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. 2025 Mar;639(8055):746-753.
doi: 10.1038/s41586-024-08510-w. Epub 2025 Feb 5.

IL-27 elicits a cytotoxic CD8+ T cell program to enforce tumour control

Béatrice Bréart #  1 Katherine Williams #  1 Stellanie Krimm #  1 Tiffany Wong  1 Brandon D Kayser  1 Lifen Wang  1 Eric Cheng  1 Mayra Cruz Tleugabulova  1 Romain Bouziat  1 Tianshi Lu  1 Kobe Yuen  1 Natalie S Firmino  1 Daniel D Bravo  1 Juliette Roels  1 Atish Bhakta  1 Jack Bevers 3rd  1 Isabelle Lehoux  1 Alan Gutierrez  1 Yajun Chestnut  1 Joanna E Klementowicz  1 Teresita L Arenzana  1 Ilseyar Akhmetzyanova  1 Elizabeth Dixon  1 Min Chen  1 Kazi Tasneem  1 Rajbharan Yadav  1 Hartmut Koeppen  1 Soyoung A Oh  1 Lélia Delamarre  1 Haochu Huang  1 Shion A Lim  1 Gerald Nakamura  1 Jianyong Wang  1 Chan Gao  1 Racquel Corpuz  1 Sören Müller  2 Nathaniel R West  3
Affiliations

IL-27 elicits a cytotoxic CD8+ T cell program to enforce tumour control

Béatrice Bréart et al. Nature. 2025 Mar.

Abstract

Although cytotoxic CD8+ T lymphocytes (CTLs) are essential for anti-tumour immunity, they are frequently dysfunctional in tumours1. Cytokines that sustain CTL activity are attractive for cancer immunotherapy, but avoiding inflammatory toxicity remains a challenge for their clinical use2. Here we show that expression of a CTL signature is strongly associated with IL27 expression in human and mouse tumours. In mice, IL-27 acts directly on tumour-specific CTLs to promote their persistence and effector function in the tumour microenvironment. Moreover, treatment with inducible IL-27 overexpression or a half-life-extended IL-27 protein in vivo is well tolerated, induces regression of established tumours, drives an enhanced cytotoxic program in anti-tumour CTLs and synergizes with PD-L1 blockade. In patients with cancer who were treated with anti-PD-1/PD-L1 therapy, high expression of IL-27 correlates with a favourable clinical response, and IL-27 supports human CTL function during chronic antigen stimulation ex vivo. Our data demonstrate that endogenous IL-27 is essential for anti-tumour immunity and that IL-27 receptor agonism can safely improve anti-tumour T cell responses alone or in combination with PD-L1 blockade.

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Conflict of interest statement

Competing interests: All of the authors are current or former members of Genentech. Data included in this study were used to support a provisional patent application (filed by Genentech) describing engineered variants of recombinant IL-27 (US patent application 63/713418).

References

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