Durable Response and Improved CD8 T Cell Plasticity in Lung Cancer Patients After PD1 Blockade and JAK Inhibition

Authors

Divij Mathew
Melina E. Marmarelis
Caitlin Foley
Joshua M. Bauml
Darwin Ye
Reem Ghinnagow
Shin Foong Ngiow
Max Klapholz
Soyeong Jun
Zhaojun Zhang
Robert Zorc
Maximillian Diehn
Wei-Ting Hwang
Nancy R. Zhang
Corey J. Langer
E. John Wherry
Andy J. Minn

Document Type

Article

Abstract

Persistent inflammation including type-one interferon (IFN-I) can cause immunosuppression. We show that delayed administration of the JAK1 inhibitor itacitinib after anti-PD1 improves immune function and anti-tumor response in mice, and results in high response rates (67%) in a phase-2 clinical trial for metastatic non-small cell lung cancer with tumor PDL1≥50%. In contrast to patients with low inflammation who responded to anti-PD1, patients with elevated inflammation had poor immune and tumor responses to anti-PD1 that improved after adding itacitinib. Itacitinib promoted features of CD8 T cell plasticity and therapeutic responses of exhausted and effector-memory clonotypes. Patients with persistent IFN-I signaling refractory to itacitinib showed progressive CD8 T cell terminal differentiation and progressive disease. Thus, JAK inhibition may improve anti-PD1 efficacy by pivoting T cell differentiation dynamics.

DOI

10.1101/2022.11.05.22281973

Publication Date

11-7-2022

Recommended Citation

Mathew D, Marmarelis ME, Foley C, Bauml JM, Ye D, Ghinnagow R, Ngiow SF, Klapholz M, Jun S, Zhang Z, Zorc R. Durable response and improved CD8 T cell plasticity in lung cancer patients after PD1 blockade and JAK inhibition. medRxiv. 2022 Nov 7:2022-11.