Single residue in CD28-costimulated CAR-T cells limits long-term persistence and antitumor durability

Sonia Guedan; Aviv Madar; Victoria Casado-Medrano; Carolyn E. Shaw; Anna Wing; Fang Liu; Regina M. Young; Carl H. June; Avery D. Posey

doi:https://doi.org/10.1172/jci133215

doi.org/10.1172/jci133215

Single residue in CD28-costimulated CAR-T cells limits long-term persistence and antitumor durability

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..., Avery D. Posey

23

Journal of Clinical Investigation15.90

Volume: 130, Issue: 6, Pages: 3087 - 3097

Published: May 4, 2020

Abstract

Chimeric antigen receptor–T (CAR-T) cell therapies can eliminate relapsed and refractory tumors, but the durability of antitumor activity requires in vivo persistence. Differential signaling through the CAR costimulatory domain can alter the T cell metabolism, memory differentiation, and influence long-term persistence. CAR-T cells costimulated with 4-1BB or ICOS persist in xenograft models but those constructed with CD28 exhibit rapid...

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Paper Details

Title

Single residue in CD28-costimulated CAR-T cells limits long-term persistence and antitumor durability

DOI

doi.org/10.1172/jci133215

Published Date

May 4, 2020

Journal

Journal of Clinical Investigation

Volume

130

Issue

6

Pages

3087 - 3097

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