Literature DB >> 33363531

Single Cell Transcriptomics Implicate Novel Monocyte and T Cell Immune Dysregulation in Sarcoidosis.

Lori Garman1, Richard C Pelikan1, Astrid Rasmussen1, Caleb A Lareau2, Kathryn A Savoy1, Umesh S Deshmukh3, Harini Bagavant3, Albert M Levin4, Salim Daouk5, Wonder P Drake6, Courtney G Montgomery1.   

Abstract

Sarcoidosis is a systemic inflammatory disease characterized by infiltration of immune cells into granulomas. Previous gene expression studies using heterogeneous cell mixtures lack insight into cell-type-specific immune dysregulation. We performed the first single-cell RNA-sequencing study of sarcoidosis in peripheral immune cells in 48 patients and controls. Following unbiased clustering, differentially expressed genes were identified for 18 cell types and bioinformatically assessed for function and pathway enrichment. Our results reveal persistent activation of circulating classical monocytes with subsequent upregulation of trafficking molecules. Specifically, classical monocytes upregulated distinct markers of activation including adhesion molecules, pattern recognition receptors, and chemokine receptors, as well as enrichment of immunoregulatory pathways HMGB1, mTOR, and ephrin receptor signaling. Predictive modeling implicated TGFβ and mTOR signaling as drivers of persistent monocyte activation. Additionally, sarcoidosis T cell subsets displayed patterns of dysregulation. CD4 naïve T cells were enriched for markers of apoptosis and Th17/Treg differentiation, while effector T cells showed enrichment of anergy-related pathways. Differentially expressed genes in regulatory T cells suggested dysfunctional p53, cell death, and TNFR2 signaling. Using more sensitive technology and more precise units of measure, we identify cell-type specific, novel inflammatory and regulatory pathways. Based on our findings, we suggest a novel model involving four convergent arms of dysregulation: persistent hyperactivation of innate and adaptive immunity via classical monocytes and CD4 naïve T cells, regulatory T cell dysfunction, and effector T cell anergy. We further our understanding of the immunopathology of sarcoidosis and point to novel therapeutic targets.
Copyright © 2020 Garman, Pelikan, Rasmussen, Lareau, Savoy, Deshmukh, Bagavant, Levin, Daouk, Drake and Montgomery.

Entities:  

Keywords:  RNA sequencing analysis; cell migration; classical monocytes; lymphocyte activation; regulatory T cells; sarcoidosis

Year:  2020        PMID: 33363531      PMCID: PMC7753017          DOI: 10.3389/fimmu.2020.567342

Source DB:  PubMed          Journal:  Front Immunol        ISSN: 1664-3224            Impact factor:   7.561


  55 in total

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4.  Transcriptome Analysis of Peripheral Blood Mononuclear Cells in Pulmonary Sarcoidosis.

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5.  The landscape of transcriptomic and proteomic studies in sarcoidosis.

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