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临床实践中的TP53突变分析:来自慢性淋巴细胞白血病的经验教训

TP53 mutation analysis in clinical practice: lessons from chronic lymphocytic leukemia.

作者信息

Malcikova Jitka, Pavlova Sarka, Kozubik Katerina Stano, Pospisilova Sarka

机构信息

Central European Institute of Technology, Center of Molecular Medicine, and Faculty of Medicine, Department of Internal Medicine - Hematology and Oncology, Masaryk University, Brno, Czech Republic.

出版信息

Hum Mutat. 2014 Jun;35(6):663-71. doi: 10.1002/humu.22508. Epub 2014 Feb 5.

Abstract

In leukemia, TP53 mutations are not frequent but clearly associate with impaired survival and therapy response. Here, we describe the biological and clinical consequences of TP53 dysfunction as well as the methodical aspects of TP53 analysis in chronic lymphocytic leukemia (CLL). In CLL, TP53 defects are routinely analyzed as part of disease prognostication. Deletions of TP53 locus (17p) have been uniformly detected using I-FISH for several years. Since monoallelic mutations have also been shown to have negative prognostic impact, it is recommended to examine both TP53 mutations and deletions. Several methods are used to detect TP53 mutations, and next-generation sequencing (NGS) is becoming a convenient option for routine analysis. Besides this, ultradeep NGS permits the detection of minor clones carrying TP53 mutations, even below 1%. The prognostic impact of minor TP53-defective subclones is currently unknown, nevertheless they unequivocally bear the risk of being selected by therapy. Prospective studies assessing the consequences of carrying such clones are in progress.

摘要

在白血病中,TP53突变并不常见,但明显与生存受损及治疗反应相关。在此,我们描述了TP53功能障碍的生物学和临床后果以及慢性淋巴细胞白血病(CLL)中TP53分析的方法学方面。在CLL中,TP53缺陷作为疾病预后评估的一部分被常规分析。使用间期荧光原位杂交(I-FISH)检测TP53基因座(17p)缺失已经有好几年了。由于单等位基因突变也已显示出具有负面预后影响,因此建议同时检测TP53突变和缺失。有几种方法用于检测TP53突变,下一代测序(NGS)正成为常规分析的便捷选择。除此之外,超深度NGS能够检测携带TP53突变的微小克隆,甚至低于1%。携带TP53缺陷微小亚克隆的预后影响目前尚不清楚,但它们无疑具有被治疗选择的风险。评估携带此类克隆后果的前瞻性研究正在进行中。

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