| Literature DB >> 30333240 |
Dionysos Slaga1, Diego Ellerman1, T Noelle Lombana1, Rajesh Vij1, Ji Li1, Maria Hristopoulos1, Robyn Clark1, Jennifer Johnston1, Amy Shelton1, Elaine Mai1, Kapil Gadkar1, Amy A Lo1, James T Koerber1, Klara Totpal1, Rodney Prell1, Genee Lee1, Christoph Spiess1, Teemu T Junttila2.
Abstract
A primary barrier to the success of T cell-recruiting bispecific antibodies in the treatment of solid tumors is the lack of tumor-specific targets, resulting in on-target off-tumor adverse effects from T cell autoreactivity to target-expressing organs. To overcome this, we developed an anti-HER2/CD3 T cell-dependent bispecific (TDB) antibody that selectively targets HER2-overexpressing tumor cells with high potency, while sparing cells that express low amounts of HER2 found in normal human tissues. Selectivity is based on the avidity of two low-affinity anti-HER2 Fab arms to high target density on HER2-overexpressing cells. The increased selectivity to HER2-overexpressing cells is expected to mitigate the risk of adverse effects and increase the therapeutic index. Results included in this manuscript not only support the clinical development of anti-HER2/CD3 1Fab-immunoglobulin G TDB but also introduce a potentially widely applicable strategy for other T cell-directed therapies. The potential of this discovery has broad applications to further enable consideration of solid tumor targets that were previously limited by on-target, but off-tumor, autoimmunity.Entities:
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Year: 2018 PMID: 30333240 DOI: 10.1126/scitranslmed.aat5775
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956