Distinct populations of antigen-specific tissue-resident CD8+ T cells in human cervix mucosa
Tao Peng, … , Lawrence Corey, Jia Zhu
Tao Peng, … , Lawrence Corey, Jia Zhu
Published June 22, 2021
Citation Information: JCI Insight. 2021;6(15):e149950. https://doi.org/10.1172/jci.insight.149950.
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Research Article Immunology Virology

Distinct populations of antigen-specific tissue-resident CD8+ T cells in human cervix mucosa

Abstract

The ectocervix is part of the lower female reproductive tract (FRT), which is susceptible to sexually transmitted infections (STIs). Comprehensive knowledge of the phenotypes and T cell receptor (TCR) repertoire of tissue-resident memory T cells (TRMs) in the human FRT is lacking. We took single-cell RNA-Seq approaches to simultaneously define gene expression and TCR clonotypes of the human ectocervix. There were significantly more CD8+ than CD4+ T cells. Unsupervised clustering and trajectory analysis identified distinct populations of CD8+ T cells with IFNGhiGZMBloCD69hiCD103lo or IFNGloGZMBhiCD69medCD103hi phenotypes. Little overlap was seen between their TCR repertoires. Immunofluorescence staining showed that CD103+CD8+ TRMs were preferentially localized in the epithelium, whereas CD69+CD8+ TRMs were distributed evenly in the epithelium and stroma. Ex vivo assays indicated that up to 14% of cervical CD8+ TRM clonotypes were HSV-2 reactive in HSV-2–seropositive persons, reflecting physiologically relevant localization. Our studies identified subgroups of CD8+ TRMs in the human ectocervix that exhibited distinct expression of antiviral defense and tissue residency markers, anatomic locations, and TCR repertoires that target anatomically relevant viral antigens. Optimization of the location, number, and function of FRT TRMs is an important approach for improving host defenses to STIs.

Authors

Tao Peng, Khamsone Phasouk, Emily Bossard, Alexis Klock, Lei Jin, Kerry J. Laing, Christine Johnston, Noel A. Williams, Julie L. Czartoski, Dana Varon, Annalyssa N. Long, Jason H. Bielas, Thomas M. Snyder, Harlan Robins, David M. Koelle, M. Juliana McElrath, Anna Wald, Lawrence Corey, Jia Zhu

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Figure 2

Two subsets of CD8+ TRMs with differential expression of tissue residency markers and cytolytic and noncytolytic genes in the human cervix.

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Two subsets of CD8+ TRMs with differential expression of tissue residenc...
Eight cervix samples from 6 participants described in Table 1 were used in the analysis. (A) More CD8+ than CD4+ T cells in the human cervix. P = 0.003 (paired t test, n = 8). (B) Unsupervised clustering analysis of single-cell gene expression data from the 8 cervical samples identified 17 clusters of cells (left). Contribution of the 8 cervical samples to individual clusters of cells (right). (C) UMAP to display gene expression of CD8A, CD4, CD3D, IFNG, GZMB, FOXP3, CD79A, HLA-DRA, SFRP2, KRT5, PECAM1, PROX1, TAGLN, and HBB in individual clusters of cells. CD8A, CD4, CD3D, IFNG, GZMB mark T cells and their cytolytic and noncytolytic gene expression; FOXP3, CD79A, HLA-DRA, SFRP2, KRT5, PECAM1, PROX1, TAGLN, and HBB mark Tregs, B cells, macrophages/monocytes/DCs, fibroblast cells, epithelial cells, vascular endothelial cells, lymphatic endothelial cells, vascular smooth muscle cells, and erythrocytes, respectively. (D) UMAP to display gene expression of CD8A, GZMB, GNLY, ITGAE, ITGA1, IL7R, ZNF683, IFNG, TNF, CCL3, CCL4, CD69, ITGB2, and EOMES. Except CD8A, all the other genes were significantly differentially expressed between the 2 clusters of CD8+ TRM (P < 10–10). The IFNG/CD69hi cluster of cells was labeled as TRM IFNG/CD69hi and the GZMB/ITGAEhi cluster of cells was labeled as TRM GZMB/ITGAEhi. (E) Expression of ITGAE and ITGB7 (CD103), ITGA1 and ITGB1 (CD49a), and ITGAL and ITGB2 (LFA-1) in TRM IFNG/CD69hi and TRM GZMB/ITGAEhi. *Three genes (ITGAE, ITGA1, and ITGB2) were significantly differentially expressed between the 2 subsets of CD8+ TRMs.