| Literature DB >> 33708358 |
Xiaowen Mao1, Longyin Zhou1, Sze Keong Tey1, Angel Po Yee Ma1, Cherlie Lot Sum Yeung1, Tung Him Ng1, Samuel Wan Ki Wong1, Bonnie Hei Man Liu1, Yi Man Eva Fung2, Edward F Patz3,4, Peihua Cao5,6, Yi Gao6,7,8,9, Judy Wai Ping Yam1,6,10.
Abstract
The complement system is involved in the immunosurveillance of pathogens and tumour cells. Proteomic profiling revealed that extracellular vesicles (EVs) released by metastatic hepatocellular carcinoma (HCC) cells contained a significant number of complement proteins. Complement Factor H (CFH), an abundant soluble serum protein that inhibits the alternative complement pathway, was found to be highly expressed in EVs of metastatic HCC cell lines. Here, we investigated the functional role of EV-CFH and explored the therapeutic efficacy of targeting EV-CFH with an anti-CFH antibody in HCC. The results showed that EVs that are enriched in CFH promoted HCC cell growth, migration, invasiveness and enhanced liver tumour formation in mice. EV-CFH also promoted metastasis, which was significantly abrogated when treated with an anti-CFH antibody. These findings demonstrate an unexplored function of EV-CFH in protecting HCC cells by evading complement attack, thereby facilitating tumorigenesis and metastasis. Lastly, we demonstrated the therapeutic efficacy of an anti-CFH antibody in suppressing tumour formation in a syngeneic mouse model. This study suggests a new therapeutic strategy for HCC, by inhibiting EV-CFH with a tumour specific anti-CFH antibody.Entities:
Keywords: Complement Factor H; complement‐mediated cytotoxicity; extracellular vesicles; hepatocellular carcinoma
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Year: 2020 PMID: 33708358 PMCID: PMC7890557 DOI: 10.1002/jev2.12031
Source DB: PubMed Journal: J Extracell Vesicles ISSN: 2001-3078