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神经2A细胞中前生长抑素的加工。β-转角结构在精氨酸-赖氨酸切割位点附近的作用。

Prosomatostatin processing in Neuro2A cells. Role of beta-turn structure in the vicinity of the Arg-Lys cleavage site.

作者信息

Brakch N, Boileau G, Simonetti M, Nault C, Joseph-Bravo P, Rholam M, Cohen P

机构信息

Biochimie des Signaux Régulateurs Cellulaires et Moléculaires, Université Pierre et Marie Curie, Paris, France.

出版信息

Eur J Biochem. 1993 Aug 15;216(1):39-47. doi: 10.1111/j.1432-1033.1993.tb18114.x.

Abstract

Proline residues located near the processing sites of human prosomatostatin were previously shown to be important for cleavage of the precursor into somatostatin 28 and somatostatin 14 [Gomez, S., Boileau, G., Zollinger, L., Nault, C., Rholam, M. & Cohen, P. (1989) EMBO J. 8, 2911-2916]. In this study, site-directed and regional mutagenesis of the human prosomatostatin cDNA coupled with analysis by circular-dichroism and Fourier-transform-infrared spectroscopies of the native and mutated peptide sequences were used to elucidate the role of proline in proteolytic processing. Glycine was substituted for proline a position -5 and the beta-turn-promoting sequence Pro-Arg-Glu-Arg, located near the somatostatin-14 cleavage site and predicted to form a beta-turn structure, was replaced by Ser-Ser-Asn-Arg or Tyr-Lys-Gly-Arg, which have been shown by X-ray diffraction to form beta turns in other proteins. Analysis of the prosomatostatin-derived peptides produced by expression of the mutated cDNA species in Neuro2A cells indicated that while Pro-5-->Ala abolished cleavage at the dibasic site, the formation of mutants [Gly-5] prosomatostatin, [Ser-5, Ser-4, Arg-3] prosomatostatin and [Tyr-5, Lys-4, Gly-3] prosomatostatin did not affect cleavage at the dibasic site but produced modifications in both the relative proportions of the generated hormones and in precursor processing efficiency. Moreover, spectroscopical analysis showed that whereas these substitutions did not modify the presence of a beta turn structure in the corresponding peptide sequences, replacement of Pro-5-->Ala resulted in a dramatic increase in alpha-helix accompanied by the significant decrease of other structures including beta turn. The data support the hypothesis that the proline residue near the processing site for somatostatin-14 production is an important structural feature for conferring on the cleavage domain the adequate conformation for accessibility to processing enzymes and permitting production of equivalent amounts of both hormones.

摘要

先前研究表明,位于人前生长抑素加工位点附近的脯氨酸残基对于将前体切割为生长抑素28和生长抑素14至关重要[戈麦斯,S.,布瓦洛,G.,佐林格,L.,诺尔特,C.,罗拉姆,M. & 科恩,P.(1989年)《欧洲分子生物学组织杂志》8,2911 - 2916]。在本研究中,利用人前生长抑素cDNA的定点和区域诱变,结合对天然和突变肽序列的圆二色光谱和傅里叶变换红外光谱分析,以阐明脯氨酸在蛋白水解加工中的作用。在 - 5位用甘氨酸取代脯氨酸,并将位于生长抑素 - 14切割位点附近且预测形成β - 转角结构的促进β - 转角的序列Pro - Arg - Glu - Arg替换为Ser - Ser - Asn - Arg或Tyr - Lys - Gly - Arg,X射线衍射已表明它们在其他蛋白质中形成β - 转角。对在Neuro2A细胞中表达突变cDNA物种产生的前生长抑素衍生肽的分析表明,虽然Pro - 5→Ala消除了在双碱性位点的切割,但突变体[Gly - 5]前生长抑素、[Ser - 5,Ser - 4,Arg - 3]前生长抑素和[Tyr - 5,Lys - 4,Gly - 3]前生长抑素的形成并不影响在双碱性位点的切割,但在生成激素的相对比例和前体加工效率方面产生了改变。此外,但光谱分析表明,虽然这些取代并未改变相应肽序列中β - 转角结构的存在,但Pro - 5→Ala的替换导致α - 螺旋显著增加,同时包括β - 转角在内的其他结构显著减少。这些数据支持以下假设:生长抑素 - 14产生加工位点附近的脯氨酸残基是赋予切割结构域适当构象以利于加工酶接近并允许产生等量两种激素的重要结构特征。

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