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Molecular characteristics by race and ethnicity of patients with high tumor mutational burden, high microsatellite instability, and mismatch repair deficiency: Real-world data from the multi-institutional Endometrial cancer Molecularly Targeted Therapy Consortium (ECMT2)
Journal article   Peer reviewed

Molecular characteristics by race and ethnicity of patients with high tumor mutational burden, high microsatellite instability, and mismatch repair deficiency: Real-world data from the multi-institutional Endometrial cancer Molecularly Targeted Therapy Consortium (ECMT2)

Sarah S. Lee, Angeles Alvarez Secord, Steven Friedman, Erinn M. Hade, Carson Smitherman, Nikita Bisht, Lindsay Borden, Amanda L. Jackson, Floor Backes, Premal Thaker, …
Gynecologic oncology, Vol.199, pp.152-158
08/01/2025
DOI: https://doi.org/10.1016/j.ygyno.2025.07.006
PMID: 40651147

Abstract

Endometrial cancer Microsatellite instability Mismatch, repair deficiency Tumor mutational burden
Mismatch repair deficiency (dMMR), high microsatellite instability (MSI-H), and high tumor mutation burden (TMB-H) are predictive and prognostic biomarkers in endometrial cancer. We aimed to characterize the racial/ethnic distribution of molecular markers and the clinical characteristics among endometrial cancer patients with TMB-H and MSI-H/dMMR. The Endometrial Cancer Molecularly Targeted Therapy Consortium is a centrally verified clinical and molecular repository. Patients with endometrial cancer who underwent tumor profiling were included. TMB-H was defined as ≥10–12 mutations per megabase. MSI-H was determined by next-generation sequencing or polymerase chain reaction, and dMMR by loss of MLH1, MSH2, MSH6, or PMS2 on immunohistochemistry. Tumor biomarker positivity was defined as TMB-H and/or MSI-H/dMMR. Overall survival was assessed using Kaplan-Meier and Cox proportional hazard models. Among 742 patients, 22 % (n = 164) were biomarker positive: 12 % (n = 87) had both TMB-H and MSI-H/dMMR, 8 % (n = 63) had MSI-H/dMMR alone, and 2 % (n = 14) had 14 TMB-H alone. Only 9 % of non-Hispanic Black patients had biomarker positive tumors compared to 26 % of patients from other racial/ethnic groups. Pathogenic POLE mutations were rare (<1 %, n = 5). Patients with TMB-H had a higher proportion of high-risk histologies (43 %) than those with MSI-H/dMMR (24 %). Biomarker positive tumors were associated with a lower risk of death compared to biomarker negative tumors (aHR 0.63, 95 % CI: 0.46, 0.88). Less than 10 % of non-Hispanic Black patients with endometrial cancer had TMB-H and/or MSI-H/dMMR, and biomarker positivity was associated with improved survival. Prospective studies are necessary to elucidate how these molecular differences impact treatment and outcomes. •22 % of patients with endometrial cancers had tumors that were either TMB-H and/or MSI-H.•8 % of endometrial cancer tumors had MSI-H/dMMR without TMB-H, and 2 % had TMB-H without MSI-H/dMMR.•Non-Hispanic Black patients were less likely to have biomarker positive tumors (TMB-H and/or MSI-H/dMMR tumors).•TMB-H and/or MSI-H/dMMR was associated with improved survival compared to those that were biomarker negative.

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