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工程化单纯疱疹病毒DNA聚合酶点突变体:α样DNA聚合酶共有的最高度保守区域参与底物识别。

Engineered herpes simplex virus DNA polymerase point mutants: the most highly conserved region shared among alpha-like DNA polymerases is involved in substrate recognition.

作者信息

Marcy A I, Hwang C B, Ruffner K L, Coen D M

机构信息

Department of Biological Chemistry and Molecular Pharmacology, Harvard Medical School, Boston, Massachusetts 02115.

出版信息

J Virol. 1990 Dec;64(12):5883-90. doi: 10.1128/JVI.64.12.5883-5890.1990.

Abstract

Eucaryotic, viral, and bacteriophage DNA polymerases of the alpha-like family share blocks of sequence similarity, the most conserved of which has been designated region I. Region I includes a YGDTDS motif that is almost invariant within the alpha-like family and that is similar to a motif conserved among RNA-directed polymerases and also includes adjacent amino acids that are more moderately conserved. To study the function of these conserved amino acids in vivo, site-specific mutagenesis was used to generate herpes simplex virus region I mutants. A recombinant virus constructed to contain a mutation within the nearly invariant YGDTDS motif was severely impaired for growth on Vero cells which do not contain a viral polymerase gene. However, three recombinants constructed to contain mutations altering more moderately conserved residues grew on Vero cells and exhibited altered sensitivities to nucleoside and PPi analogs and to aphidicolin. Marker rescue and DNA sequencing of one such recombinant demonstrated that the region I alteration confers the altered drug sensitivity phenotype. These results indicate that this region has an essential role in polymerase function in vivo and is involved directly or indirectly in drug and substrate recognition.

摘要

α-样家族的真核生物、病毒和噬菌体DNA聚合酶具有序列相似性区域,其中最保守的区域被命名为区域I。区域I包含一个YGDTDS基序,该基序在α-样家族中几乎是不变的,并且与RNA指导的聚合酶中保守的一个基序相似,还包括相邻的氨基酸,其保守程度较低。为了研究这些保守氨基酸在体内的功能,使用位点特异性诱变产生单纯疱疹病毒区域I突变体。构建的一种重组病毒在几乎不变的YGDTDS基序内含有一个突变,在不含病毒聚合酶基因的Vero细胞上生长严重受损。然而,构建的三个含有改变保守程度较低残基的突变的重组病毒在Vero细胞上生长,并对核苷和焦磷酸类似物以及对阿非科林表现出改变的敏感性。对其中一个这样的重组病毒进行标记拯救和DNA测序表明,区域I的改变赋予了改变的药物敏感性表型。这些结果表明,该区域在体内聚合酶功能中具有重要作用,并且直接或间接参与药物和底物识别。

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