Single-Cell Omics Reveals Dyssynchrony of the Innate and Adaptive Immune System in Progressive COVID-19

Unterman, Avraham; Sumida, Tomokazu; Nouri, Nima; Yan, Xiting; Zhao, Amy; Gasque, Victor; Schupp, Jonas C.; Asashima, Hiromitsu; Liu, Yunqing; Cosme, Carlos; Deng, Wenxuan; Chen, Ming; Raredon, Micha Sam Brickman; Hoehn, Kenneth B.; Wang, Guilin; Wang, Zuoheng; DeIuliis, Giuseppe; Ravindra, Neal G.; Li, Ningshan; Castaldi, Christopher; Wong, Patrick; Fournier, John; Bermejo, Santos; Sharma, Lokesh; Casanovas‐Massana, Arnau; Vogels, Chantal B.F.; Wyllie, Anne L.; Grubaugh, Nathan D.; Melillo, Anthony; Meng, Hailong; Minasyan, Maksym; Niklason, Laura E.; Ko, Albert Icksang; Montgomery, Ruth R.; Farhadian, Shelli; Iwasaki, Akiko; Shaw, Albert C.; Dijk, David van; Zhao, Hongyu; Kleinstein, Steven H.; Hafler, David A.; Kaminski, Naftali; Cruz, Charles S. Dela

doi:10.1101/2020.07.16.20153437

Cited by 36 publications

(81 citation statements)

References 107 publications

(115 reference statements)

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“…Consistent with previous scRNAseq studies, COVID19-A samples also showed an elevated S100A score compared to A.HD (Figure 3d) 19 . Pathway enrichment on shared down-regulated genes in monocytes and neutrophils revealed a significant reduction in antigen-presentation and processing, and as in COVID-19 23 , MIS-C patients had significantly reduced HLA class II (HLA-DP, DQ, and DR) expression ( Figure 3e there was a significant enrichment in myeloid-derived proteins among the differentially expressed proteins in serum (p = 1.7x10 -12 ) (Figure 3g).…”

Section: Elevated Alarmin Expression In Myeloid Cells With Post-inflasupporting

confidence: 91%

Post-infectious inflammatory disease in MIS-C features elevated cytotoxicity signatures and autoreactivity that correlates with severity

Ramaswamy¹,

Brodsky²,

Sumida³

et al. 2020

Preprint

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SUMMARYMultisystem inflammatory syndrome in children (MIS-C) is a life-threatening post-infectious complication occurring unpredictably weeks after mild or asymptomatic SARS-CoV2 infection in otherwise healthy children. Here, we define immune abnormalities in MIS-C compared to adult COVID-19 and pediatric/adult healthy controls using single-cell RNA sequencing, antigen receptor repertoire analysis, unbiased serum proteomics, and in vitro assays. Despite no evidence of active infection, we uncover elevated S100A-family alarmins in myeloid cells and marked enrichment of serum proteins that map to myeloid cells and pathways including cytokines, complement/coagulation, and fluid shear stress in MIS-C patients. Moreover, NK and CD8 T cell cytotoxicity genes are elevated, and plasmablasts harboring IgG1 and IgG3 are expanded. Consistently, we detect elevated binding of serum IgG from severe MIS-C patients to activated human cardiac microvascular endothelial cells in culture. Thus, we define immunopathology features of MIS-C with implications for predicting and managing this SARS-CoV2-induced critical illness in children.

