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Spatial transcriptomics demonstrates the role of CD4 T cells in effector CD8 T cell differentiation during chronic viral infection

Paytsar Topchyan, Ryan Zander, Moujtaba Y. Kasmani, Christine Nguyen, Ashley K. Brown, Siying Lin, Robert Burns, Weiguo Cui

2022Cell Reports22 citationsDOIOpen Access PDF

Abstract

CD4 T cell help is critical to sustain effector CD8 T cell responses during chronic infection, notably via T follicular helper (Tfh)-derived interleukin-21 (IL-21). Conversely, CD4 depletion results in severe CD8 T cell dysfunction and lifelong viremia despite CD4 T cell reemergence following transient depletion. These observations suggest that repopulating CD4 subsets are functionally or numerically insufficient to orchestrate a robust CD8 response. We utilize spatial transcriptomics and single-cell RNA sequencing (scRNA-seq) to investigate CD4 T cell heterogeneity under CD4-replete and -deplete conditions and explore cellular interactions during chronic infection. Although IL-21-producing Tfh cells repopulate following transient CD4 depletion, they are outnumbered by immunomodulatory CD4 T cells. Moreover, the splenic architecture appears perturbed, with decreases in white pulp regions, coinciding with germinal center losses. These disruptions in splenic architecture are associated with diminished Tfh and progenitor CD8 T cell colocalization, providing a potential mechanism for impaired progenitor-to-effector CD8 T cell differentiation during "un-helped" conditions.

Topics & Concepts

EffectorTranscriptomeCD8BiologyCytotoxic T cellCell biologyImmunologyCellular differentiationViral infectionVirologyVirusGeneticsImmune systemGene expressionGeneIn vitroT-cell and B-cell ImmunologyImmune Cell Function and InteractionImmunotherapy and Immune Responses
Spatial transcriptomics demonstrates the role of CD4 T cells in effector CD8 T cell differentiation during chronic viral infection | Litcius