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Ciliated Cells in Ovarian Cancer Decrease with Increasing Tumor Grade and Disease Progression.

Authors :
Richardson, Michael
Richardson, Michael
Recouvreux, Maria
Walts, Ann
Orsulic, Sandra
Karlan, Beth
Richardson, Michael
Richardson, Michael
Recouvreux, Maria
Walts, Ann
Orsulic, Sandra
Karlan, Beth
Source :
Cells; vol 11, iss 24
Publication Year :
2022

Abstract

Ciliated cell markers expressed in epithelial ovarian cancers (EOC) are associated with improved survival. We examined the distribution of cells expressing ciliated cell markers in various EOC histologies and stages. Immunohistochemistry and/or multiplex immunofluorescence were used to determine the expression of FOXJ1 and/or CAPS (ciliated cell markers) in tissue microarrays including 4 normal fallopian tubes, 6 normal endometria, 16 cystadenomas, 25 borderline tumors, 21 low-grade carcinomas, and 118 high-grade carcinomas (HGSOC) (46 serous, 29 endometrioid, 30 clear cell, 13 mucinous). CAPS+ cells were observed in normal fallopian tubes and endometria and in ~85% of serous benign and borderline tumors and low-grade carcinomas but only in <40% of HGSOC. mRNA data from an independent cohort showed higher FOXJ1 and CAPS expression in serous borderline tumors and low-grade carcinomas compared to HGSOC. In HGSOC, ciliated cell-positive markers were observed in 52% primary tumors compared to 26% of patient-matched synchronous metastases, and 24% metachronous metastases (p = 0.009). mRNA data from an independent HGSOC cohort showed lower levels of CAPS in metastases than in primary tumors (p = 0.03). Overall, the study revealed that ciliated cells were less common in mucinous EOC, the percentage of ciliated cell marker-positive cases decreased with increasing grade, and the percentage of ciliated cells decreased in HGSOC metastases compared to patient-matched primary tumors.

Details

Database :
OAIster
Journal :
Cells; vol 11, iss 24
Notes :
application/pdf, Cells vol 11, iss 24
Publication Type :
Electronic Resource
Accession number :
edsoai.on1401040786
Document Type :
Electronic Resource