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Dynamic Changes in the Extracellular Matrix in Primary, Metastatic, and Recurrent Ovarian Cancers

Authors :
Gertych, Arkadiusz
Gertych, Arkadiusz
Walts, Ann E
Cheng, Keyi
Liu, Manyun
John, Joshi
Lester, Jenny
Karlan, Beth Y
Orsulic, Sandra
Gertych, Arkadiusz
Gertych, Arkadiusz
Walts, Ann E
Cheng, Keyi
Liu, Manyun
John, Joshi
Lester, Jenny
Karlan, Beth Y
Orsulic, Sandra
Source :
Cells; vol 11, iss 23, 3769; 2073-4409
Publication Year :
2022

Abstract

Cancer-associated fibroblasts (CAFs) and their extracellular matrix are active participants in cancer progression. While it is known that functionally different subpopulations of CAFs co-exist in ovarian cancer, it is unclear whether certain CAF subsets are enriched during metastatic progression and/or chemotherapy. Using computational image analyses of patient-matched primary high-grade serous ovarian carcinomas, synchronous pre-chemotherapy metastases, and metachronous post-chemotherapy metastases from 42 patients, we documented the dynamic spatiotemporal changes in the extracellular matrix, fibroblasts, epithelial cells, immune cells, and CAF subsets expressing different extracellular matrix components. Among the different CAF subsets, COL11A1+ CAFs were associated with linearized collagen fibers and exhibited the greatest enrichment in pre- and post-chemotherapy metastases compared to matched primary tumors. Although pre- and post-chemotherapy metastases were associated with increased CD8+ T cell infiltration, the infiltrate was not always evenly distributed between the stroma and cancer cells, leading to an increased frequency of the immune-excluded phenotype where the majority of CD8+ T cells are present in the tumor stroma but absent from the tumor parenchyma. Overall, most of the differences in the tumor microenvironment were observed between primary tumors and metastases, while fewer differences were observed between pre- and post-treatment metastases. These data suggest that the tumor microenvironment is largely determined by the primary vs. metastatic location of the tumor while chemotherapy does not have a significant impact on the host microenvironment.

Details

Database :
OAIster
Journal :
Cells; vol 11, iss 23, 3769; 2073-4409
Notes :
application/pdf, Cells vol 11, iss 23, 3769 2073-4409
Publication Type :
Electronic Resource
Accession number :
edsoai.on1401039077
Document Type :
Electronic Resource