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Optimising IL-2 for Cancer Immunotherapy

Abstract

The key role of T cells in cancer immunotherapy is well established and is highlighted by the remarkable capacity of Ab-mediated checkpoint blockade to overcome T-cell exhaustion and amplify anti-tumor responses. However, total or partial tumor remission following checkpoint blockade is still limited to only a few types of tumors. Hence, concerted attempts are being made to devise new methods for improving tumor immunity. Currently, much attention is being focused on therapy with IL-2. This cytokine is a powerful growth factor for T cells and optimises their effector functions. When used at therapeutic doses for cancer treatment, however, IL-2 is highly toxic. Nevertheless, recent work has shown that modifying the structure or presentation of IL-2 can reduce toxicity and lead to effective anti-tumor responses in synergy with checkpoint blockade. Here, we review the complex interaction of IL-2 with T cells: first during normal homeostasis, then during responses to pathogens, and finally in anti-tumor responses.

Type Journal
ISBN 1598-2629 (Print) 2092-6685 (Electronic) 1598-2629 (Linking)
Authors Sprent, J.; Boyman, O.
Publisher Name Immune Network
Published Date 2024-01-31
Published Volume 24
Published Issue 1
Published Pages e5
Status Published in-print
DOI 10.4110/in.2024.24.e5
URL link to publisher's version https://www.ncbi.nlm.nih.gov/pubmed/38455463