CAR-T Cells Targeting Epstein-Barr Virus Gp350 Validated in a Humanized Mouse Model of EBV Infection and Lymphoproliferative Disease

Overview

Journal Mol Ther Oncolytics

Publisher Cell Press

Date 2020 Sep 21

PMID 32953984

Citations 28

Authors

Constanze Slabik

Maja Kalbarczyk

Simon Danisch

Reinhard Zeidler

Frank Klawonn

Valery Volk

Nicole Kronke

Friedrich Feuerhake

Constanca Ferreira de Figueiredo

Rainer Blasczyk

Henning Olbrich

Sebastian J Theobald

Andreas Schneider

Arnold Ganser

Constantin von Kaisenberg

Stefan Lienenklaus

Andre Bleich

Wolfgang Hammerschmidt

Renata Stripecke

Affiliations

Soon will be listed here.

Abstract

Epstein-Barr virus (EBV) is a latent and oncogenic human herpesvirus. Lytic viral protein expression plays an important role in EBV-associated malignancies. The EBV envelope glycoprotein 350 (gp350) is expressed abundantly during EBV lytic reactivation and sporadically on the surface of latently infected cells. Here we tested T cells expressing gp350-specific chimeric antigen receptors (CARs) containing scFvs derived from two novel gp350-binding, highly neutralizing monoclonal antibodies. The scFvs were fused to CD28/CD3ζ signaling domains in a retroviral vector. The produced gp350CAR-T cells specifically recognized and killed gp350 293T cells . The best-performing 7A1-gp350CAR-T cells were cytotoxic against the EBV B95-8 cell line, showing selectivity against gp350 cells. Fully humanized Nod.Rag.Gamma mice transplanted with cord blood CD34 cells and infected with the EBV/M81/fLuc lytic strain were monitored dynamically for viral spread. Infected mice recapitulated EBV-induced lymphoproliferation, tumor development, and systemic inflammation. We tested adoptive transfer of autologous CD8gp350CAR-T cells administered protectively or therapeutically. After gp350CAR-T cell therapy, 75% of mice controlled or reduced EBV spread and showed lower frequencies of EBER B cell malignant lymphoproliferation, lack of tumor development, and reduced inflammation. In summary, CD8gp350CAR-T cells showed proof-of-concept preclinical efficacy against impending EBV lymphoproliferation and lymphomagenesis.

Citing Articles

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