TP53 Gain-of-Function Mutation is a Poor Prognostic Factor in High-Methylated Metastatic Colorectal Cancer

IF 4.3 3区材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC

ACS Applied Electronic Materials Pub Date : 2023-09-01 DOI:10.1016/j.clcc.2023.06.001

Shonosuke Wakayama , Kota Ouchi , Shin Takahashi , Yasuhide Yamada , Yoshito Komatsu , Ken Shimada , Tatsuro Yamaguchi , Hidekazu Shirota , Masanobu Takahashi , Chikashi Ishioka

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Abstract

Background

Neither TP53 mutation nor DNA methylation status has been established as a biomarker alone of metastatic colorectal cancer. We analyzed the association between TP53 mutation functional subtypes and genome-wide DNA methylation status (GWMS) as combined prognostic markers.

Methods

Patient clinical data were obtained from the TRICOLORE study, a randomized phase III trial. The TP53 mutations were classified into wild-type, gain-of-function (GOF) mutations, and non-gain-of-function (non-GOF) mutations. GWMS of the tumor tissues classified them into high-methylated colorectal cancer (HMCC) and low-methylated colorectal cancer (LMCC). Overall survival (OS) was compared based on these subgroups.

Results

Of the 209 patients, 60 (28.7%) were HMCC and 149 (71.3%) were LMCC, 35 (16.7%) were TP53 wild-type and 174 (83.3%) were TP53 mutants including 79 (45.4%) GOF mutations and 95 (54.6%) non-GOF mutations. The OS of the HMCC group was shorter than that of the LMCC group (median 25.3 vs. 40.3 months, P < .001, hazard ratio 1.87) in the total cohort. The combined subgroup analyses of GWMS and TP53 mutation subtypes showed that the HMCC/GOF group had significantly shorter OS than the HMCC/non-GOF group, the LMCC/GOF group, and the LMCC/non-GOF group (median 17.7; 35.3, 40.3, and 41.2 months, P = .007, P < .001, and P < .001, respectively), regardless of the primary tumor location. By the multivariate analysis, only HMCC (P = .009) was a poor prognostic factor in the GOF mutation group.

Conclusions

TP53 GOF with HMCC is a newly identified poorest prognostic molecular subset in metastatic colorectal cancer.

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TP53功能获得突变是癌症高甲基转移结直肠癌的预后不良因素

背景TP53突变和DNA甲基化状态均未被确定为转移性癌症的单独生物标志物。我们分析了TP53突变功能亚型与全基因组DNA甲基化状态（GWMS）作为联合预后标志物之间的关系。方法患者的临床数据来自TRICOLORE研究，一项随机的III期试验。TP53突变分为野生型、功能获得（GOF）突变和非功能获得（非GOF）变异。肿瘤组织GWMS将其分为高甲基化癌症（HMCC）和低甲基化癌症（LMCC）。根据这些亚组比较总生存率（OS）。结果209例患者中，60例（28.7%）为HMCC，149例（71.3%）为LMCC，35例（16.7%）为TP53野生型，174例（83.3%）为TP五十三突变体，其中GOF突变79例（45.4%），非GOF突变95例（54.6%）。在整个队列中，HMCC组的OS比LMCC组短（中位数为25.3个月对40.3个月，P<；.001，危险比1.87）。GWMS和TP53突变亚型的联合亚组分析显示，无论原发肿瘤的位置如何，HMCC/GOF组的OS明显短于HMCC/非GOF组、LMCC/GOF组和LMCC/No-GOF组（中位数分别为17.7、35.3、40.3和41.2个月，P=0.007、P<；.001和P<；0.001）。通过多变量分析，只有HMCC（P=.009）是GOF突变组的不良预后因素。结论sTP53 GOF伴HMCC是转移性癌症最差预后分子亚群。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

ACS Applied Electronic Materials Multiple-

CiteScore

7.20

自引率

4.30%

发文量

567