Author:
Palmer Douglas,Webber Beau,Patel Yogin,Johnson Matthew,Kariya Christine,Lahr Walker,Parkhurst Maria,Gartner Jared,Prickett Todd,Lowery Frank,Kishton Rigel,Gurusamy Devikala,Franco Zulmarie,Vodnala Suman,Diers Miechaleen,Wolf Natalie,Slipek Nicholas,McKenna David,Sumstad Darin,Viney Lydia,Henley Tom,Bürckstümmer Tilmann,Baker Oliver,Hu Ying,Yan Chunhua,Meerzaman Daoud,Padhan Kartik,Lo Winnie,Malekzadeh Parisa,Jia Li,Deniger Drew,Patel Shashank,Robbins Paul,Scott McIvor R,Choudhry Modassir,Rosenberg Steven,Moriarity Branden,Restifo Nicholas
Abstract
BackgroundNeoantigen-specific T cells isolated from tumors have shown promise clinically but fail to consistently elicit durable tumor regression. Expression of the intracellular checkpoint CISH is elevated in human tumor infiltrating lymphocytes (TIL) and has been shown to inhibit neoantigen reactivity in murine TIL.MethodsTo explore CISH function in human T cells we developed a CRISPR/Cas9-based strategy to knockout (KO) CISH in human T cells with high-efficiency (>90%) and without detectable off-target editing.ResultsCISH KO in peripheral blood T cells enhanced proliferation, cytokine polyfunctionality, and cytotoxicity in vitro. To determine if CISH KO similarly enhances TIL function, we developed a clinical-scale, GMP-compliant manufacturing process for CISH disruption in primary human TIL. In process validation runs we achieved CISH KO efficiencies >90% without detectable off-target editing while maintaining high viability and expansion. Compared to WT controls, CISH KO in patient-derived TIL demonstrated increased proliferation, T cell receptor (TCR) avidity, neoantigen recognition, and unmasked reactivity to common p53 mutations. Hyperactivation in CISH KO TIL did not increase differentiation, suggesting that CISH KO may uncouple activation and differentiation pathways. Single cell profiling identifies a pattern of CISH expression inverse to key regulators of activation, and CISH KO in human TIL increases PD1 expression. Adoptive transfer of Cish KO T cells synergistically combines with PD1 inhibition resulting in durable tumor regression in mice, highlighting orthogonal dual cell surface and intracellular checkpoint inhibition as a novel combinatorial approach for T cell immunotherapy.ConclusionsThese pre-clinical data offer new insight into neoantigen recognition and serve as the basis for a recently initiated human clinical trial at the University of Minnesota (NCT04426669) evaluating inhibition of the novel intracellular immune checkpoint CISH in a CRISPR-engineered, neoantigen-specific T cell therapy for solid tumors. Updates from the clinical trial will be highlighted.Trial RegistrationNCT04426669
Subject
Cancer Research,Pharmacology,Oncology,Molecular Medicine,Immunology,Immunology and Allergy