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载脂蛋白B mRNA编辑酶催化多肽样3B:一种先天性免疫DNA突变酶的病理后果

APOBEC3B: pathological consequences of an innate immune DNA mutator.

作者信息

Burns Michael B, Leonard Brandon, Harris Reuben S

机构信息

Masonic Cancer Center; Institute for Molecular Virology; Center for Genome Engineering; Biochemistry, Molecular Biology and Biophysics Department, University of Minnesota, Minneapolis, MN, USA.

出版信息

Biomed J. 2015 Mar-Apr;38(2):102-10. doi: 10.4103/2319-4170.148904.

Abstract

Cancer is a disease that results from alterations in the cellular genome. Several recent studies have identified mutational signatures that implicate a variety of mutagenic processes in cancer, a major one of which is explained by the enzymatic activity of the DNA cytosine deaminase, APOBEC3B. As a deaminase, APOBEC3B converts cytosines to uracils in single-stranded DNA. Failure to properly repair these uracil lesions can result in a diverse array of mutations. For instance, DNA uracils can template the insertion of complementary adenines leading to C-to-T transition mutations. DNA uracils can also be converted into abasic sites that, depending upon the DNA polymerase recruited to bypass this lesion in the template strand, can lead to adenine insertion and C-to-T mutations as well as cytosine insertion and C-to-G transversion mutations. Finally, DNA uracils can also be converted into DNA breaks that may precipitate some types of larger chromosomal aberrations observed in cancer. These studies cumulatively demonstrate that APOBEC3B is a major source of genetic heterogeneity in several human cancers and, as such, this enzyme may prove to be a critical diagnostic and therapeutic target.

摘要

癌症是一种由细胞基因组改变引发的疾病。最近的几项研究已鉴定出突变特征,这些特征表明癌症中存在多种诱变过程,其中一个主要过程可由DNA胞嘧啶脱氨酶APOBEC3B的酶活性来解释。作为一种脱氨酶,APOBEC3B可将单链DNA中的胞嘧啶转化为尿嘧啶。未能正确修复这些尿嘧啶损伤会导致各种各样的突变。例如,DNA尿嘧啶可作为模板插入互补腺嘌呤,导致C到T的转换突变。DNA尿嘧啶也可转化为无碱基位点,根据招募来绕过模板链中此损伤的DNA聚合酶不同,可导致腺嘌呤插入和C到T突变,以及胞嘧啶插入和C到G的颠换突变。最后,DNA尿嘧啶还可转化为DNA断裂,这可能促成在癌症中观察到的某些类型的较大染色体畸变。这些研究累积表明,APOBEC3B是几种人类癌症中遗传异质性的主要来源,因此,这种酶可能被证明是一个关键的诊断和治疗靶点。

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