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. 2020 Jan;1(1):86-98.
doi: 10.1038/s43018-019-0004-z. Epub 2019 Nov 18.

Trispecific antibodies enhance the therapeutic efficacy of tumor-directed T cells through T cell receptor co-stimulation

Lan Wu #  1 Edward Seung #  1 Ling Xu  1 Ercole Rao  2 Dana M Lord  1 Ronnie R Wei  1 Virna Cortez-Retamozo  1 Beatriz Ospina  1 Valeriya Posternak  1 Gregory Ulinski  1 Peter Piepenhagen  1 Elisa Francesconi  3 Nizar El-Murr  3 Christian Beil  2 Patrick Kirby  1 Aiqun Li  1 Jennifer Fretland  1 Rita Vicente  3 Gejing Deng  1 Tarik Dabdoubi  3 Beatrice Cameron  3 Thomas Bertrand  3 Paul Ferrari  3 Stéphanie Pouzieux  3 Cendrine Lemoine  3 Catherine Prades  3 Anna Park  1 Huawei Qiu  1 Zhili Song  1 Bailin Zhang  1 Fangxian Sun  1 Marielle Chiron  3 Srinivas Rao  1 Katarina Radošević  3 Zhi-Yong Yang  4 Gary J Nabel  5
Affiliations

Trispecific antibodies enhance the therapeutic efficacy of tumor-directed T cells through T cell receptor co-stimulation

Lan Wu et al. Nat Cancer. 2020 Jan.

Abstract

Despite the significant therapeutic advances provided by immune-checkpoint blockade and chimeric antigen receptor T cell treatments, many malignancies remain unresponsive to immunotherapy. Bispecific antibodies targeting tumor antigens and activating T cell receptor signaling have shown some clinical efficacy; however, providing co-stimulatory signals may improve T cell responses against tumors. Here, we developed a trispecific antibody that interacts with CD38, CD3 and CD28 to enhance both T cell activation and tumor targeting. The engagement of both CD3 and CD28 affords efficient T cell stimulation, whereas the anti-CD38 domain directs T cells to myeloma cells, as well as to certain lymphomas and leukemias. In vivo administration of this antibody suppressed myeloma growth in a humanized mouse model and also stimulated memory/effector T cell proliferation and reduced regulatory T cells in non-human primates at well-tolerated doses. Collectively, trispecific antibodies represent a promising platform for cancer immunotherapy.

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