| Literature DB >> 33998600 |
Zhen Lu1, Angelica Ortiz1, Ioannis I Verginadis2, Amy R Peck3, Farima Zahedi1, Christina Cho1, Pengfei Yu1, Rachel M DeRita1, Hongru Zhang1, Ryan Kubanoff3, Yunguang Sun4, Andrew T Yaspan4, Elise Krespan5, Daniel P Beiting5, Enrico Radaelli5, Sandra W Ryeom6, J Alan Diehl7, Hallgeir Rui4, Constantinos Koumenis2, Serge Y Fuchs1.
Abstract
Intercellular biomolecule transfer (ICBT) between malignant and benign cells is a major driver of tumor growth, resistance to anticancer therapies, and therapy-triggered metastatic disease. Here we characterized cholesterol 25-hydroxylase (CH25H) as a key genetic suppressor of ICBT between malignant and endothelial cells (ECs) and of ICBT-driven angiopoietin-2-dependent activation of ECs, stimulation of intratumoral angiogenesis, and tumor growth. Human CH25H was downregulated in the ECs from patients with colorectal cancer and the low levels of stromal CH25H were associated with a poor disease outcome. Knockout of endothelial CH25H stimulated angiogenesis and tumor growth in mice. Pharmacologic inhibition of ICBT by reserpine compensated for CH25H loss, elicited angiostatic effects (alone or combined with sunitinib), augmented the therapeutic effect of radio-/chemotherapy, and prevented metastatic disease induced by these regimens. We propose inhibiting ICBT to improve the overall efficacy of anticancer therapies and limit their prometastatic side effects.Entities:
Keywords: Colorectal cancer; Endothelial cells; Oncology; Vascular Biology
Year: 2021 PMID: 33998600 PMCID: PMC8121529 DOI: 10.1172/JCI144225
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808