| Literature DB >> 27882353 |
Yogindra Vedvyas1,2, Enda Shevlin1, Marjan Zaman1, Irene M Min3, Alejandro Amor-Coarasa1, Spencer Park1,2, Susan Park1, Keon-Woo Kwon1, Turner Smith1, Yonghua Luo1, Dohyun Kim1, Young Kim1,4, Benedict Law1, Richard Ting1, John Babich1, Moonsoo M Jin1,2,3.
Abstract
Clinical monitoring of adoptive T cell transfer (ACT) utilizes serial blood analyses to discern T cell activity. While useful, these data are 1-dimensional and lack spatiotemporal information related to treatment efficacy or toxicity. We utilized a human genetic reporter, somatostatin receptor 2 (SSTR2), and PET, to quantitatively and longitudinally visualize whole-body T cell distribution and antitumor dynamics using a clinically approved radiotracer. Initial evaluations determined that SSTR2-expressing T cells were detectable at low densities with high sensitivity and specificity. SSTR2-based PET was applied to ACT of chimeric antigen receptor (CAR) T cells targeting intercellular adhesion molecule-1, which is overexpressed in anaplastic thyroid tumors. Timely CAR T cell infusions resulted in survival of tumor-bearing mice, while later infusions led to uniform death. Real-time PET imaging revealed biphasic T cell expansion and contraction at tumor sites among survivors, with peak tumor burden preceding peak T cell burden by several days. In contrast, nonsurvivors displayed unrelenting increases in tumor and T cell burden, indicating that tumor growth was outpacing T cell killing. Thus, longitudinal PET imaging of SSTR2-positive ACT dynamics enables prognostic, spatiotemporal monitoring with unprecedented clarity and detail to facilitate comprehensive therapy evaluation with potential for clinical translation.Entities:
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Year: 2016 PMID: 27882353 PMCID: PMC5111513 DOI: 10.1172/jci.insight.90064
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708