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Systemic administration of an RNA binding and cell-­ penetrating antibody targets therapeutic RNA to multiple mouse models of cancer

Science Translation Medicine. 2025-07; 
Elias Quijano, Diana Martinez-Saucedo, Zaira Ianniello, Natasha Pinto-Medici, Madison Rackear, Haoting Chen, Luiz Lola-Pereira, Yanfeng Liu, Denise Hegan, Xinning Shan, Robert Tseng, Deanne Yugawa, Sumedha Chowdhury, Minsoo Khang, Jay P Singh, Rashed Abdullah, Perisa Azhir, Soki Kashima, Wendy S Woods, Nicholas Gosstola, Bruce C Turner, Stephen Squinto, Dale L Ludwig, Ranjit S Bindra, Marie E Robert, David A Braun, Pablo Perez Pinera, W Mark Saltzman, Luisa F Escobar-Hoyos, Peter M Glazer
Products/Services Used Details Operation
Recombinant Antibody Expression TMAB1, TMAB3, and TMAB3h antibodies were synthesized by GenScript using codon-optimized expression vectors for individual light and heavy chains in pcDNA3.4 (for example,pTMAB3-HC and pTMAB3-LC) transfected into Chinese hamster ovary (CHO)–K1SP cells (a version of CHO cells from GenScript) grown in chemically defined CHO medium + 25 μM L-S--S-methylsulfoximine (Sigma-Aldrich) + anti-clumping agent (200×). Antibodies were purified by protein A, eluted with Pierce Gentle Elution Buffer (pH 6.5), Get A Quote
Stable Cell Lines Get A Quote

Abstract

There is intense interest in the advancement of RNAs as rationally designed therapeutic agents, especially in oncology, where a major focus is to use RNAs to stimulate pattern recognition receptors to leverage innate immune responses. However, the inability to selectively deliver therapeutic RNAs within target cells after intravenous administration now hinders the development of this type of treatment for cancer and other disorders. Here, we found that a tumor-targeting, cell-penetrating, and RNA binding monoclonal antibody, TMAB3, can form stable, noncovalent antibody/RNA complexes of a discrete size that mediate highly specific and functional delivery of RNAs into tumors. Using 3p-hpRNA, an agonist of the pat... More

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