CD123-engager T cells as a novel immunotherapeutic for acute myeloid leukemia

Challice L. Bonifant; Arpad Szoor; David Torres; Nicholos Joseph; Mireya Paulina Velasquez; Kota Iwahori; Amos Gaikwad; Phuong Nguyen; Caroline Arber; Xiao Tong Song; Michele Redell; Stephen Gottschalk

doi:10.1038/mt.2016.116

CD123-engager T cells as a novel immunotherapeutic for acute myeloid leukemia

Challice L. Bonifant, Arpad Szoor, David Torres, Nicholos Joseph, Mireya Paulina Velasquez, Kota Iwahori, Amos Gaikwad, Phuong Nguyen, Caroline Arber, Xiao Tong Song, Michele Redell, Stephen Gottschalk

Research output: Contribution to journal › Article › peer-review

37 Scopus citations

Abstract

Immunotherapy with CD123-specific T-cell engager proteins or with T cells expressing CD123-specific chimeric antigen receptors is actively being pursued for acute myeloid leukemia. T cells secreting bispecific engager molecules (ENG-T cells) may present a promising alternative to these approaches. To evaluate therapeutic potential, we generated T cells to secrete CD123/CD3-bispecific engager molecules. CD123-ENG T cells recognized primary acute myeloid leukemia (AML) cells and cell lines in an antigen-dependent manner as judged by cytokine production and/or tumor killing, and redirected bystander T cells to AML cells. Infusion of CD123-ENG T cells resulted in regression of AML in xenograft models conferring a significant survival advantage of treated mice in comparison to mice that received control T cells. At high effector to target ratios, CD123-ENG T cells recognized normal hematopoietic stem and progenitor cells (HSPCs) with preferential recognition of HSPCs from cord blood compared to bone marrow. We therefore introduced the CD20 suicide gene that can be targeted in vivo with rituximab into CD123-ENG T cells. The expression of CD20 did not diminish the anti-AML activity of CD123-ENG T cells, but allowed for rituximab-mediated ENG-T cell elimination. Thus, ENG-T cells coexpressing CD20 suicide and CD123 engager molecules may present a promising immunotherapeutic approach for AML.

Original language	English (US)
Pages (from-to)	1615-1626
Number of pages	12
Journal	Molecular Therapy
Volume	24
Issue number	9
DOIs	https://doi.org/10.1038/mt.2016.116
State	Published - Sep 1 2016
Externally published	Yes

ASJC Scopus subject areas

Molecular Medicine
Molecular Biology
Genetics
Pharmacology
Drug Discovery

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10.1038/mt.2016.116

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@article{5bd340b25ec6451e8ed2b881659fd751,

title = "CD123-engager T cells as a novel immunotherapeutic for acute myeloid leukemia",

abstract = "Immunotherapy with CD123-specific T-cell engager proteins or with T cells expressing CD123-specific chimeric antigen receptors is actively being pursued for acute myeloid leukemia. T cells secreting bispecific engager molecules (ENG-T cells) may present a promising alternative to these approaches. To evaluate therapeutic potential, we generated T cells to secrete CD123/CD3-bispecific engager molecules. CD123-ENG T cells recognized primary acute myeloid leukemia (AML) cells and cell lines in an antigen-dependent manner as judged by cytokine production and/or tumor killing, and redirected bystander T cells to AML cells. Infusion of CD123-ENG T cells resulted in regression of AML in xenograft models conferring a significant survival advantage of treated mice in comparison to mice that received control T cells. At high effector to target ratios, CD123-ENG T cells recognized normal hematopoietic stem and progenitor cells (HSPCs) with preferential recognition of HSPCs from cord blood compared to bone marrow. We therefore introduced the CD20 suicide gene that can be targeted in vivo with rituximab into CD123-ENG T cells. The expression of CD20 did not diminish the anti-AML activity of CD123-ENG T cells, but allowed for rituximab-mediated ENG-T cell elimination. Thus, ENG-T cells coexpressing CD20 suicide and CD123 engager molecules may present a promising immunotherapeutic approach for AML.",

