Please use this identifier to cite or link to this item: https://doi.org/10.1126/sciadv.adf3120
Title: Cord blood-derived V62+and V62-T cells acquire differential cell state compositions upon in vitro expansion
Authors: Ng, Jeremy Wee Kiat
Tan, Kar Wai 
Guo, Dian Yan
Lai, Joey Jia Hui
Fan, Xiubo 
Poon, Zhiyong
Lim, Tse Hui 
Lim, Alvin Soon Tiong 
Lim, Tony Kiat Hon
Hwang, William Ying Khee 
Li, Shang 
Eaves, Connie J
Goh, Yeow Tee 
Cheung, Alice Man Sze
Keywords: Science & Technology
Multidisciplinary Sciences
Science & Technology - Other Topics
DELTA-T-CELLS
RECOGNITION
IMMUNOTHERAPY
RECEPTOR
COMPLEX
Issue Date: 16-Jun-2023
Publisher: AMER ASSOC ADVANCEMENT SCIENCE
Citation: Ng, Jeremy Wee Kiat, Tan, Kar Wai, Guo, Dian Yan, Lai, Joey Jia Hui, Fan, Xiubo, Poon, Zhiyong, Lim, Tse Hui, Lim, Alvin Soon Tiong, Lim, Tony Kiat Hon, Hwang, William Ying Khee, Li, Shang, Eaves, Connie J, Goh, Yeow Tee, Cheung, Alice Man Sze (2023-06-16). Cord blood-derived V62+and V62-T cells acquire differential cell state compositions upon in vitro expansion. SCIENCE ADVANCES 9 (24). ScholarBank@NUS Repository. https://doi.org/10.1126/sciadv.adf3120
Abstract: Human cord blood-derived γδ T cells (CBγδ) display a highly diverse TCRγδ repertoire and have a unique subtype composition different from fetal or adult peripheral blood counterparts. We expanded CBγδ in vitro using an irradiated Epstein-Barr virus-transformed feeder cell-based modified rapid expansion protocol (REP). Singlecell RNA sequencing tracked progressive differentiation of naive CBγδ into cells expressing neoantigen-reactive tumor-infiltrating lymphocyte aswell as tissue-resident memory precursor-like and antigen-presenting cell-like gene signatures. TCRγδ clonal tracing revealed a bias toward cytotoxic effector differentiation in a much larger proportion of Vδ2- clones compared to Vδ2+ clones, resulting in the former being more cytotoxic at the population level. These clonotype-specific differentiation dynamics were not restricted to REP and were recapitulated upon secondary nonviral antigen stimulations. Thus, our data showed intrinsic cellular differences between major subtypes of human γδ T cells already in operation at early postnatal stage and highlighted key areas of consideration in optimizing cell manufacturing processes.
Source Title: SCIENCE ADVANCES
URI: https://scholarbank.nus.edu.sg/handle/10635/248815
ISSN: 2375-2548
DOI: 10.1126/sciadv.adf3120
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