NY-ESO-1-specific TCR-engineered T Cells Mediate Sustained Antigen-specific Antitumor Effects in Myeloma

Overview

Journal Nat Med

Specialties General Medicine
Molecular Biology

Date 2015 Jul 21

PMID 26193344

Citations 455

Authors

Aaron P Rapoport

Edward A Stadtmauer

Gwendolyn K Binder-Scholl

Olga Goloubeva

Dan T Vogl

Simon F Lacey

Ashraf Z Badros

Alfred Garfall

Brendan Weiss

Jeffrey Finklestein

Irina Kulikovskaya

Sanjoy K Sinha

Shari Kronsberg

Minnal Gupta

Sarah Bond

Luca Melchiori

Joanna E Brewer

Alan D Bennett

Andrew B Gerry

Nicholas J Pumphrey

Daniel Williams

Helen K Tayton-Martin

Lilliam Ribeiro

Tom Holdich

Saul Yanovich

Nancy Hardy

Jean Yared

Naseem Kerr

Sunita Philip

Sandra Westphal

Don L Siegel

Bruce L Levine

Bent K Jakobsen

Michael Kalos

Carl H June

Affiliations

Soon will be listed here.

Abstract

Despite recent therapeutic advances, multiple myeloma (MM) remains largely incurable. Here we report results of a phase I/II trial to evaluate the safety and activity of autologous T cells engineered to express an affinity-enhanced T cell receptor (TCR) recognizing a naturally processed peptide shared by the cancer-testis antigens NY-ESO-1 and LAGE-1. Twenty patients with antigen-positive MM received an average 2.4 × 10(9) engineered T cells 2 d after autologous stem cell transplant. Infusions were well tolerated without clinically apparent cytokine-release syndrome, despite high IL-6 levels. Engineered T cells expanded, persisted, trafficked to marrow and exhibited a cytotoxic phenotype. Persistence of engineered T cells in blood was inversely associated with NY-ESO-1 levels in the marrow. Disease progression was associated with loss of T cell persistence or antigen escape, in accordance with the expected mechanism of action of the transferred T cells. Encouraging clinical responses were observed in 16 of 20 patients (80%) with advanced disease, with a median progression-free survival of 19.1 months. NY-ESO-1-LAGE-1 TCR-engineered T cells were safe, trafficked to marrow and showed extended persistence that correlated with clinical activity against antigen-positive myeloma.

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