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. 2024 Dec:134:144-161.
doi: 10.1016/j.matbio.2024.10.006. Epub 2024 Oct 13.

Fibroblast integrin α11β1 is a collagen assembly receptor in mechanoregulated fibrillar adhesions

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Free article

Fibroblast integrin α11β1 is a collagen assembly receptor in mechanoregulated fibrillar adhesions

Moses Musiime et al. Matrix Biol. 2024 Dec.
Free article

Abstract

Solid epithelial cancers with significant desmoplasia are characterized by an excessive deposition of collagen-based matrix, which often supports tumor progression. However, the mechanism of how collagen receptors mediate collagen fibrillogenesis still remains mostly unclear. We show that the collagen-binding integrin α11β1 can co-localize with tensin-1 and deposited collagen I in human pancreatic ductal adenocarcinoma (PDAC) stroma. In addition to the canonical fibrillar adhesion integrin α5β1 expressed by human PDAC cancer-associated fibroblasts (CAFs), tensin-1-positive fibrillar adhesions contained α11β1 but lacked α1β1 and α2β1. CAFs lacking α5β1 expression displayed mechanoregulated and tensin-1 dependent α11β1 fibrillar adhesions, suggesting independent roles of the two integrins with regards to fibrillar adhesions-based de novo fibrillogenesis. Further, we demonstrate that cell surface-associated collagen I assembly necessitated α11β1, but not α5β1 expression. In summary, α11β1 integrin is a novel component of fibrillar adhesions, which is strategically positioned to mediate de novo collagen fibrillogenesis at the cell surface under pro-fibrotic conditions.

Keywords: Cancer-associated fibroblast; Collagen assembly; Fibrillar adhesions; Fibrosis; Integrin.

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Conflict of interest statement

Declaration of competing interest The authors declare no competing interests.

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