4.7 Editorial Material

PD-L1 Crosslinking as a New Strategy of 4-1BB Agonism Immunotherapy

CLINICAL CANCER RESEARCH (2022)

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Journal

CLINICAL CANCER RESEARCH
Volume 28, Issue 15, Pages 3182-3184

Publisher

AMER ASSOC CANCER RESEARCH
DOI: 10.1158/1078-0432.CCR-22-0541

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Categories

Oncology

Funding

  1. Department of Pathology of New York University Grossman School of Medicine (New York, NY)

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4-1BB has long been considered a promising target for cancer immunotherapy, but early targeted agents showed significant liver toxicity. A new approach is being developed to circumvent hepatotoxicity by directing 4-1BB agonism to the tumor microenvironment using a bispecific molecule targeting the tumor-associated immune checkpoint molecule PD-L1.
4-1BB has been considered a promising target in cancer immunotherapy for decades. Nevertheless, early 4-1BB-targeted agents demonstrated significant liver immuno-toxicity. A new wave of 4-1BB-based therapy is being developed to circumvent hepatotoxicity with a bispecific molecule that directs 4-1BB agonism to the tumor microenvironment by targeting tumor-associated immune checkpoint molecule PD-L1.

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