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非洲爪蟾卵母细胞和小鼠骨髓瘤细胞中变异型MOPC 315 λ链的翻译后命运

Post-translational fate of variant MOPC 315 lambda chains in Xenopus oocytes and mouse myeloma cells.

作者信息

Valle G, Besley J, Williamson A R, Mosmann T R, Colman A

出版信息

Eur J Biochem. 1983 Apr 15;132(1):131-8. doi: 10.1111/j.1432-1033.1983.tb07337.x.

Abstract

The post-translational fates of three immunoglobulin lambda chain variants of MOPC 315 were investigated in mouse plasmacytoma cell lines and in mRNA-microinjected Xenopus oocytes. Quite unexpectedly we found that one non-secretory variant chain (lambda-43) underwent extensive post-translational N-glycosylation: however the presence of the oligosaccharide moiety did not account for the nonsecretory phenotype nor did it affect the rate of degradation of this lambda chain. Another variant chain (lambda-47) at first believed to be non-secretory, was found to be secreted from oocytes at a very low level, but mostly as a lambda-lambda dimer. In myeloma cells a low level of lambda-47 chain was secreted and again lambda-lambda dimers were the favoured secretory form. The secretory lambda-48 chain also formed lambda-lambda dimers, whereas lambda-43, which was never secreted, was only found as a monomeric lambda chain in both oocytes and myeloma cells. A similar relationship between assembly and secretion was found when oocytes were coinjected with MOPC 21 heavy (gamma 1) chain mRNA and MOPC 315 lambda chain mRNAs. The wild type lambda chain (lambda-48) was able to assemble with the gamma chain in a covalently bound tetramer (gamma gamma lambda lambda). The variant lambda-47 chain was also able to form gamma gamma lambda lambda tetramers, whereas the lambda-43 was not, even when glycosylation was prevented by tunicamycin. Both types of tetramer were secreted. These data reinforce the idea that conformational changes play a major role in the routing of secretory proteins and that the cellular mechanisms by which these changes are recognized are not cell-type specific.

摘要

在小鼠浆细胞瘤细胞系和mRNA显微注射的非洲爪蟾卵母细胞中,研究了MOPC 315的三种免疫球蛋白λ链变体的翻译后命运。非常出乎意料的是,我们发现一种非分泌性变体链(λ-43)经历了广泛的翻译后N-糖基化:然而,寡糖部分的存在既不能解释非分泌表型,也不影响该λ链的降解速率。另一种最初被认为是非分泌性的变体链(λ-47),被发现以非常低的水平从卵母细胞中分泌出来,但大多是以λ-λ二聚体的形式。在骨髓瘤细胞中,低水平的λ-47链被分泌出来,同样,λ-λ二聚体是最常见的分泌形式。分泌性的λ-48链也形成λ-λ二聚体,而从未分泌的λ-43在卵母细胞和骨髓瘤细胞中都只以单体λ链的形式存在。当卵母细胞同时注射MOPC 21重链(γ1)mRNA和MOPC 315 λ链mRNA时,发现组装和分泌之间存在类似的关系。野生型λ链(λ-48)能够与γ链组装成共价结合的四聚体(γγλλ)。变体λ-47链也能够形成γγλλ四聚体,而λ-43即使在衣霉素阻止糖基化的情况下也不能形成,两种类型的四聚体都被分泌。这些数据强化了这样一种观点,即构象变化在分泌蛋白的转运过程中起主要作用,并且识别这些变化的细胞机制不是细胞类型特异性的。

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