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蛋白质合成的调控:前胶原衍生片段的翻译控制

Regulation of protein synthesis: translational control by procollagen-derived fragments.

作者信息

Hörlein D, McPherson J, Goh S H, Bornstein P

出版信息

Proc Natl Acad Sci U S A. 1981 Oct;78(10):6163-7. doi: 10.1073/pnas.78.10.6163.

Abstract

Previous studies have shown that a type I procollagen-derived peptide, called pN alpha 1(I)-Col 1, selectively inhibits collagen synthesis by fibroblasts in culture and the translation of procollagen mRNA in a rabbit reticulocyte lysate system. We prepared the 10,700-dalton peptide from dermatosparactic calf skin, which contained high levels of incompletely processed type I procollagen, by collagenase digestion. Time-course and dose-response studies showed that the peptide specifically inhibited the translation of procollagen mRNA in preparations of human fibroblast RNA while not affecting the translation of globin mRNA or of other messenger RNAs in fibroblast RNA. After reduction and alkylation, the peptide lost its specificity but became a nonspecific inhibitor of translation. Enzymatic cleavage enabled us to localize the nonspecific activity to a short sequence -Pro-Thr-Asp-Glu, an assignment confirmed by peptide synthesis. Using pactamycin, a specific inhibitor of translational initiation, we showed that the intact peptide acts on procollagen mRNA translation by inhibition of polypeptide chain elongation or termination, or both, whereas the nonspecific inhibitory activity of the unfolded peptide and its derivatives can be attributed to an inhibition of chain initiation. Although the native peptide may function in feedback regulation of collagen synthesis, the physiological role of the lower molecular weight fragments, if any, is uncertain.

摘要

先前的研究表明,一种源自I型前胶原的肽,称为pNα1(I)-Col 1,可在培养物中选择性抑制成纤维细胞的胶原合成,并在兔网织红细胞裂解物系统中抑制前胶原mRNA的翻译。我们通过胶原酶消化从含有高水平未完全加工的I型前胶原的皮肤松垂小牛皮肤中制备了10,700道尔顿的肽。时间进程和剂量反应研究表明,该肽特异性抑制人成纤维细胞RNA制剂中前胶原mRNA的翻译,而不影响成纤维细胞RNA中珠蛋白mRNA或其他信使RNA的翻译。还原和烷基化后,该肽失去其特异性,但成为翻译的非特异性抑制剂。酶切使我们能够将非特异性活性定位到一个短序列-Pro-Thr-Asp-Glu,肽合成证实了这一归属。使用翻译起始的特异性抑制剂 pactamycin,我们表明完整的肽通过抑制多肽链延伸或终止,或两者兼而有之,作用于前胶原mRNA翻译,而未折叠肽及其衍生物的非特异性抑制活性可归因于对链起始的抑制。尽管天然肽可能在胶原合成的反馈调节中起作用,但较低分子量片段的生理作用(如果有的话)尚不确定。

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Inhibition of procollagen cell-free synthesis by amino-terminal extension peptides.
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