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在用蛋白质合成抑制剂处理的单形和多形锥虫的血流形式中,多核糖体、前环素mRNA会积累。

Polysomal, procyclin mRNAs accumulate in bloodstream forms of monomorphic and pleomorphic trypanosomes treated with protein synthesis inhibitors.

作者信息

Graham S V, Barry J D

机构信息

Wellcome Unit of Molecular Parasitology, Anderson College University of Glasgow, UK.

出版信息

Mol Biochem Parasitol. 1996 Oct 1;80(2):179-91. doi: 10.1016/0166-6851(96)02674-6.

Abstract

The major surface antigen of insect stage (procyclic and epimastigote form) Trypanosoma brucei is termed procyclin or procyclic acidic repetitive protein (PARP). Procyclin/PARP is not expressed in bloodstream form parasites, which are coated instead with the variant surface glycoprotein (VSG). Although procyclin/PARP protein is not present and the mRNA is barely detectable, procyclin/PARP genes are transcribed at this life cycle stage. We examined the mechanism for down-regulation of procyclin/PARP expression in bloodstream trypanosomes by using protein synthesis inhibitors to effect accumulation of procyclin/PARP transcripts. We show that the accumulation is not due to increased transcription of procyclin/PARP genes. Further, transcripts which accumulate under these conditions are of mature size, polyadenylated and polysome-associated indicating that normally, in bloodstream trypanosomes, down-regulation of procyclin/PARP expression is exerted either during transcript processing or at the level of mRNA stability. A comparison of the inhibitor-induced accumulation of procyclin/PARP transcripts in bloodstream forms of monomorphic and pleomorphic cell lines of trypanosome stock EATRO 795 shows that accumulation occurs with similar kinetics in both cell lines.

摘要

布氏锥虫昆虫阶段(前循环型和上鞭毛体形式)的主要表面抗原被称为前循环素或前循环酸性重复蛋白(PARP)。前循环素/PARP在血流形式的寄生虫中不表达,取而代之的是被可变表面糖蛋白(VSG)所覆盖。尽管前循环素/PARP蛋白不存在且mRNA几乎检测不到,但前循环素/PARP基因在这个生命周期阶段仍会转录。我们通过使用蛋白质合成抑制剂来促使前循环素/PARP转录本的积累,从而研究了血流型锥虫中前循环素/PARP表达下调的机制。我们发现这种积累并非由于前循环素/PARP基因转录增加所致。此外,在这些条件下积累的转录本具有成熟的大小、多聚腺苷酸化且与多核糖体相关,这表明正常情况下,在血流型锥虫中,前循环素/PARP表达的下调发生在转录本加工过程中或mRNA稳定性水平上。对锥虫品系EATRO 795的单形和多形细胞系的血流形式中抑制剂诱导的前循环素/PARP转录本积累进行比较,结果表明两种细胞系中积累的动力学相似。

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