PLK3 amplification and tumor immune microenvironment of metastatic tumors are linked to adjuvant treatment outcomes in uterine serous cancer

Author:

Jones Wendell1ORCID,Tait David2,Livasy Chad3,Ganapathi Mahrukh2,Ganapathi Ram2

Affiliation:

1. Bioinformatics, Q2 Solutions Genomics , Durham , NC, USA

2. Levine Cancer Institute, Atrium Health , Charlotte , NC, USA

3. Carolinas Pathology Group , Charlotte , NC, USA

Abstract

Abstract Uterine serous carcinoma (USC), an aggressive variant of endometrial cancer representing approximately 10% of endometrial cancer diagnoses, accounts for ∼39% of endometrial cancer-related deaths. We examined the role of genomic alterations in advanced-stage USC associated with outcome using paired primary-metastatic tumors (n = 29) treated with adjuvant platinum and taxane chemotherapy. Comparative genomic analysis of paired primary-metastatic patient tumors included whole exome sequencing and targeted gene expression. Both PLK3 amplification and the tumor immune microenvironment (TIME) in metastatic tumors were linked to time-to-recurrence (TTR) risk without any such association observed with primary tumors. TP53 loss was significantly more frequent in metastatic tumors of platinum-resistant versus platinum-sensitive patients and was also associated with increased recurrence and mortality risk. Increased levels of chr1 breakpoints in USC metastatic versus primary tumors co-occur with PLK3 amplification. PLK3 and the TIME are potential targets for improving outcomes in USC adjuvant therapy.

Funder

Atrium Health Foundation

Publisher

Oxford University Press (OUP)

Subject

General Medicine

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