POLE-Mutated Uterine Carcinosarcomas: A Clinicopathologic and Molecular Study of 11 Cases

Phoebe M Hammer; Amir Momeni-Boroujeni; David L Kolin; Leandra Kingsley; Ann Folkins; Rachel L P Geisick; Chandler Ho; Carlos J Suarez; Brooke E Howitt

doi:10.1016/j.modpat.2024.100676

POLE-Mutated Uterine Carcinosarcomas: A Clinicopathologic and Molecular Study of 11 Cases

Mod Pathol. 2024 Nov 29;38(3):100676. doi: 10.1016/j.modpat.2024.100676. Online ahead of print.

Authors

Phoebe M Hammer¹, Amir Momeni-Boroujeni², David L Kolin³, Leandra Kingsley¹, Ann Folkins¹, Rachel L P Geisick¹, Chandler Ho¹, Carlos J Suarez¹, Brooke E Howitt⁴

Affiliations

¹ Department of Pathology, Stanford University School of Medicine, Stanford, California.
² Department of Pathology, Memorial Sloan Kettering Cancer Center, New York, New York.
³ Division of Women's and Perinatal Pathology, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts.
⁴ Department of Pathology, Stanford University School of Medicine, Stanford, California. Electronic address: [email protected].

PMID: 39615841
DOI: 10.1016/j.modpat.2024.100676

Abstract

Uterine carcinosarcomas (UCS) are high-grade biphasic neoplasms with generally poor outcomes. Based on The Cancer Genome Atlas molecular classification of endometrial carcinomas, the majority of UCS are classified as copy-number high/serous-like (p53-abnormal); however, a small subset represent other molecular subtypes, including those that harbor POLE mutations. We identified 11 POLE-mutated (POLEmut) UCS across 3 institutions and assessed the clinical, histopathologic, immunohistochemical, and molecular features of these tumors. POLEmut UCS occurred in adult women (median age, 64 years; range, 48-79 years) and usually presented as The International Federation of Gynecology and Obstetrics 2009 clinical stage IA (n = 4) or IB (n = 3). Almost all tumors were predominantly carcinomatous (n = 10), with most showing endometrioid morphology (n = 7), followed by ambiguous (n = 4) and serous (n = 3) histotypes. By immunohistochemistry, 7 tumors showed aberrant or subclonally aberrant expression of p53, 6 of which harbored pathogenic mutations in TP53 by sequencing. Other frequent mutations included PIK3CA (10/11), PTEN (8/11), RB1 (7/11), ARID1A (7/11), ATM (6/11), PIK3RA (5/11), and FBXW7 (4/11). Two tumors demonstrated loss of mismatch repair protein expression, and 1 had subclonal loss. Heterologous differentiation was uncommon, and only chondrosarcomatous type (n = 2) was observed. Mean and median follow-ups were 24.3 and 14.1 months, respectively (range, 1.4-61.1 months). Ten patients (91%) had no recurrences or death from disease, although 3 of these had follow-up periods <1 year. One patient, with the subclonal POLE variant, presented with stage IV disease and died 1.4 months after surgery. In conclusion, POLEmut UCS demonstrate unique morphologic and immunohistochemical features compared with their p53-abnormal counterparts and may have significant prognostic differences. Our study supports full molecular classification of UCS. We also raise awareness for potentially assessing POLE mutation allele frequency and clonality in consideration of classifying a tumor as POLEmut.

Keywords: POLE; endometrial carcinoma; molecular classification of endometrial carcinomas; uterine carcinosarcoma.