Identification of functional and diverse circulating cancer‐associated fibroblasts in metastatic castration‐naïve prostate cancer patients

Author:

Booijink Richell1,Terstappen Leon W. M. M.23ORCID,Dathathri Eshwari2ORCID,Isebia Khrystany4ORCID,Kraan Jaco4,Martens John4ORCID,Bansal Ruchi1ORCID

Affiliation:

1. Personalized Diagnostics and Therapeutics, Department of Bioengineering Technologies, Technical Medical Centre, Faculty of Science and Technology University of Twente Enschede The Netherlands

2. Department of Medical Cell BioPhysics, Technical Medical Centre, Faculty of Science and Technology University of Twente Enschede The Netherlands

3. Department of General, Visceral and Pediatric Surgery University Hospital Düsseldorf, Heinrich‐Heine University Germany

4. Department of Medical Oncology Erasmus MC Cancer Institute, University Medical Center Rotterdam The Netherlands

Abstract

In prostate cancer (PCa), cancer‐associated fibroblasts (CAFs) promote tumor progression, drug resistance, and metastasis. Although circulating tumor cells are studied as prognostic and diagnostic markers, little is known about other circulating cells and their association with PCa metastasis. Here, we explored the presence of circulating CAFs (cCAFs) in metastatic castration‐naïve prostate cancer (mCNPC) patients. cCAFs were stained with fibroblast activation protein (FAP), epithelial cell adhesion molecule (EpCAM), and receptor‐type tyrosine‐protein phosphatase C (CD45), then FAP+EpCAM cCAFs were enumerated and sorted using fluorescence‐activated cell sorting. FAP+EpCAM cCAFs ranged from 60 to 776 (389 mean ± 229 SD) per 2 × 108 mononuclear cells, whereas, in healthy donors, FAP+ EpCAM cCAFs ranged from 0 to 71 (28 mean ± 22 SD). The mCNPC‐derived cCAFs showed positivity for vimentin and intracellular collagen‐I. They were viable and functional after sorting, as confirmed by single‐cell collagen‐I secretion after 48 h of culturing. Two cCAF subpopulations, FAP+CD45 and FAP+CD45+, were identified, both expressing collagen‐I and vimentin, but with distinctly different morphologies. Collectively, this study demonstrates the presence of functional and viable circulating CAFs in mCNPC patients, suggesting the role of these cells in prostate cancer.

Funder

Techmed Centre, University of Twente

KWF Kankerbestrijding

Publisher

Wiley

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