| Literature DB >> 34876527 |
Chih-Wei Lin1,2, Yu-Jen Wang2,3, Ting-Yen Lai2, Tsui-Ling Hsu2, Shin-Ying Han2, Han-Chung Wu4, Chia-Ning Shen2, Van Dang5, Ming-Wei Chen5, Lan-Bo Chen5,6, Chi-Huey Wong7,2.
Abstract
Pancreatic cancer is usually asymptomatic in the early stages; the 5-y survival rate is around 9%; and there is a lack of effective treatment. Here we show that SSEA-4 is more expressed in all pancreatic cancer cell lines examined but not detectable in normal pancreatic cells; and high expression of SSEA-4 or the key enzymes B3GALT5 + ST3GAL2 associated with SSEA-4 biosynthesis significantly lowers the overall survival rate. To evaluate potential new treatments for pancreatic cancer, homogeneous antibodies with a well-defined Fc glycan for optimal effector functions and CAR-T cells with scFv construct designed to target SSEA-4 were shown highly effective against pancreatic cancer in vitro and in vivo. This was further supported by the finding that a subpopulation of natural killer (NK) cells isolated by the homogeneous antibody exhibited enhancement in cancer-cell killing activity compared to the unseparated NK cells. These results indicate that targeting SSEA-4 by homologous antibodies or CAR-T strategies can effectively inhibit cancer growth, suggesting SSEA-4 as a potential immunotherapy target for treating pancreatic disease.Entities:
Keywords: CAR-T; SSEA-4 expression; homogeneous antibody; pancreatic cancer
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Year: 2021 PMID: 34876527 PMCID: PMC8685897 DOI: 10.1073/pnas.2114774118
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 12.779