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密码子上下文对于理解乳腺癌中TP53突变的Ig样体细胞超突变链偏向模式的重要性。

The importance of codon context for understanding the Ig-like somatic hypermutation strand-biased patterns in TP53 mutations in breast cancer.

作者信息

Lindley Robyn A

机构信息

Melville Analytics Pty Ltd, Jindabyne, Australia.

出版信息

Cancer Genet. 2013 Jun;206(6):222-6. doi: 10.1016/j.cancergen.2013.05.016. Epub 2013 Jul 21.

Abstract

Evidence already exists that the activation-induced deaminase (AID)/APOBEC family constitutes a set of differentially expressed enzymes capable of deaminating cytosines (C to U) in single-stranded DNA (ssDNA) and that they are potentially powerful mutagens. The mutagenic processes involved are believed to be activated in many nonlymphoid tissue types-for example, initiating some cancers and/or leading to further somatic mutagenesis. To investigate the extent that codon context might be important in influencing the likely location of TP53 mutations in breast cancer, the codon-bias patterns resulting from the ssDNA target specificities of cytidine deaminases of the AID/APOBEC family were analyzed. The data indicate that codon context strongly influences the likely location of mutations at motifs for AID/APOBEC1/APOBEC3G, and at WA sites. An unexpected finding is a highly significant preference for transitions of cytosine to occur at the first nucleotide position and for transitions of guanosine to occur at the second nucleotide position in the mutated codon (read 3' to 5'). Thus, the mechanisms involved appear to be sensitive to codon reading frames and to have an intrinsic ability to differentiate between the cytosines on the nontranscribed strand and those on the transcribed strand in the context of an open "transcription bubble."

摘要

已有证据表明,激活诱导的脱氨酶(AID)/载脂蛋白B mRNA编辑酶催化多肽样家族(APOBEC)构成了一组能够使单链DNA(ssDNA)中的胞嘧啶(C到U)脱氨的差异表达酶,并且它们可能是强大的诱变剂。据信,所涉及的诱变过程在许多非淋巴组织类型中被激活,例如引发某些癌症和/或导致进一步的体细胞诱变。为了研究密码子上下文在影响乳腺癌中TP53突变可能位置方面的重要程度,分析了AID/APOBEC家族胞嘧啶脱氨酶的ssDNA靶标特异性所导致的密码子偏好模式。数据表明,密码子上下文强烈影响AID/APOBEC1/APOBEC3G基序以及WA位点处突变的可能位置。一个意外发现是,在突变密码子(从3'到5'读取)中,胞嘧啶向鸟嘌呤的转换高度显著地倾向于发生在第一个核苷酸位置,而鸟嘌呤向胞嘧啶的转换则倾向于发生在第二个核苷酸位置。因此,所涉及的机制似乎对密码子阅读框敏感,并且在开放的“转录泡”背景下具有区分非转录链和转录链上胞嘧啶的内在能力。

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