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多核苷酸磷酸化酶结构与功能的遗传分析

Genetic analysis of polynucleotide phosphorylase structure and functions.

作者信息

Briani Federica, Del Favero Marta, Capizzuto Rossana, Consonni Chiara, Zangrossi Sandro, Greco Claudio, De Gioia Luca, Tortora Paolo, Dehò Gianni

机构信息

Dipartimento di Scienze Biomolecolari e Biotecnologie, Università degli Studi di Milano, Via Celoria 26, 20133 Milan, Italy.

出版信息

Biochimie. 2007 Jan;89(1):145-57. doi: 10.1016/j.biochi.2006.09.020. Epub 2006 Oct 18.

DOI:10.1016/j.biochi.2006.09.020
PMID:17084501
Abstract

Polynucleotide phosphorylase (PNPase) is a phosphate-dependent 3' to 5' exonuclease widely diffused among bacteria and eukaryotes. The enzyme, a homotrimer, can also be found associated with the endonuclease RNase E and other proteins in a heteromultimeric complex, the RNA degradosome. PNPase negatively controls its own gene (pnp) expression by destabilizing pnp mRNA. A current model of autoregulation maintains that PNPase and a short duplex at the 5'-end of pnp mRNA are the only determinants of mRNA stability. During the cold acclimation phase autoregulation is transiently relieved and cellular pnp mRNA abundance increases significantly. Although PNPase has been extensively studied and widely employed in molecular biology for about 50 years, several aspects of structure-function relationships of such a complex protein are still elusive. In this work, we performed a systematic PCR mutagenesis of discrete pnp regions and screened the mutants for diverse phenotypic traits affected by PNPase. Overall our results support previous proposals that both first and second core domains are involved in the catalysis of the phosphorolytic reaction, and that both phosphorolytic activity and RNA binding are required for autogenous regulation and growth in the cold, and give new insights on PNPase structure-function relationships by implicating the alpha-helical domain in PNPase enzymatic activity.

摘要

多核苷酸磷酸化酶(PNPase)是一种依赖磷酸的3'至5'核酸外切酶,广泛存在于细菌和真核生物中。该酶为同三聚体,也可在异源多聚体复合物RNA降解体中与核酸内切酶RNase E及其他蛋白质结合。PNPase通过使pnp mRNA不稳定来负向调控其自身基因(pnp)的表达。目前的一种自动调节模型认为,PNPase和pnp mRNA 5'端的短双链体是mRNA稳定性的唯一决定因素。在冷驯化阶段,自动调节会暂时解除,细胞内pnp mRNA丰度会显著增加。尽管PNPase已被广泛研究并在分子生物学中广泛应用了约50年,但这种复杂蛋白质的结构-功能关系的几个方面仍然不清楚。在这项工作中,我们对pnp的离散区域进行了系统的PCR诱变,并筛选了受PNPase影响的各种表型特征的突变体。总体而言,我们的结果支持了先前的观点,即第一和第二核心结构域都参与磷酸解反应的催化,并且磷酸解活性和RNA结合对于自身调节和低温生长都是必需的,并且通过将α-螺旋结构域与PNPase酶活性联系起来,为PNPase的结构-功能关系提供了新的见解。

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