| Literature DB >> 30107179 |
Gururaj Shivange1, Karol Urbanek1, Piotr Przanowski2, Justin S A Perry3, James Jones4, Robert Haggart4, Christina Kostka4, Tejal Patki4, Edward Stelow5, Yuliya Petrova6, Danielle Llaneza6, Marty Mayo7, Kodi S Ravichandran3, Charles N Landen6, Sanchita Bhatnagar2, Jogender Tushir-Singh8.
Abstract
Therapeutic antibodies targeting ovarian cancer (OvCa)-enriched receptors have largely been disappointing due to limited tumor-specific antibody-dependent cellular cytotoxicity. Here we report a symbiotic approach that is highly selective and superior compared with investigational clinical antibodies. This bispecific-anchored cytotoxicity activator antibody is rationally designed to instigate "cis" and "trans" cytotoxicity by combining specificities against folate receptor alpha-1 (FOLR1) and death receptor 5 (DR5). Whereas the in vivo agonist DR5 signaling requires FcγRIIB interaction, the FOLR1 anchor functions as a primary clustering point to retain and maintain a high level of tumor-specific apoptosis. The presented proof of concept study strategically makes use of a tumor cell-enriched anchor receptor for agonist death receptor targeting to potentially generate a clinically viable strategy for OvCa.Entities:
Keywords: TRAIL-R2; antibody therapy; cancer; cancer signaling; caspases; cell signaling; dual-specificity targeting; folate receptor alpha-1; ovarian cancer; targeted therapies
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Year: 2018 PMID: 30107179 PMCID: PMC6404966 DOI: 10.1016/j.ccell.2018.07.005
Source DB: PubMed Journal: Cancer Cell ISSN: 1535-6108 Impact factor: 31.743