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克氏锥虫聚腺苷酸结合蛋白C端结构域的溶液结构:一种植物型PABC结构域

Solution structure of the C-terminal domain from poly(A)-binding protein in Trypanosoma cruzi: a vegetal PABC domain.

作者信息

Siddiqui Nadeem, Kozlov Guennadi, D'Orso Iván, Trempe Jean-François, Gehring Kalle

机构信息

Department of Biochemistry, McGill University, Montreal, Quebec H3G 1Y6, Canada.

出版信息

Protein Sci. 2003 Sep;12(9):1925-33. doi: 10.1110/ps.0390103.

Abstract

PABC is a phylogenetically conserved peptide-binding domain primarily found within the C terminus of poly(A)-binding proteins (PABPs). This domain recruits a series of translation factors including poly(A)-interacting proteins (Paip1 and Paip2) and release factor 3 (RF3/GSPT) to the initiation complex on mRNA. Here, we determine the solution structure of the Trypanosoma cruzi PABC domain (TcPABC), a representative of the vegetal class of PABP proteins. TcPABC is similar to human PABC (hPABC) and consists of five alpha-helices, in contrast to the four helices observed in PABC domains from yeast (yPABC) and hyper plastic disk proteins (hHYD). A mobile N-terminal helix is observed in TcPABC that does not pack against the core of the protein, as found in hPABC. Characteristic to all PABC domains, the last four helices of TcPABC fold into a right-handed super coil. TcPABC demonstrates high-affinity binding to PABP interacting motif-2 (PAM-2) and reveals a peptide-binding surface homologous to that of hPABC. Our results demonstrate the last four helices in TcPABC are sufficient for peptide recognition and we predict a similar binding mode in PABC domains. Furthermore, these results point to the presence of putative PAM-2 site-containing proteins in trypanosomes.

摘要

聚腺苷酸结合蛋白C端结构域(PABC)是一种在进化上保守的肽结合结构域,主要存在于聚腺苷酸结合蛋白(PABP)的C末端。该结构域可将一系列翻译因子招募到mRNA上的起始复合物,这些因子包括聚腺苷酸相互作用蛋白(Paip1和Paip2)以及释放因子3(RF3/GSPT)。在此,我们确定了克氏锥虫PABC结构域(TcPABC)的溶液结构,它是植物类PABP蛋白的代表。TcPABC与人类PABC(hPABC)相似,由五个α螺旋组成,这与酵母(yPABC)和超塑性盘蛋白(hHYD)的PABC结构域中观察到的四个螺旋不同。在TcPABC中观察到一个可移动的N端螺旋,它不像在hPABC中那样紧密堆积在蛋白质核心上。所有PABC结构域的特征是,TcPABC的最后四个螺旋折叠成一个右手超螺旋。TcPABC表现出与PABP相互作用基序2(PAM-2)的高亲和力结合,并揭示了一个与hPABC同源的肽结合表面。我们的结果表明,TcPABC中的最后四个螺旋足以进行肽识别,并且我们预测PABC结构域中存在类似的结合模式。此外,这些结果表明锥虫中存在假定的含PAM-2位点的蛋白质。

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