Synthetic Dual Co-stimulation Increases the Potency of HIT and TCR-targeted Cell Therapies

Overview

Journal Nat Cancer

Specialty Oncology

Date 2024 Mar 20

PMID 38503896

Authors

Anton Dobrin

Pieter L Lindenbergh

Yuzhe Shi

Karlo Perica

Hongyao Xie

Nayan Jain

Andrew Chow

Jedd D Wolchok

Taha Merghoub

Michel Sadelain

Mohamad Hamieh

Affiliations

Soon will be listed here.

Abstract

Chimeric antigen receptor T cells have dramatically improved the treatment of hematologic malignancies. T cell antigen receptor (TCR)-based cell therapies are yet to achieve comparable outcomes. Importantly, chimeric antigen receptors not only target selected antigens but also reprogram T cell functions through the co-stimulatory pathways that they engage upon antigen recognition. We show here that a fusion receptor comprising the CD80 ectodomain and the 4-1BB cytoplasmic domain, termed 80BB, acts as both a ligand and a receptor to engage the CD28 and 4-1BB pathways, thereby increasing the antitumor potency of human leukocyte antigen-independent TCR (HIT) receptor- or TCR-engineered T cells and tumor-infiltrating lymphocytes. Furthermore, 80BB serves as a switch receptor that provides agonistic 4-1BB co-stimulation upon its ligation by the inhibitory CTLA4 molecule. By combining multiple co-stimulatory features in a single antigen-agnostic synthetic receptor, 80BB is a promising tool to sustain CD3-dependent T cell responses in a wide range of targeted immunotherapies.

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