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In vivo tracking of T cells in humans unveils decade-long survival and activity of genetically modified T memory stem cells

干细胞 基因工程 体内 转基因生物 生物 转基因 细胞生物学 免疫学 癌症研究 基因 遗传学
作者
Luca Biasco,Serena Scala,Luca Basso‐Ricci,Francesca Dionisio,Cristina Baricordi,Andrea Calabria,Stefania Giannelli,Nicoletta Cieri,Federica Barzaghi,Roberta Pajno,Hamoud Al‐Mousa,Alessia Scarselli,Caterina Cancrini,Claudio Bordignon,Maria Grazia Roncarolo,Eugenio Montini,Chiara Bonini,Alessandro Aiuti
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science]
卷期号:7 (273) 被引量:161
标识
DOI:10.1126/scitranslmed.3010314
摘要

A definitive understanding of survival and differentiation potential in humans of T cell subpopulations is of paramount importance for the development of effective T cell therapies. In particular, uncovering the dynamics in vivo in humans of the recently described T memory stem cells (TSCM) would be crucial for therapeutic approaches that aim at taking advantage of a stable cellular vehicle with precursor potential. We exploited data derived from two gene therapy clinical trials for an inherited immunodeficiency, using either retrovirally engineered hematopoietic stem cells or mature lymphocytes to trace individual T cell clones directly in vivo in humans. We compared healthy donors and bone marrow-transplanted patients, studied long-term in vivo T cell composition under different clinical conditions, and specifically examined TSCM contribution according to age, conditioning regimen, disease background, cell source, long-term reconstitution, and ex vivo gene correction processing. High-throughput sequencing of retroviral vector integration sites (ISs) allowed tracing the fate of more than 1700 individual T cell clones in gene therapy patients after infusion of gene-corrected hematopoietic stem cells or mature lymphocytes. We shed light on long-term in vivo clonal relationships among different T cell subtypes, and we unveiled that TSCM are able to persist and to preserve their precursor potential in humans for up to 12 years after infusion of gene-corrected lymphocytes. Overall, this work provides high-resolution tracking of T cell fate and activity and validates, in humans, the safe and functional decade-long survival of engineered TSCM, paving the way for their future application in clinical settings.
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