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Next-generation cell-penetrating antibodies for tumor targeting and RAD51 inhibition

Oncotarget. 2024-10; 
Madison Rackear, Elias Quijano, Zaira Ianniello, Daniel A Colón-Ríos, Adam Krysztofiak, Rashed Abdullah, Yanfeng Liu, Faye A Rogers, Dale L Ludwig, Rohini Dwivedi, Franziska Bleichert, Peter M Glazer
Products/Services Used Details Operation
Mammalian Expression Variants were designed, synthesized, expressed in Chinese hamster ovary cells, and purified following standard operating procedures (Genscript, Piscataway NJ). Complexes were generated by mixing 3E10 (250 µg) and cytosolic GFP mRNA (10 µg, Genscript) and incubating at room temperature for 10 min. Get A Quote
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摘要

Monoclonal antibody therapies for cancer have demonstrated extraordinary clinical success in recent years. However, these strategies are thus far mostly limited to specific cell surface antigens, even though many disease targets are found intracellularly. Here we report studies on the humanization of a full-length, nucleic acid binding, monoclonal lupus-derived autoantibody, 3E10, which exhibits a novel mechanism of cell penetration and tumor specific targeting. Comparing humanized variants of 3E10, we demonstrate that cell uptake depends on the nucleoside transporter ENT2, and that faster cell uptake and superior in vivo tumor targeting are associated with higher affinity nucleic acid binding. We show that one... More

关键词

3E10; RAD51; cell penetration; nucleic acid binding; nucleic acid delivery.