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Disruption of TET2 Promotes the Therapeutic Efficacy of CD19-targeted T-cells

Authors :
Simon F. Lacey
Jamie E. DeNizio
Shantan Reddy
Rahul M. Kohli
Stefan Lundh
Irina Kulikovskaya
Jennifer J.D. Morrissette
Shelley L. Berger
Joseph A. Fraietta
Morgan A. Sammons
Yangbing Zhao
Alexandria P. Cogdill
Mercy Gohil
Marvin H. Gee
David L. Porter
Yan Wang
Enrique Lin-Shiao
Christopher L. Nobles
Xiaojun Liu
J. Joseph Melenhorst
Martha S. Jordan
David E Ambrose
Bruce L. Levine
Shannon A. Carty
Michael Kalos
Regina M. Young
Katherine A. Alexander
Frederic D. Bushman
Katherine T. Marcucci
Farzana Nazimuddin
Minnal Gupta
John K. Everett
Carl H. June
Jun Xu
K. Christopher Garcia
Fang Chen
Young Hwang
Tyler J. Reich
Publication Year :
2018

Abstract

Cancer immunotherapy based on genetically redirecting T cells has been used successfully to treat B cell malignancies1-3. In this strategy, the T cell genome is modified by integration of viral vectors or transposons encoding chimaeric antigen receptors (CARs) that direct tumour cell killing. However, this approach is often limited by the extent of expansion and persistence of CAR T cells4,5. Here we report mechanistic insights from studies of a patient with chronic lymphocytic leukaemia treated with CAR T cells targeting the CD19 protein. Following infusion of CAR T cells, anti-tumour activity was evident in the peripheral blood, lymph nodes and bone marrow; this activity was accompanied by complete remission. Unexpectedly, at the peak of the response, 94% of CAR T cells originated from a single clone in which lentiviral vector-mediated insertion of the CAR transgene disrupted the methylcytosine dioxygenase TET2 gene. Further analysis revealed a hypomorphic mutation in this patient's second TET2 allele. TET2-disrupted CAR T cells exhibited an epigenetic profile consistent with altered T cell differentiation and, at the peak of expansion, displayed a central memory phenotype. Experimental knockdown of TET2 recapitulated the potency-enhancing effect of TET2 dysfunction in this patient's CAR T cells. These findings suggest that the progeny of a single CAR T cell induced leukaemia remission and that TET2 modification may be useful for improving immunotherapies.

Details

Language :
English
Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....f9d9594ff7433f45db65c0b1c37925dc