Author
Listed:
- Masao Hashimoto
(Emory University School of Medicine
Emory University School of Medicine)
- Koichi Araki
(Emory University School of Medicine
Emory University School of Medicine
Cincinnati Children’s Hospital Medical Center
University of Cincinnati College of Medicine)
- Maria A. Cardenas
(Emory University School of Medicine)
- Peng Li
(National Heart, Lung, and Blood Institute (NHLBI), National Institutes of Health (NIH))
- Rohit R. Jadhav
(Mayo Clinic School of Medicine and Sciences
Stanford University School of Medicine)
- Haydn T. Kissick
(Emory University School of Medicine
Emory University School of Medicine
Emory University School of Medicine
Emory University)
- William H. Hudson
(Emory University School of Medicine
Emory University School of Medicine)
- Donald J. McGuire
(Emory University School of Medicine
Emory University School of Medicine)
- Rebecca C. Obeng
(Emory University School of Medicine
Emory University School of Medicine
Emory University School of Medicine
Northwestern University Feinberg School of Medicine)
- Andreas Wieland
(Emory University School of Medicine
Emory University School of Medicine
The Ohio State University College of Medicine
The Ohio State University Comprehensive Cancer Center)
- Judong Lee
(Emory University School of Medicine
Emory University School of Medicine)
- Daniel T. McManus
(Emory University School of Medicine
Emory University School of Medicine)
- James L. Ross
(Emory University School of Medicine
Emory University School of Medicine)
- Se Jin Im
(Emory University School of Medicine
Emory University School of Medicine
Sungkyunkwan University School of Medicine)
- Junghwa Lee
(Emory University School of Medicine
Emory University School of Medicine
Sungkyunkwan University School of Medicine)
- Jian-Xin Lin
(National Heart, Lung, and Blood Institute (NHLBI), National Institutes of Health (NIH))
- Bin Hu
(Stanford University School of Medicine)
- Erin E. West
(National Heart, Lung, and Blood Institute (NHLBI), National Institutes of Health (NIH)
National Heart, Lung, and Blood Institute (NHLBI), National Institutes of Health (NIH))
- Christopher D. Scharer
(Emory University School of Medicine)
- Gordon J. Freeman
(Dana-Farber Cancer Institute
Harvard Medical School)
- Arlene H. Sharpe
(Blavatnik Institute, Harvard Medical School
Harvard Medical School and Brigham and Women’s Hospital)
- Suresh S. Ramalingam
(Emory University
Emory University School of Medicine)
- Alex Pellerin
(Biogen)
- Volker Teichgräber
(Roche Innovation Center Basel)
- William J. Greenleaf
(Stanford University School of Medicine)
- Christian Klein
(Roche Innovation Center Zurich)
- Jorg J. Goronzy
(Mayo Clinic School of Medicine and Sciences
Stanford University School of Medicine)
- Pablo Umaña
(Roche Innovation Center Zurich)
- Warren J. Leonard
(National Heart, Lung, and Blood Institute (NHLBI), National Institutes of Health (NIH))
- Kendall A. Smith
(Weill Medical College of Cornell University)
- Rafi Ahmed
(Emory University School of Medicine
Emory University School of Medicine
Emory University)
Abstract
Combination therapy with PD-1 blockade and IL-2 is highly effective during chronic lymphocytic choriomeningitis virus infection1. Here we examine the underlying basis for this synergy. We show that PD-1 + IL-2 combination therapy, in contrast to PD-1 monotherapy, substantially changes the differentiation program of the PD-1+TCF1+ stem-like CD8+ T cells and results in the generation of transcriptionally and epigenetically distinct effector CD8+ T cells that resemble highly functional effector CD8+ T cells seen after an acute viral infection. The generation of these qualitatively superior CD8+ T cells that mediate viral control underlies the synergy between PD-1 and IL-2. Our results show that the PD-1+TCF1+ stem-like CD8+ T cells, also referred to as precursors of exhausted CD8+ T cells, are not fate-locked into the exhaustion program and their differentiation trajectory can be changed by IL-2 signals. These virus-specific effector CD8+ T cells emerging from the stem-like CD8+ T cells after combination therapy expressed increased levels of the high-affinity IL-2 trimeric (CD25–CD122–CD132) receptor. This was not seen after PD-1 blockade alone. Finally, we show that CD25 engagement with IL-2 has an important role in the observed synergy between IL-2 cytokine and PD-1 blockade. Either blocking CD25 with an antibody or using a mutated version of IL-2 that does not bind to CD25 but still binds to CD122 and CD132 almost completely abrogated the synergistic effects observed after PD-1 + IL-2 combination therapy. There is considerable interest in PD-1 + IL-2 combination therapy for patients with cancer2,3, and our fundamental studies defining the underlying mechanisms of how IL-2 synergizes with PD-1 blockade should inform these human translational studies.
Suggested Citation
Masao Hashimoto & Koichi Araki & Maria A. Cardenas & Peng Li & Rohit R. Jadhav & Haydn T. Kissick & William H. Hudson & Donald J. McGuire & Rebecca C. Obeng & Andreas Wieland & Judong Lee & Daniel T. , 2022.
"PD-1 combination therapy with IL-2 modifies CD8+ T cell exhaustion program,"
Nature, Nature, vol. 610(7930), pages 173-181, October.
Handle:
RePEc:nat:nature:v:610:y:2022:i:7930:d:10.1038_s41586-022-05257-0
DOI: 10.1038/s41586-022-05257-0
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