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MATE-Seq: microfluidic antigen-TCR engagement sequencing

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Abstract
Adaptive immunity is based on peptide antigen recognition. Our ability to harness the immune system for therapeutic gain relies on the discovery of the T cell receptor (TCR) genes that selectively target antigens from infections, mutated proteins, and foreign agents. Here we present a method that selectively labels peptide antigen-specific CD8+ T cells using magnetic nanoparticles functionalized with peptide-MHC tetramers, isolates these specific cells within an integrated microfluidic device, and directly amplifies the TCR genes for sequencing. Critically, the identity of the peptide recognized by the TCR is preserved, providing the link between peptide and gene. The platform requires inputs on the order of just 100000 CD8+ T cells, can be multiplexed for simultaneous analysis of multiple peptides, and performs sorting and isolation on chip. We demonstrate 1000-fold sensitivity enhancement of detecting antigen-specific TCRs relative to bulk analysis and simultaneous capture of two virus antigen-specific TCRs from a population of T cells.
Author(s)
Ng, Alphonsus H. C.Peng, SongmingXu, Alexander M.Noh, Won JunGuo, KatherineBethune, Michael T.Chour, WilliamChoi, JongchanYang, SungBaltimore, DavidHeath, James R.
Issued Date
2019-09
Type
Article
DOI
10.1039/c9lc00538b
URI
https://scholar.gist.ac.kr/handle/local/12566
Publisher
ROYAL SOC CHEMISTRY
Citation
LAB ON A CHIP, v.19, no.18, pp.3011 - 3021
ISSN
1473-0197
Appears in Collections:
Department of Mechanical and Robotics Engineering > 1. Journal Articles
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