Neoadjuvant chemotherapy induces phenotypic mast cell changes in high grade serous ovarian cancer

Julia McAdams; Jasmine Ebott; Corinne Jansen; Chloe Kim; Daniela Maiz; Joyce Ou; Linda C. Hanley; Payton De La Cruz; Nicole E. James

doi:10.1186/s13048-024-01516-y

Journal of Ovarian Research (Sep 2024)

Neoadjuvant chemotherapy induces phenotypic mast cell changes in high grade serous ovarian cancer

Julia McAdams,
Jasmine Ebott,
Corinne Jansen,
Chloe Kim,
Daniela Maiz,
Joyce Ou,
Linda C. Hanley,
Payton De La Cruz,
Nicole E. James

Affiliations

Julia McAdams: Program in Women’s Oncology, Women and Infants Hospital
Jasmine Ebott: Program in Women’s Oncology, Women and Infants Hospital
Corinne Jansen: Program in Women’s Oncology, Women and Infants Hospital
Chloe Kim: School of Public Health, Brown University
Daniela Maiz: Department of Pathobiology, Brown University
Joyce Ou: Department of Pathology, Women and Infants Hospital
Linda C. Hanley: Department of Pathology, Women and Infants Hospital
Payton De La Cruz: Department of Pathobiology, Brown University
Nicole E. James: Program in Women’s Oncology, Women and Infants Hospital

DOI: https://doi.org/10.1186/s13048-024-01516-y
Journal volume & issue: Vol. 17, no. 1
pp. 1 – 12

Abstract

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Abstract Background High grade serous ovarian cancer (HGSOC) is the most lethal gynecologic malignancy in which patients have still yet to respond meaningfully to clinically available immunotherapies. Hence, novel immune targets are urgently needed. Our past work has identified that mast cells are significantly upregulated at the mRNA level in HGSOC patient tumors following neoadjuvant chemotherapy (NACT) exposure. Therefore, in this current investigation we sought to characterize intratumoral mast cell phenotypic changes as a result of NACT exposure and determine how these adaptations are associated with patient clinical outcomes. Methods Hematologic immunohistochemistry was employed to determine mast cell levels in 36 matched pre- and post-NACT HGSOC patient tumors. Fluorescent Immunohistochemistry was utilized to identify Tryptase+(carboxypeptidase A3 (CPA3) + mast cells as well as histamine levels in 29 and 20, respectively, matched pre- and post-NACT HGSOC patient tumors. Finally, human immortalized mast cells, LUVA were stimulated with carboplatin and paclitaxel and genomic changes were analyzed by quantitative PCR. Results Hematologic labeled intratumoral mast cells were significantly upregulated in the intraepithelial and stromal regions of the tumor, post-NACT. Lower levels of pre-NACT mast cells were significantly associated with an improved progression-free survival (PFS). Histamine, a marker of mast cell degranulation was similarly upregulated in post-NACT exposed tumors. Through the characterization of mast cell specific proteases Tryptase and CPA3, it was found that Tryptase+/ CPA3 + mast cells were significantly upregulated both in the intraepithelial and stromal compartments of the tumor, while Tryptase + cells were significantly upregulated in the stromal regions of the tumor. Lower post-NACT treated levels with Tryptase+/ CPA3 + cells were significantly associated with improved overall survival (OS) and PFS while higher Tryptase + mast cells were associated with improved OS. Finally, following chemotherapy exposure mast cell activating factors AREG and CCL2 were significantly upregulated while TGFB1, an inhibitor of mast cell activation was downregulated in LUVA cells. Conclusions Enhanced mast cell numbers, as well as activation and degranulation are a consequence of NACT exposure. Post-NACT mast cells displayed differing associations with survival outcomes that was dependent upon granule classification. Ultimately, mast cells represent a clinically relevant putative HGSOC immune target.

Published in Journal of Ovarian Research

ISSN: 1757-2215 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Gynecology and obstetrics
Website: https://ovarianresearch.biomedcentral.com/

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