| Literature DB >> 32901086 |
Xin-Yu Wang1, Yan Wang2,3, Qiong Wu1, Jing-Jing Liu1, Yu Liu1, Dong-Hui Pan1, Wei Qi4, Li-Zhen Wang1, Jun-Jie Yan1, Yu-Ping Xu1, Guang-Ji Wang5, Li-Yan Miao6,7, Lei Yu8, Min Yang9.
Abstract
Clinical tracking of chimeric antigen receptor (CAR) T cells in vivo by positron emission tomography (PET) imaging is an area of intense interest. But the long-lived positron emitter-labeled CAR T cells stay in the liver and spleen for days or even weeks. Thus, the excessive absorbed effective dose becomes a major biosafety issue leading it difficult for clinical translation. In this study we used 68Ga, a commercially available short-lived positron emitter, to label CAR T cells for noninvasive cell tracking in vivo. CAR T cells could be tracked in vivo by 68Ga-PET imaging for at least 6 h. We showed a significant correlation between the distribution of 89Zr and 68Ga-labeled CAR T cells in the same tissues (lungs, liver, and spleen). The distribution and homing behavior of CAR T cells at the early period is highly correlated with the long-term fate of CAR T cells in vivo. And the effective absorbed dose of 68Ga-labeled CAR T cells is only one twenty-fourth of 89Zr-labeled CAR T cells, which was safe for clinical translation. We conclude the feasibility of 68Ga instead of 89Zr directly labeling CAR T cells for noninvasive tracking of the cells in vivo at an early stage based on PET imaging. This method provides a potential solution to the emerging need for safe and practical PET tracer for cell tracking clinically.Entities:
Keywords: CAR T; Gallium-68; Zirconium-89; cell tracking; noninvasive imaging; positron emission tomography
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Year: 2020 PMID: 32901086 PMCID: PMC8115074 DOI: 10.1038/s41401-020-00511-5
Source DB: PubMed Journal: Acta Pharmacol Sin ISSN: 1671-4083 Impact factor: 6.150