Thrombopoietin-based CAR-T cells demonstrate in vitro and in vivo cytotoxicity to MPL positive acute myelogenous leukemia and hematopoietic stem cells

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作者
Jaquelyn T. Zoine
Chengyu Prince
Jamie Y. Story
Gianna M. Branella
Allison M. Lytle
Andrew Fedanov
Jordan S. Alexander
Christopher C. Porter
Christopher B. Doering
H. Trent Spencer
Shanmuganathan Chandrakasan
机构
[1] Emory University School of Medicine,Aflac Cancer and Blood Disorders Center, Department of Pediatrics
[2] Emory University School of Medicine,Cancer Biology Program, Graduate Division of Biological and Biomedical Sciences
[3] Emory University School of Medicine,Molecular and Systems Pharmacology Program, Graduate Division of Biological and Biomedical Sciences
[4] Children’s Healthcare of Atlanta,undefined
来源
Gene Therapy | 2022年 / 29卷
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摘要
While targeting CD19+ hematologic malignancies with CAR T cell therapy using single chain variable fragments (scFv) has been highly successful, novel strategies for applying CAR T cell therapy with other tumor types are necessary. In the current study, CAR T cells were designed using a ligand binding domain instead of an scFv to target stem-like leukemia cells. Thrombopoietin (TPO), the natural ligand to the myeloproliferative leukemia protein (MPL) receptor, was used as the antigen binding domain to engage MPL expressed on hematopoietic stem cells (HSC) and erythropoietic and megakaryocytic acute myeloid leukemias (AML). TPO-CAR T cells were tested in vitro against AML cell lines with varied MPL expression to test specificity. TPO-CAR T cells were specifically activating and cytotoxic against MPL+ leukemia cell lines. Though the TPO-CAR T cells did not extend survival in vivo, it successfully cleared the MPL+ fraction of leukemia cells. As expected, we also show the TPO-CAR is cytotoxic against MPL expressing bone marrow compartment in AML xenograft models. The data collected demonstrate preclinical potential of TPO-CAR T cells for stem-like leukemia through assessment of targeted killing of MPL+ cells and may facilitate subsequent HSC transplant under reduced intensity conditioning regimens.
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页数:11
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