Safety and Efficacy of Durvalumab and Tremelimumab Alone or in Combination in Patients with Advanced Gastric and Gastroesophageal Junction Adenocarcinoma

Overview

Journal Clin Cancer Res

Specialty Oncology

Date 2019 Nov 3

PMID 31676670

Citations 73

Authors

Ronan J Kelly

Jeeyun Lee

Yung-Jue Bang

Khaldoun Almhanna

Mariela Blum-Murphy

Daniel V T Catenacci

Hyun Cheol Chung

Zev A Wainberg

Michael K Gibson

Keun-Wook Lee

Johanna C Bendell

Crystal S Denlinger

Cheng Ean Chee

Takeshi Omori

Rom Leidner

Heinz-Josef Lenz

Yee Chao

Marlon C Rebelatto

Philip Z Brohawn

Peng He

Jennifer McDevitt

Siddharth Sheth

Judson M Englert

Geoffrey Y Ku

Affiliations

Soon will be listed here.

Abstract

Purpose: This randomized, multicenter, open-label, phase Ib/II study assessed durvalumab and tremelimumab in combination or as monotherapy for chemotherapy-refractory gastric cancer or gastroesophageal junction (GEJ) cancer.

Patients And Methods: Second-line patients were randomized 2:2:1 to receive durvalumab plus tremelimumab (arm A), or durvalumab (arm B) or tremelimumab monotherapy (arm C), and third-line patients received durvalumab plus tremelimumab (arm D). A tumor-based IFNγ gene signature was prospectively evaluated as a potential predictive biomarker in second- and third-line patients receiving the combination (arm E). The coprimary endpoints were objective response rate and progression-free survival (PFS) rate at 6 months.

Results: A total of 113 patients were treated: 6 in phase Ib and 107 (arm A, 27; arm B, 24; arm C, 12; arm D, 25; arm E, 19) in phase II. Overall response rates were 7.4%, 0%, 8.3%, 4.0%, and 15.8% in the five arms, respectively. PFS rates at 6 months were 6.1%, 0%, 20%, 15%, and 0%, and 12-month overall survival rates were 37.0%, 4.6%, 22.9%, 38.8%, and NA, respectively. Treatment-related grade 3/4 adverse events were reported in 17%, 4%, 42%, 16%, and 11% of patients, respectively.

Conclusions: Response rates were low regardless of monotherapy or combination strategies. No new safety signals were identified. Including use of a tumor-based IFNγ signature and change in baseline and on-treatment circulating tumor DNA are clinically feasible and may be novel strategies to improve treatment response in this difficult-to-treat population.

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