Single cell analysis of host response to helminth infection reveals the clonal breadth, heterogeneity, and tissue-specific programming of the responding CD4+ T cell repertoire

Author:

Brown Ivy K.ORCID,Dyjack NathanORCID,Miller Mindy M.ORCID,Krovi HarshaORCID,Rios Cydney,Woolaver RachelORCID,Harmacek Laura,Tu Ting-HuiORCID,O’Connor Brian P.ORCID,Danhorn ThomasORCID,Vestal BrianORCID,Gapin LaurentORCID,Pinilla Clemencia,Seibold Max A.ORCID,Scott-Browne James,Santos Radleigh G.ORCID,Reinhardt R. LeeORCID

Abstract

The CD4+ T cell response is critical to host protection against helminth infection. How this response varies across different hosts and tissues remains an important gap in our understanding. Using IL-4-reporter mice to identify responding CD4+ T cells to Nippostrongylus brasiliensis infection, T cell receptor sequencing paired with novel clustering algorithms revealed a broadly reactive and clonally diverse CD4+ T cell response. While the most prevalent clones and clonotypes exhibited some tissue selectivity, most were observed to reside in both the lung and lung-draining lymph nodes. Antigen-reactivity of the broader repertoires was predicted to be shared across both tissues and individual mice. Transcriptome, trajectory, and chromatin accessibility analysis of lung and lymph-node repertoires revealed three unique but related populations of responding IL-4+ CD4+ T cells consistent with T follicular helper, T helper 2, and a transitional population sharing similarity with both populations. The shared antigen reactivity of lymph node and lung repertoires combined with the adoption of tissue-specific gene programs allows for the pairing of cellular and humoral responses critical to the orchestration of anti-helminth immunity.

Funder

National Institutes of Health

Publisher

Public Library of Science (PLoS)

Subject

Virology,Genetics,Molecular Biology,Immunology,Microbiology,Parasitology

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