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疟原虫伯氏疟原虫RNA聚合酶II的C末端结构域。

The C-terminal domain of RNA polymerase II of the malaria parasite Plasmodium berghei.

作者信息

Giesecke H, Barale J C, Langsley G, Cornelissen A W

机构信息

Max-Planck-Institut für Biologie, Molecular Parasitology Unit, Tübingen, FRG.

出版信息

Biochem Biophys Res Commun. 1991 Nov 14;180(3):1350-5. doi: 10.1016/s0006-291x(05)81344-0.

Abstract

The C-terminal domain (CTD) of RNA polymerase II (RNAP) has an essential function in the regulation of transcription. The CTD of the human malaria parasite, Plasmodium falciparum, differs dramatically from that of higher eukaryotes. To determine whether this is a general feature of malarial parasites, we have analysed the CTD of the distantly related rodent malaria parasite P.berghei. The CTDs of the two parasites enzymes are very similar in amino acid composition and contain the basic structure of most eukaryotic CTDs, which is a tandem repeat of a heptapeptide (SPTSPSY). The CTD of P.berghei differs, however, in three aspects from the CTD of P.falciparum and other eukaryotes. First, both domains show a divergence from the consensus sequence at position 6 of the heptapeptide repeat. The Ser6 is always substituted, with a bias for lysine. The latter substitution might increase the binding efficiency to the DNA template. Second, the rodent and human malarial CTDs contain a 3' extension of, respectively, 66 or 67 amino acid residues. This tail-piece is unique among eukaryotes. Third, the enlargement of the CTD of the human parasite by six heptapeptide repeats is most likely generated by a recent amplification of a specific repeat unit.

摘要

RNA聚合酶II(RNAP)的C末端结构域(CTD)在转录调控中具有重要功能。人类疟原虫恶性疟原虫的CTD与高等真核生物的CTD有显著差异。为了确定这是否是疟原虫的普遍特征,我们分析了亲缘关系较远的啮齿动物疟原虫伯氏疟原虫的CTD。这两种寄生虫酶的CTD在氨基酸组成上非常相似,并且包含大多数真核生物CTD的基本结构,即七肽(SPTSPSY)的串联重复序列。然而,伯氏疟原虫的CTD在三个方面与恶性疟原虫和其他真核生物的CTD不同。首先,两个结构域在七肽重复序列的第6位与共有序列存在差异。Ser6总是被取代,偏向于赖氨酸。后一种取代可能会提高与DNA模板的结合效率。其次,啮齿动物和人类疟原虫的CTD分别含有一个由66或67个氨基酸残基组成的3'延伸部分。这个尾段在真核生物中是独特的。第三,人类寄生虫的CTD通过六个七肽重复序列的扩增很可能是由最近一个特定重复单元的扩增产生的。

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