epitope at its carboxy-terminus. We extend those results by demonstrating that intracellular delivery of the trans-Golgi network protease furin increases both proteolytic maturation and antigen presentation of the chimeric HBe proteins. An additional class I epitope from the HIV envelope gp160 protein was inserted into this COOH-terminal region of two different chimeric HBe proteins. This epitope was also presented to CTL in a transporter-independent manner involving furin, and protein maturation and antigen presentation were also enhanced by furin over-expression. Presentation of this second epitope was restricted by a different class I allele, thus suggesting that antigen presentation by this new pathway may apply to any antigenic epitope and class I molecule. These results define the furin proteolytic maturation pathway of HBe in the secretory route as a general antigen processing route for MHC class I presentation.

摘要

蛋白酶体对内源合成蛋白质的胞质降解以及与抗原呈递相关的转运体将加工后的肽转运至内质网,构成了MHC I类蛋白进行抗原呈递的经典途径。我们之前在分泌途径中定义了一条替代途径,该途径涉及对嵌合型乙型肝炎病毒分泌核心蛋白HBe的前体前蛋白进行蛋白水解成熟,HBe在其羧基末端含有一个I类表位。我们通过证明跨高尔基体网络蛋白酶弗林蛋白酶的细胞内递送可增加嵌合型HBe蛋白的蛋白水解成熟和抗原呈递,扩展了这些结果。将来自HIV包膜糖蛋白gp160的另一个I类表位插入到两种不同嵌合型HBe蛋白的该羧基末端区域。该表位也以一种不依赖转运体的方式呈递给CTL,此方式涉及弗林蛋白酶,并且弗林蛋白酶的过表达也增强了蛋白质成熟和抗原呈递。这第二个表位的呈递受不同的I类等位基因限制,因此表明通过这条新途径进行的抗原呈递可能适用于任何抗原表位和I类分子。这些结果将分泌途径中HBe的弗林蛋白酶蛋白水解成熟途径定义为MHC I类呈递的一般抗原加工途径。

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