author = "Bonifant, {Challice L.} and Arpad Szoor and David Torres and Nicholos Joseph and Velasquez, {Mireya Paulina} and Kota Iwahori and Amos Gaikwad and Phuong Nguyen and Caroline Arber and Song, {Xiao Tong} and Michele Redell and Stephen Gottschalk",

note = "Funding Information: We thank Cliona Rooney, Malcolm Brenner, and Helen Heslop for helpful discussions and advice. This work was supported by The Leukemia & Lymphoma Society, Ladies Leukemia League, Alex's Lemonade Stand Foundation for Childhood Cancer, When Everyone Survives Foundation, and a philanthropic gift to fund AML research at the Center for Cell and Gene Therapy. C.L.B. was supported by NIH grant 5T32HL092332-12. M.P.V. is a St. Baldrick's Foundation fellow. C.A. is an ASH Research Scholar. The Center for Cell and Gene Therapy had a research collaboration with Celgene and Bluebird Bio. K.I., M.P.V., C.A., and S.G. have patent applications in the field of T cell and gene-modified T-cell therapy for cancer. Publisher Copyright: {\textcopyright} 2016 The American Society of Gene & Cell Therapy.",

year = "2016",

month = sep,

day = "1",

doi = "10.1038/mt.2016.116",

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AU - Bonifant, Challice L.

AU - Szoor, Arpad

AU - Torres, David

AU - Joseph, Nicholos

AU - Velasquez, Mireya Paulina

AU - Iwahori, Kota

AU - Gaikwad, Amos

AU - Nguyen, Phuong

AU - Arber, Caroline

AU - Song, Xiao Tong

AU - Redell, Michele

AU - Gottschalk, Stephen

N1 - Funding Information: We thank Cliona Rooney, Malcolm Brenner, and Helen Heslop for helpful discussions and advice. This work was supported by The Leukemia & Lymphoma Society, Ladies Leukemia League, Alex's Lemonade Stand Foundation for Childhood Cancer, When Everyone Survives Foundation, and a philanthropic gift to fund AML research at the Center for Cell and Gene Therapy. C.L.B. was supported by NIH grant 5T32HL092332-12. M.P.V. is a St. Baldrick's Foundation fellow. C.A. is an ASH Research Scholar. The Center for Cell and Gene Therapy had a research collaboration with Celgene and Bluebird Bio. K.I., M.P.V., C.A., and S.G. have patent applications in the field of T cell and gene-modified T-cell therapy for cancer. Publisher Copyright: © 2016 The American Society of Gene & Cell Therapy.

PY - 2016/9/1

Y1 - 2016/9/1

N2 - Immunotherapy with CD123-specific T-cell engager proteins or with T cells expressing CD123-specific chimeric antigen receptors is actively being pursued for acute myeloid leukemia. T cells secreting bispecific engager molecules (ENG-T cells) may present a promising alternative to these approaches. To evaluate therapeutic potential, we generated T cells to secrete CD123/CD3-bispecific engager molecules. CD123-ENG T cells recognized primary acute myeloid leukemia (AML) cells and cell lines in an antigen-dependent manner as judged by cytokine production and/or tumor killing, and redirected bystander T cells to AML cells. Infusion of CD123-ENG T cells resulted in regression of AML in xenograft models conferring a significant survival advantage of treated mice in comparison to mice that received control T cells. At high effector to target ratios, CD123-ENG T cells recognized normal hematopoietic stem and progenitor cells (HSPCs) with preferential recognition of HSPCs from cord blood compared to bone marrow. We therefore introduced the CD20 suicide gene that can be targeted in vivo with rituximab into CD123-ENG T cells. The expression of CD20 did not diminish the anti-AML activity of CD123-ENG T cells, but allowed for rituximab-mediated ENG-T cell elimination. Thus, ENG-T cells coexpressing CD20 suicide and CD123 engager molecules may present a promising immunotherapeutic approach for AML.

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CD123-engager T cells as a novel immunotherapeutic for acute myeloid leukemia

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