Pre-ciliated tubal epithelial cells are prone to initiation of high-grade serous ovarian carcinoma

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Abstract

The distal region of the uterine (Fallopian) tube is commonly associated with high-grade serous carcinoma (HGSC), the predominant and most aggressive form of ovarian or extra-uterine cancer. Specific cell states and lineage dynamics of the adult tubal epithelium (TE) remain insufficiently understood, hindering efforts to determine the cell of origin for HGSC. Here, we report a comprehensive census of cell types and states of the mouse uterine tube. We show that distal TE cells expressing the stem/progenitor cell marker Slc1a3 can differentiate into both secretory ( Ovgp1 +) and ciliated ( Fam183b +) cells. Inactivation of Trp53 and Rb1 , whose pathways are commonly altered in HGSC, leads to elimination of targeted Slc1a3 + cells by apoptosis, thereby preventing their malignant transformation. In contrast, pre-ciliated cells ( Krt5 +, Prom1+ , Trp73 +) remain cancer-prone and give rise to serous tubal intraepithelial carcinomas and overt HGSC. These findings identify transitional pre-ciliated cells as a previously unrecognized cancer-prone cell state and point to pre-ciliation mechanisms as novel diagnostic and therapeutic targets.

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