首页> 外文OA文献 >Biosynthesis of phosphatidylinositol-glycan (PI-G)-anchored membrane proteins in cell-free systems: PI-G is an obligatory cosubstrate for COOH-terminal processing of nascent proteins.
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Biosynthesis of phosphatidylinositol-glycan (PI-G)-anchored membrane proteins in cell-free systems: PI-G is an obligatory cosubstrate for COOH-terminal processing of nascent proteins.

机译:无细胞系统中磷脂酰肌醇聚糖(PI-G)锚定膜蛋白的生物合成:PI-G是用于新生蛋白COOH末端加工的强制性共底物。

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摘要

It is generally recognized that nascent proteins destined to be processed to a phosphatidylinositol-glycan (PI-G)-anchored membrane form contain a hydrophobic signal peptide at both their NH2 and COOH termini. In previous studies we showed that rough microsomal membranes (RM) prepared from CHO cells can carry out COOH-terminal processing. We have now investigated RM prepared from many additional cell types, including frog oocytes, B cells, and T cells, and found that all are competent with respect to COOH-terminal processing. Exceptions were certain mutant T cells that had been shown to be defective at various steps of PI-G anchor biosynthesis [Sugiyama, E., De Gasperi, R., Urakaze, M., Chang, H.-M., Thomas, L. J., Hyman, R., Warren, C. D. & Yeh, E. T. H. (1991) J. Biol. Chem. 266, 12119-12122]. In one such defective mutant, COOH-terminal processing activity of RM could be restored either by transfecting the intact cells with the gene for the deficient step in PI-G synthesis or by adding PI-G extracts to the RM in vitro. Cleavage of the COOH-terminal signal peptide in the RM is therefore dependent on the presence of intact PI-G incorporated into the mature protein.
机译:通常公认的是,注定要加工成磷脂酰肌醇聚糖(PI-G)锚定膜形式的新生蛋白质在其NH2和COOH末端均包含疏水信号肽。在以前的研究中,我们表明,从CHO细胞制备的粗糙的微粒体膜(RM)可以进行COOH末端加工。现在,我们已经研究了从许多其他细胞类型(包括青蛙卵母细胞,B细胞和T细胞)制备的RM,并发现它们在COOH末端加工方面均能胜任。某些突变T细胞例外,在PI-G锚生物合成的各个步骤中已显示出缺陷[Sugiyama,E.,De Gasperi,R.,Urakaze,M.,Chang,H.-M.,Thomas,LJ ,Hyman,R.,Warren,CD和Yeh,ETH(1991)J. Biol。Chem。化学266,12119-12122]。在一个这样的缺陷突变体中,RM的COOH末端加工活性可以通过将基因转染完整的细胞用于PI-G合成的缺陷步骤来恢复,也可以通过在体外向PI添加PI-G提取物来恢复。因此,RM中COOH末端信号肽的切割取决于整合到成熟蛋白中的完整PI-G的存在。

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