Trafficking of CAR-Engineered Human T Cells Following Regional or Systemic Adoptive Transfer in SCID Beige Mice

被引:0
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作者
Ana Caterina Parente-Pereira
Jerome Burnet
David Ellison
Julie Foster
David Marc Davies
Sjoukje van der Stegen
Sophie Burbridge
Laura Chiapero-Stanke
Scott Wilkie
Stephen Mather
John Maher
机构
[1] King’s College London School of Medicine,The CAR Mechanics Group
[2] Guy’s Hospital Campus,Centre for Molecular Oncology and Imaging, Barts Cancer Institute
[3] Queen Mary University of London,Department of Immunology
[4] Barnet and Chase Farm NHS Trust,Department of Clinical Immunology and Allergy
[5] King’s College Hospital NHS Foundation Trust,Research Oncology, Division of Cancer Studies
[6] King’s College London School of Medicine,undefined
[7] Guy’s Hospital Campus,undefined
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关键词
Adoptive immunotherapy; chimeric antigen receptor; SPECT-CT;
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摘要
Adoptive immunotherapy using chimeric antigen receptor-engrafted T cells is a promising emerging therapy for cancer. Prior to clinical testing, it is mandatory to evaluate human therapeutic cell products in meaningful in vivo pre-clinical models. Here, we describe the use of fused single-photon emission CT–CT imaging to monitor real-time migration of chimeric antigen receptor-engineered T cells in immune compromised (SCID Beige) mice. Following intravenous administration, human T cells migrate in a highly similar manner to that reported in man, but penetrate poorly into established tumors. By contrast, when delivered via intraperitoneal or subcutaneous routes, T cells remain at the site of inoculation with minimal systemic absorption—irrespective of the presence or absence of tumor. Together, these data support the validity of pre-clinical testing of human T-cell immunotherapy in SCID Beige mice. In light of their established efficacy, regional administration of engineered human T cells represents an attractive therapeutic option to minimize toxicity in the treatment of selected malignancies.
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页码:710 / 718
页数:8
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