Donor T cells for CAR T cell therapy

被引:0
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作者
Tiffany C. Y. Tang
Ning Xu
Robert Nordon
Michelle Haber
Kenneth Micklethwaite
Alla Dolnikov
机构
[1] UNSW Sydney,Graduate School of Biomedical Engineering, Faculty of Engineering
[2] Children’s Cancer Institute,School of Women’s and Children’s Health, Faculty of Medicine
[3] Lowy Cancer Research Center,Kids Cancer Center
[4] UNSW Sydney,Blood Transplant and Cell Therapies Program, Department of Hematology
[5] UNSW Sydney,Blood Transplant and Cell Therapies Laboratory
[6] Sydney Children’s Hospital,Sydney Medical School
[7] Westmead Hospital,undefined
[8] NSW Health Pathology,undefined
[9] ICPMR Westmead,undefined
[10] Westmead Institute for Medical Research,undefined
[11] The University of Sydney,undefined
来源
关键词
Donor CAR T cells; Genome editing; CRISPR-Cas9; TALENs; GVHD;
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摘要
Adoptive cell therapy using patient-derived chimeric receptor antigen (CAR) T cells redirected against tumor cells has shown remarkable success in treating hematologic cancers. However, wider accessibility of cellular therapies for all patients is needed. Manufacture of patient-derived CAR T cells is limited by prolonged lymphopenia in heavily pre-treated patients and risk of contamination with tumor cells when isolating T cells from patient blood rich in malignant blasts. Donor T cells provide a good source of immune cells for adoptive immunotherapy and can be used to generate universal off-the-shelf CAR T cells that are readily available for administration into patients as required. Genome editing tools such as TALENs and CRISPR-Cas9 and non-gene editing methods such as short hairpin RNA and blockade of protein expression are currently used to enhance CAR T cell safety and efficacy by abrogating non-specific toxicity in the form of graft versus host disease (GVHD) and preventing CAR T cell rejection by the host.
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