Results of a phase I study of bispecific anti-CD19, anti-CD20 chimeric antigen receptor (CAR) modified T cells for relapsed, refractory, non-Hodgkin lymphoma.

Nirav N. Shah; Fenlu Zhu; Dina Schneider; Carolyn Taylor; Winfried Krueger; Andrew Worden; Walter Longo; Mehdi Hamadani; Timothy S. Fenske; Bryon D. Johnson; Boro Dropulić; Rimas J. Orentas; Parameswaran Hari

doi:10.1200/jco.2019.37.15_suppl.2510

Results of a phase I study of bispecific anti-CD19, anti-CD20 chimeric antigen receptor (CAR) modified T cells for relapsed, refractory, non-Hodgkin lymphoma.

Nirav N. Shah(Medical College of Wisconsin), Fenlu Zhu(Medical College of Wisconsin), Dina Schneider(Lentigen Technology (United States)), Carolyn Taylor(Medical College of Wisconsin), Winfried Krueger(Lentigen Technology (United States)), Andrew Worden(Lentigen Technology (United States)), Walter Longo(University of Wisconsin–Madison), Mehdi Hamadani(Medical College of Wisconsin), Timothy S. Fenske(Medical College of Wisconsin), Bryon D. Johnson(Medical College of Wisconsin), Boro Dropulić(Lentigen Technology (United States)), Rimas J. Orentas(Lentigen Technology (United States)), Parameswaran Hari(Medical College of Wisconsin)

Journal of Clinical Oncology

May 20, 2019

10.1200/jco.2019.37.15_suppl.2510

Cited by 42

Abstract

2510 Background: Anti-CD19 CAR-T cell therapy is a breakthrough treatment (tx) for patients (pts) with relapsed/refractory (R/R) B-cell non-Hodgkin lymphoma (NHL). Despite impressive outcomes, non-response and relapse with CD19 negative disease remain challenges. Through dual B-cell antigen targeting of CD20 and CD19, with a first-in-human bispecific lentiviral CAR-T cell (LV20.19CAR), we aim to improve response rates while limiting CD19 negative relapse. Methods: Pts were treated on a Phase 1 dose escalation + expansion trial (NCT03019055) to demonstrate safety of a 41BB/CD3z LV20.19CAR T cell for adults with R/R B-cell NHL. Safety was assessed by incidence of dose limiting toxicities (DLTs) within 28 days post-infusion. Starting dose was 2.5 x 10^5 cells/kg with a target dose of 2.5 x 10^6 cells/kg. All pts received fludarabine+cyclophosphamide for lymphodepletion. Results: 11 pts have completed tx to date. 9 pts in dose escalation and 2 pts in expansion phase. Median age was 54 years (46-67) and histology included DLBCL = 5 pts, MCL = 4 pts, and CLL = 2 pts. In dose escalation, 3 pts were treated at 2.5 x 10^5 cells/kg, 3 pts at 7.5 x 10^5 cells/kg, and 3 pts at 2.5 x 10^6 cells/kg with no DLTs. As a result, 2.5 x 10^6 cells/kg was selected for expansion. In terms of safety, 6 pts developed Grade 1-2 cytokine release syndrome (CRS) and 3 pts had Grade 1-2 neurotoxicity (NTX). No patient had grade 3-4 CRS or NTX and none required ICU level care. 4 pts required 1-2 doses of tocilizumab for CRS. The day 28 overall response rate (ORR) for all pts was 82% (6/11 = complete response (CR) and 3/11 = partial response). All CR pts remain in remission, the longest > 1 year. All progressing pts underwent repeat biopsy, and all retained either CD19 or CD20 positivity. Additional pts are being enrolled in the expansion phase and updated data will be presented. Conclusions: Phase 1 results from the LV20.19 CAR T clinical trial demonstrate that infusion of 2.5 x 10^6 cells/kg is safe for further investigation with no DLTs among treated pts. Down-regulation of target antigens was not identified as a mechanism of resistance in progressing pts. With limited toxicity and encouraging ORR, dual targeted LV20.19CAR T cells merits further investigation. Clinical trial information: NCT03019055.

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