Immunohistochemistry of p53 surrogates TP53 mutation as an accurate predictor for early-relapse of surgically resected stage I-III lung adenocarcinoma

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Abstract

Introduction

TP53 is a strong tumor suppressor gene; its deactivation contributes to carcinogenesis and influences clinical outcomes. However, the prognostic influence of p53 deactivation on early relapse in patients with surgically resected non–small cell lung cancer remains unclear.

Materials and methods

A cohort of 170 patients with primary stage I through III lung adenocarcinoma (LADC) and lung squamous cell carcinoma who underwent complete resection at Tokyo Medical and Dental University was screened for TP53 mutations using panel testing, and association studies between TP53 mutations and clinical data, including histology and postoperative recurrence, were performed. The association between TP53 mutations and postoperative recurrence was validated using data from 604 patients with MSK-IMPACT from The Cancer Genome Atlas. Additional immunohistochemistry for p53 was performed on some subsets of the Tokyo Medical and Dental University population.

Results

Mutations in TP53 were recurrently observed (35.9%; 61 out of 170) in the Tokyo Medical and Dental University cohort. In the histology-stratified analysis, patients with LADC histology showed TP53 mutations that were associated with poor relapse-free survival (log-rank test; P = .020), whereas patients with lung squamous cell carcinoma histology showed TP53 mutations that were not (P = .99). The poor prognosis of TP53 mutation-positive LADCs was validated in The Cancer Genome Atlas-LADC cohort (log-rank test; P = .0065). Additional immunohistochemistry for p53 in patients with LADC histology in the Tokyo Medical and Dental University cohort showed a significant correlation between TP53 mutations and abnormal IHC pattern of p53 (Cramer's correlation coefficient V = 0.67).

Conclusions

TP53 mutation is a potential marker for worse prognosis in surgically resected LADC; immunohistochemistry for p53 could be a surrogate method to identify patients with LADC with a worse prognosis.

p53 代理基因 TP53 突变的免疫组化是手术切除的 I-III 期肺癌早期复发的准确预测指标
导言TP53是一种强抑癌基因;其失活会导致癌变并影响临床预后。材料和方法在东京医科齿科大学接受完全切除术的 170 例原发性 I 至 III 期肺腺癌(LADC)和肺鳞癌患者队列中,使用面板测试筛查 TP53 突变,并进行 TP53 突变与临床数据(包括组织学和术后复发)之间的关联研究。利用癌症基因组图谱(The Cancer Genome Atlas)中604名MSK-IMPACT患者的数据验证了TP53突变与术后复发之间的关联。结果在东京医科齿科大学队列中反复观察到 TP53 突变(35.9%;170 例中有 61 例)。在组织学分层分析中,肺腺癌组织学患者的TP53突变与无复发生存率低有关(对数秩检验;P = .020),而肺鳞癌组织学患者的TP53突变与无复发生存率低无关(P = .99)。在癌症基因组图谱-LADC队列中验证了TP53突变阳性LADC的不良预后(对数rank检验;P = .0065)。结论TP53突变是手术切除的LADC预后较差的潜在标志物;p53免疫组化可作为一种替代方法来鉴别预后较差的LADC患者。
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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