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脑肿瘤的临床病理特征与 TP53 突变的存在和模式相关:来自 IARC TP53 数据库的证据。

Clinicopathologic characteristics of brain tumors are associated with the presence and patterns of TP53 mutations: evidence from the IARC TP53 Database.

机构信息

N.I. Vavilov Institute of General Genetics, Russian Academy of Sciences, 3 Gubkin Street, 117971, Moscow, Russia,

出版信息

Neuromolecular Med. 2014 Jun;16(2):431-47. doi: 10.1007/s12017-014-8290-1. Epub 2014 Jan 31.

Abstract

Biological diversity in the development and progression of brain tumors may be based on the consequences of the nature of the TP53 mutation in the cancer sample. This study was designed to estimate the possible impact of the presence and spectrum of TP53 mutations on clinical variability of brain tumors using the IARC TP53 Database (R17). Somatic and germline mutation patterns differ in brain tumor carriers. The most frequent mutation in sporadic brain tumors is mutation R273C, which is relatively rare in grade 4 tumors compared with lower-grade tumors (p = 1.2 × 10(-5), OR 0.43, 95% CI 0.29-0.63). Mutations at all hot spots, DNA contact mutations, and mutations in the conserved regions of the TP53 gene are also more common in grade 1-3 tumors than in grade 4 tumors. The frequencies of missense mutations at hotspot codons and DNA contact mutations gradually decrease in all three age groups studied, indicating the role of these mutations in early-onset tumors. The role of TP53 somatic mutations in the development of brain tumors has been elucidated in the individual-participant meta-analysis that provided, for the first time, strong evidence that mean age at the onset of sporadic brain tumor is significantly lower in patients with mutated compared with wild-type TP53 in all groups stratified by tumor grade. The presence and patterns of TP53 mutations are associated mainly with the age at the onset and with the development of less malignant brain tumors. Malignant degeneration of brain tumors may depend on other genetic determinants.

摘要

脑肿瘤发生和发展过程中的生物多样性可能基于癌症样本中 TP53 突变的性质所产生的后果。本研究旨在使用 IARC TP53 数据库(R17)评估 TP53 突变的存在和谱对脑肿瘤临床变异性的可能影响。脑肿瘤携带者的体细胞和种系突变模式存在差异。散发性脑肿瘤中最常见的突变是 R273C 突变,与低级别肿瘤相比,它在 4 级肿瘤中相对较少见(p = 1.2×10(-5),OR 0.43,95%CI 0.29-0.63)。所有热点、DNA 接触突变和 TP53 基因保守区的突变在 1-3 级肿瘤中也比在 4 级肿瘤中更为常见。所有三个研究年龄组中,热点密码子错义突变和 DNA 接触突变的频率逐渐降低,表明这些突变在早发性肿瘤中起作用。个体参与者荟萃分析阐明了 TP53 体细胞突变在脑肿瘤发生中的作用,该分析首次提供了强有力的证据,表明与野生型 TP53 相比,突变型 TP53 患者的散发性脑肿瘤发病年龄在所有按肿瘤分级分层的组中显著降低。TP53 突变的存在和模式主要与发病年龄和较少恶性脑肿瘤的发展相关。脑肿瘤的恶性转化可能取决于其他遗传决定因素。

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