Integrating Pathology, Chromosomal Instability and Mutations for Risk Stratification in Early-stage Endometrioid Endometrial Carcinoma

Overview

Journal Cell Biosci

Publisher Biomed Central

Specialty Biology

Date 2020 Oct 28

PMID 33110489

Citations 3

Authors

Yuan Li

Jiaqi Li

Ensong Guo

Jia Huang

Guangguang Fang

Shaohua Chen

Bin Yang

Yu Fu

Fuxia Li

Zizhuo Wang

Rourou Xiao

Chen Liu

Yuhan Huang

Xue Wu

Funian Lu

Lixin You

Ling Feng

Ling Xi

Peng Wu

Ding Ma

Chaoyang Sun

Beibei Wang

Gang Chen

Affiliations

Soon will be listed here.

Abstract

Background: Risk stratifications for endometrial carcinoma (EC) depend on histopathology and molecular pathology. Histopathological risk stratification lacks reproducibility, neglects heterogeneity and contributes little to surgical procedures. Existing molecular stratification is useless in patients with specific pathological or molecular characteristics and cannot guide postoperative adjuvant radiotherapies. Chromosomal instability (CIN), the numerical and structural alterations of chromosomes resulting from ongoing errors of chromosome segregation, is an intrinsic biological mechanism for the evolution of different prognostic factors of histopathology and molecular pathology and may be applicable to the risk stratification of EC.

Results: By analyzing CIN25 and CIN70, two reliable gene expression signatures for CIN, we found that EC with unfavorable prognostic factors of histopathology or molecular pathology had serious CIN. However, the POLE mutant, as a favorable prognostic factor, had elevated CIN signatures, and the CTNNB1 mutant, as an unfavorable prognostic factor, had decreased CIN signatures. Only if these two mutations were excluded were CIN signatures strongly prognostic for outcomes in different adjuvant radiotherapy subgroups. Integrating pathology, CIN signatures and POLE/CTNNB1 mutation stratified stageIendometrioid EC into four groups with improved risk prognostication and treatment recommendations.

Conclusions: We revealed the possibility of integrating histopathology and molecular pathology by CIN for risk stratification in early-stage EC. Our integrated risk model deserves further improvement and validation.

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