4.7 Article

Comprehensive analysis of TCR repertoire in COVID-19 using single cell sequencing

Journal

GENOMICS
Volume 113, Issue 2, Pages 456-462

Publisher

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.ygeno.2020.12.036

Keywords

COVID-19; scTCR-seq; TCR repertoire; TCR bias

Funding

  1. National Natural Science Foundation of China [61822108, 62041102, 6203000303]
  2. Emergency Research Project for COVID-19 of Harbin Institute of Technology [2020-001]

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This study analyzed the TCR repertoire in COVID-19 patients using single-cell V(D)J sequencing and found distinct T cell clonal expansion as well as significant changes in VJ gene combinations. Moreover, preferential usage of V and J gene segments was observed in samples infected by different viruses, providing novel insights on the immune response in COVID-19.
T-cell receptor (TCR) is crucial in T cell-mediated virus clearance. To date, TCR bias has been observed in various diseases. However, studies on the TCR repertoire of COVID-19 patients are lacking. Here, we used single-cell V (D)J sequencing to conduct comparative analyses of TCR repertoire between 12 COVID-19 patients and 6 healthy controls, as well as other virus-infected samples. We observed distinct T cell clonal expansion in COVID-19. Further analysis of VJ gene combination revealed 6 VJ pairs significantly increased, while 139 pairs significantly decreased in COVID-19 patients. When considering the VJ combination of alpha and beta chains at the same time, the combination with the highest frequency on COVID-19 was TRAV12-2-J27-TRBV7-9-J2-3. Besides, preferential usage of V and J gene segments was also observed in samples infected by different viruses. Our study provides novel insights on TCR in COVID-19, which contribute to our understanding of the immune response induced by SARS-CoV-2.

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