Rational Design of Anti-GITR-based Combination Immunotherapy

Overview

Journal Nat Med

Specialties General Medicine
Molecular Biology

Date 2019 May 1

PMID 31036879

Citations 120

Authors

Roberta Zappasodi

Cynthia Sirard

Yanyun Li

Sadna Budhu

Mohsen Abu-Akeel

Cailian Liu

Xia Yang

Hong Zhong

Walter Newman

Jingjing Qi

Phillip Wong

David Schaer

Henry Koon

Vamsidhar Velcheti

Matthew D Hellmann

Michael A Postow

Margaret K Callahan

Jedd D Wolchok

Taha Merghoub

Affiliations

Soon will be listed here.

Abstract

Modulating T cell homeostatic mechanisms with checkpoint blockade can efficiently promote endogenous anti-tumor T cell responses. However, many patients still do not benefit from checkpoint blockade, highlighting the need for targeting of alternative immune pathways. Glucocorticoid-induced tumor necrosis factor receptor-related protein (GITR) is an attractive target for immunotherapy, owing to its capacity to promote effector T cell (T) functions and hamper regulatory T cell (T) suppression. On the basis of the potent preclinical anti-tumor activity of agonist anti-GITR antibodies, reported by us and others, we initiated the first in-human phase 1 trial of GITR agonism with the anti-GITR antibody TRX518 ( NCT01239134 ). Here, we report the safety profile and immune effects of TRX518 monotherapy in patients with advanced cancer and provide mechanistic preclinical evidence to rationally combine GITR agonism with checkpoint blockade in future clinical trials. We demonstrate that TRX518 reduces circulating and intratumoral T cells to similar extents, providing an easily assessable biomarker of anti-GITR activity. Despite T reductions and increased T:T ratios, substantial clinical responses were not seen. Similarly, in mice with advanced tumors, GITR agonism was not sufficient to activate cytolytic T cells due to persistent exhaustion. We demonstrate that T cell reinvigoration with PD-1 blockade can overcome resistance of advanced tumors to anti-GITR monotherapy. These findings led us to start investigating TRX518 with PD-1 pathway blockade in patients with advanced refractory tumors ( NCT02628574 ).

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