Molecular substratification of endometrial carcinomas with no special molecular profile (NSMP) by using a limited NGS custom panel may facilitate effective patient selection for the PIK3CA-targeted therapy
Ondrej Ondič, Květoslava Michalová, Marián Švajdler, Jiří Presl, Jan Kosťun, Veronika Hájková, Petr Martínek, Michal Michal

TL;DR
This study shows that a limited NGS panel can identify PIK3CA mutations in endometrial carcinomas, helping select patients for targeted therapy.
Contribution
The study introduces a practical NGS panel for molecular stratification of NSMP endometrial carcinomas to guide PIK3CA-targeted therapy.
Findings
30% of NSMP EC cases had PIK3CA mutations.
79% of PIK3CA-mutated cases had at least one additional oncogenic mutation.
A limited NGS panel effectively identifies relevant mutations in EC tissue.
Abstract
Endometrial carcinomas (EC) of no special molecular profile (NSMP) represent the largest molecular category of EC, comprising a mixture of tumors with different histology and molecular profiles. These facts likely point to different tumor biology, clinical outcomes, and targeted therapy responses within this molecular category. The PIK3CA is currently the only targetable kinase oncoprotein directly implicated in EC carcinogenesis. Investigating a unique single-institution cohort, we attempted to stratify NSMP ECs based on the presence of the PIK3CA pathogenic mutation. Those cases were further analyzed for other well-established-associated oncogenic driver gene mutations. Histological and clinical variables were also correlated in each case. Altogether, 175 ECs were prospectively tested by a limited custom NGS panel containing ARID1A, BCOR, BRCA1, BRCA2, CTNNB1, KRAS, MLH1, MSH2, MSH6,…
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Taxonomy
TopicsOvarian cancer diagnosis and treatment · Cancer Mechanisms and Therapy · Chromatin Remodeling and Cancer
