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持续蛋白质合成对恰加斯利什曼原虫中Gp63 RNA稳态水平的影响。

The effect of ongoing protein synthesis on the steady state levels of Gp63 RNAs in Leishmania chagasi.

作者信息

Wilson M E, Paetz K E, Ramamoorthy R, Donelson J E

机构信息

Department of Medicine, University of Iowa, Iowa City 52242.

出版信息

J Biol Chem. 1993 Jul 25;268(21):15731-6.

PMID:8340397
Abstract

G63, the major surface glycoprotein of Leishmania chagasi promastigotes, increases 11-fold in amount as promastigotes grow from logarithmic to stationary phase. Transcripts from three different classes of gp63 genes are differentially expressed during this development (Ramamoorthy, R., Donelson, J. E., Paetz, K. E., Maybodi, M., Roberts, S. P., and Wilson, M. E. (1992) J. Biol. Chem. 267, 1888-1895). We studied the effect of protein synthesis inhibitors on gp63 mRNAs. The steady state level of log class gp63 RNA, expressed primarily in logarithmic phase promastigotes, increased 16.5-fold after incubation in cycloheximide. A similar increase in log gp63 RNAs was caused by inhibitors that block different steps in translation. In contrast, the levels of stationary class gp63 RNA, expressed in stationary phase parasites, and constitutive class gp63 RNA, expressed throughout promastigote growth, increased only 2.3- and 1.5-fold, respectively. The latter was not statistically significant. Nuclear run-on assays showed that the cycloheximide effect was not due to an increased rate of transcription. However, the t1/2 of log RNAs was prolonged 6.5-fold after incubation in cycloheximide, in contrast to a 1.7-fold increase in the t1/2 of ATPase RNA, suggesting that cycloheximide specifically stabilizes log gp63 mRNAs. Thus, a highly labile negative regulatory protein, such as an RNase, may specifically target log gp63 RNAs for degradation.

摘要

G63是恰加斯利什曼原虫前鞭毛体的主要表面糖蛋白,当前鞭毛体从对数生长期生长至稳定期时,其含量增加11倍。在这一发育过程中,来自三类不同gp63基因的转录本差异表达(拉马穆尔蒂,R.,多尼尔森,J.E.,佩茨,K.E.,迈博迪,M.,罗伯茨,S.P.,以及威尔逊,M.E.(1992年)《生物化学杂志》267卷,1888 - 1895页)。我们研究了蛋白质合成抑制剂对gp63信使核糖核酸的影响。主要在对数期前鞭毛体中表达的对数期类gp63核糖核酸的稳态水平,在环己酰亚胺中孵育后增加了16.5倍。阻断翻译不同步骤的抑制剂也导致对数期gp63核糖核酸有类似的增加。相比之下,在稳定期寄生虫中表达的稳定期类gp63核糖核酸以及在前鞭毛体整个生长过程中表达的组成型类gp63核糖核酸的水平分别仅增加了2.3倍和1.5倍。后者无统计学意义。细胞核连续转录分析表明,环己酰亚胺的作用并非由于转录速率增加。然而,与ATP酶核糖核酸的半衰期增加1.7倍相比,对数期核糖核酸在环己酰亚胺中孵育后半衰期延长了6.5倍,这表明环己酰亚胺特异性地稳定了对数期gp63信使核糖核酸。因此,一种高度不稳定的负调控蛋白,如核糖核酸酶,可能特异性地靶向对数期gp63核糖核酸进行降解。

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