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通过掺入亮氨酸类似物抑制腹水肿瘤裂解物中的前体蛋白加工。

Inhibition of preprotein processing in ascites tumor lysates by incorporation of a leucine analog.

作者信息

Hortin G, Boime I

出版信息

Proc Natl Acad Sci U S A. 1980 Mar;77(3):1356-60. doi: 10.1073/pnas.77.3.1356.

Abstract

Leucine analogs were tested in the Krebs II ascites cell-free translation system for the ability to inhibit preprotein cleavage by replacing leucine in nascent chains of bovine preprolactin, rat preprolactin, human placental prelactogen (pre-hPL), and pre-alpha subunit of human chorionic gonadotropin (alpha-hCG). In the absence of analog, ascites microsomal membranes cleaved these preproteins to their mature forms and sequestered the processed products. Also, two asparagine residues in alpha-hCG were glycosylated. When 4 mM beta-DL-hydroxyleucine was added to the lysate instead of L-leucine, cotranslational processing and sequestration of both species of preprolactin and pre-hPL were inhibited. Sequential Edman degradation confirmed that pre-hPL was not cleaved. The inhibition of processing by beta-hydroxyleucine resulted from its incorporation into protein. This was shown by reversal of the effect by addition of leucine and by inhibition of [(3)H]leucine incorporation into protein. Of significance, the processing of pre-alpha-hCG was less sensitive to beta-hydroxyleucine because its prepeptide contains only four scattered leucine residues, whereas the presegments of hPL and the prolactins contain six to eight clustered leucine residues. These experiments demonstrate that translocation and processing of secretory proteins require structural features determined by the primary amino acid sequence.

摘要

在克雷布斯II腹水无细胞翻译系统中测试了亮氨酸类似物,以评估其通过取代牛前催乳素、大鼠前催乳素、人胎盘催乳素原(pre-hPL)和人绒毛膜促性腺激素前α亚基(α-hCG)新生链中的亮氨酸来抑制前体蛋白切割的能力。在不存在类似物的情况下,腹水微粒体膜将这些前体蛋白切割成成熟形式并隔离加工后的产物。此外,α-hCG中的两个天冬酰胺残基发生了糖基化。当向裂解物中添加4 mMβ-DL-羟基亮氨酸而非L-亮氨酸时,两种前催乳素和pre-hPL的共翻译加工和隔离均受到抑制。连续的埃德曼降解证实pre-hPL未被切割。β-羟基亮氨酸对加工的抑制作用源于其掺入蛋白质中。添加亮氨酸使该效应逆转以及抑制[³H]亮氨酸掺入蛋白质均证明了这一点。重要的是,前α-hCG的加工对β-羟基亮氨酸不太敏感,因为其前肽仅含有四个分散的亮氨酸残基,而hPL和催乳素的前肽段含有六个至八个成簇的亮氨酸残基。这些实验表明,分泌蛋白的易位和加工需要由一级氨基酸序列决定的结构特征。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/363e/348493/2fdb7e256386/pnas00666-0134-a.jpg

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