Pre-encoded Responsiveness to Type I Interferon in the Peripheral Immune System Defines Outcome of PD1 Blockade Therapy

Overview

Journal Nat Immunol

Date 2022 Jul 14

PMID 35835962

Authors

Giselle M Boukhaled

Ramy Gadalla

Heidi J Elsaesser

Diala Abd-Rabbo

Rene Quevedo

S Y Cindy Yang

Mengdi Guo

Ben X Wang

Babak Noamani

Diana Gray

Sally C M Lau

Kirsty Taylor

Kyaw Aung

Anna Spreafico

Aaron R Hansen

Samuel D Saibil

Naoto Hirano

Cynthia Guidos

Trevor J Pugh

Tracy L McGaha

Pamela S Ohashi

Adrian G Sacher

Marcus O Butler

David G Brooks

Affiliations

Soon will be listed here.

Abstract

Type I interferons (IFN-Is) are central regulators of anti-tumor immunity and responses to immunotherapy, but they also drive the feedback inhibition underlying therapeutic resistance. In the present study, we developed a mass cytometry approach to quantify IFN-I-stimulated protein expression across immune cells and used multi-omics to uncover pre-therapy cellular states encoding responsiveness to inflammation. Analyzing peripheral blood cells from multiple cancer types revealed that differential responsiveness to IFN-Is before anti-programmed cell death protein 1 (PD1) treatment was highly predictive of long-term survival after therapy. Unexpectedly, IFN-I hyporesponsiveness efficiently predicted long-term survival, whereas high responsiveness to IFN-I was strongly associated with treatment failure and diminished survival time. Peripheral IFN-I responsive states were not associated with tumor inflammation, identifying a disconnect between systemic immune potential and 'cold' or 'hot' tumor states. Mechanistically, IFN-I responsiveness was epigenetically imprinted before therapy, poising cells for differential inflammatory responses and dysfunctional T cell effector programs. Thus, we identify physiological cell states with clinical importance that can predict success and long-term survival of PD1-blocking immunotherapy.

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