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Section: Elevated Alarmin Expression In Myeloid Cells With Post-inflasupporting

confidence: 91%

Post-infectious inflammatory disease in MIS-C features elevated cytotoxicity signatures and autoreactivity that correlates with severity

Ramaswamy¹,

Brodsky²,

Sumida³

et al. 2020

Preprint

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“…While proof-of-principle, our classifier of severe disease shows robustness and overall value in predicting disease progression based on immune profiling and near-real-time disease monitoring. Thus, it may be valuable to inform clinical action like that proposed in chronic diseases with other high-dimensional assays [50][51][52] . Moreover, we demonstrated that a classifier with a limited number of markers retains good performance.…”

Section: Discussionmentioning

confidence: 99%

“…While this may not necessarily imply absolute changes in cell numbers, we observed good overall agreement between changes in proportions and absolute counts when comparing severe and mild disease status ( Supplementary Figure 6 and Supplementary Table 7). This highlights the importance of studies employing orthogonal modalities such as cytokine profiling 51 , single-cell RNA sequencing [52][53][54][55][56] , and their integration 57,58 . Nevertheless, even without orthogonal studies, our machine learning approach for predicting disease severity demonstrates predictive potential, although it should be tested in a validation cohort before use in a clinical setting.…”

Section: Discussionmentioning

confidence: 99%

Longitudinal immune profiling of mild and severe COVID-19 reveals innate and adaptive immune dysfunction and provides an early prediction tool for clinical progression

Rendeiro

Casano

Vorkas

et al. 2020

Preprint

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With a rising incidence of COVID-19-associated morbidity and mortality worldwide, it is critical to elucidate the innate and adaptive immune responses that drive disease severity. We performed longitudinal immune profiling of peripheral blood mononuclear cells from 45 patients and healthy donors. We observed a dynamic immune landscape of innate and adaptive immune cells in disease progression and absolute changes of lymphocyte and myeloid cells in severe versus mild cases or healthy controls. Intubation and death were coupled with selected natural killer cell KIR receptor usage and IgM+ B cells and associated with profound CD4 and CD8 T cell exhaustion. Pseudo-temporal reconstruction of the hierarchy of disease progression revealed dynamic time changes in the global population recapitulating individual patients and the development of an eight-marker classifier of disease severity. Estimating the effect of clinical progression on the immune response and early assessment of disease progression risks may allow implementation of tailored therapies.

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“…ARID5A, SOCS3, PIM1, BCL3, BATF, MYC that are associated with the IL-6 pathway 56 . Cytotoxicity associated genes include PRF1, GZMH, IFNG, NKG7, KLRG1, PRF1 56 and GNLY, GZMB, GZMK 78 .…”

Section: Methodsmentioning

confidence: 99%

Chronic lung diseases are associated with gene expression programs favoring SARS-CoV-2 entry and severity

Bui

Winters

Chung

et al. 2020

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Patients with chronic lung disease (CLD) have an increased risk for severe coronavirus disease-19 (COVID-19) and poor outcomes. Here, we analyzed the transcriptomes of 605,904 single cells isolated from healthy and CLD lungs to identify molecular characteristics of lung cells that may account for worse COVID-19 outcomes in patients with chronic lung diseases. We observed a similar cellular distribution and relative expression of SARS-CoV-2 entry factors in control and CLD lungs. CLD epithelial cells expressed higher levels of genes linked directly to the efficiency of viral replication and innate immune response. Additionally, we identified basal differences in inflammatory gene expression programs that highlight how CLD alters the inflammatory microenvironment encountered upon viral exposure to the peripheral lung. Our study indicates that CLD is accompanied by changes in cell-type-specific gene expression programs that prime the lung epithelium for and influence the innate and adaptive immune responses to SARS-CoV-2 infection.

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Single-Cell Omics Reveals Dyssynchrony of the Innate and Adaptive Immune System in Progressive COVID-19

Cited by 36 publications

References 107 publications

Post-infectious inflammatory disease in MIS-C features elevated cytotoxicity signatures and autoreactivity that correlates with severity

Post-infectious inflammatory disease in MIS-C features elevated cytotoxicity signatures and autoreactivity that correlates with severity

Longitudinal immune profiling of mild and severe COVID-19 reveals innate and adaptive immune dysfunction and provides an early prediction tool for clinical progression

Chronic lung diseases are associated with gene expression programs favoring SARS-CoV-2 entry and severity

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