Cathelicidin suppresses colon cancer development by inhibition of cancer associated fibroblasts

Cathelicidin suppresses colon cancer development by inhibition of cancer associated fibroblasts

Cathelicidin (LL-37 in humans and mCRAMP in mice) represents a family of endogenous antimicrobial and anti-inflammatory peptides. Cancer-associated fibroblasts can promote the proliferation of colon cancer cells and growth of colon cancer tumors. We examined the role of cathelicidin in the developme...

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Veröffentlicht in:Clinical and experimental gastroenterology 2015-01, Vol.8 (default), p.13-29
Hauptverfasser: Cheng, Michelle, Ho, Samantha, Yoo, Jun Hwan, Tran, Deanna Hoang-Yen, Bakirtzi, Kyriaki, Su, Bowei, Tran, Diana Hoang-Ngoc, Kubota, Yuzu, Ichikawa, Ryan, Koon, Hon Wai
Format: Artikel
Sprache:eng
Schlagworte:
Analysis
Apoptosis
Cancer
Cancer therapies
Care and treatment
Cathelicidins
Cell growth
Colon cancer
Colorectal cancer
Dosage and administration
Drug dosages
Fibroblasts
Gastric cancer
Gastroenterology
Growth factors
Inflammatory bowel disease
Intermediate filament proteins
Laboratory animals
Medical research
Original Research
Penicillin
Peptides
Prevention
Tumors
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Zusammenfassung:Cathelicidin (LL-37 in humans and mCRAMP in mice) represents a family of endogenous antimicrobial and anti-inflammatory peptides. Cancer-associated fibroblasts can promote the proliferation of colon cancer cells and growth of colon cancer tumors. We examined the role of cathelicidin in the development of colon cancer, using subcutaneous human HT-29 colon-cancer-cell-derived tumor model in nude mice and azoxymethane- and dextran sulfate-mediated colon cancer model in C57BL/6 mice. We also determined the indirect antitumoral mechanism of cathelicidin via the inhibition of epithelial-mesenchymal transition (EMT) of colon cancer cells and fibroblast-supported colon cancer cell proliferation. Intravenous administration of cathelicidin expressing adeno-associated virus significantly reduced the size of tumors, tumor-derived collagen expression, and tumor-derived fibroblast expression in HT-29-derived subcutaneous tumors in nude mice. Enema administration of the mouse cathelicidin peptide significantly reduced the size and number of colonic tumors in azoxymethane- and dextran sulfate-treated mice without inducing apoptosis in tumors and the adjacent normal colonic tissues. Cathelicidin inhibited the collagen expression and vimentin-positive fibroblast expression in colonic tumors. Cathelicidin did not directly affect HT-29 cell viability, but did significantly reduce tumor growth factor-β1-induced EMT of colon cancer cells. Media conditioned by the human colonic CCD-18Co fibroblasts promoted human colon cancer HT-29 cell proliferation. Cathelicidin pretreatment inhibited colon cancer cell proliferation mediated by media conditioned by human colonic CCD-18Co fibroblasts. Cathelicidin disrupted tubulin distribution in colonic fibroblasts. Disruption of tubulin in fibroblasts reduced fibroblast-supported colon cancer cell proliferation. Cathelicidin effectively inhibits colon cancer development by interfering with EMT and fibroblast-supported colon cancer cell proliferation.
ISSN:1178-7023
1178-7023
DOI:10.2147/CEG.S70906