Author: Mitamura, Yasutaka; Schulz, Daniel; Oro, Saskia; Li, Nick; Kolm, Isabel; Lang, Claudia; Ziadlou, Reihane; Tan, Ge; Bodenmiller, Bernd; Steiger, Peter; Marzano, Angelo; de Prost, Nicolas; Caudin, Olivier; Levesque, Mitchell; Stoffel, Corinne; Schmidâ€Grendelmeier, Peter; Maverakis, Emanual; Akdis, Cezmi A.; Brüggen, Marieâ€Charlotte
Title: Cutaneous and systemic hyperinflammation drives maculopapular drug exanthema in severely ill COVIDâ€19 patients Cord-id: uo5jmixg Document date: 2021_7_19
ID: uo5jmixg
Snippet: BACKGROUND: Coronavirus diseaseâ€2019 (COVIDâ€19) has been associated with cutaneous findings, some being the result of drug hypersensitivity reactions such as maculopapular drug rashes (MDR). The aim of this study was to investigate whether COVIDâ€19 may impact the development of the MDR. METHODS: Blood and skin samples from COVIDâ€19 patients (based on a positive nasopharyngeal PCR) suffering from MDR (COVIDâ€MDR), healthy controls, nonâ€COVIDâ€19—related patients with drug rash with
Document: BACKGROUND: Coronavirus diseaseâ€2019 (COVIDâ€19) has been associated with cutaneous findings, some being the result of drug hypersensitivity reactions such as maculopapular drug rashes (MDR). The aim of this study was to investigate whether COVIDâ€19 may impact the development of the MDR. METHODS: Blood and skin samples from COVIDâ€19 patients (based on a positive nasopharyngeal PCR) suffering from MDR (COVIDâ€MDR), healthy controls, nonâ€COVIDâ€19—related patients with drug rash with eosinophilia and systemic symptoms (DRESS), and MDR were analyzed. We utilized imaging mass cytometry (IMC) to characterize the cellular infiltrate in skin biopsies. Furthermore, RNA sequencing transcriptome of skin biopsy samples and highâ€throughput multiplexed proteomic profiling of serum were performed. RESULTS: IMC revealed by clustering analyses a more prominent, phenotypically shifted cytotoxic CD8(+) T cell population and highly activated monocyte/macrophage (Mo/Mac) clusters in COVIDâ€MDR. The RNA sequencing transcriptome demonstrated a more robust cytotoxic response in COVIDâ€MDR skin. However, severe acute respiratory syndrome coronavirus 2 was not detected in skin biopsies at the time point of MDR diagnosis. Serum proteomic profiling of COVIDâ€MDR patients revealed upregulation of various inflammatory mediators (ILâ€4, ILâ€5, ILâ€6, TNF, and IFNâ€Î³), eosinophil and Mo/Mac â€attracting chemokines (MCPâ€2, MCPâ€3, MCPâ€4 and CCL11). Proteomics analyses demonstrated a massive systemic cytokine storm in COVIDâ€MDR compared with the relatively milder cytokine storm observed in DRESS, while MDR did not exhibit such features. CONCLUSION: A systemic cytokine storm may promote activation of Mo/Mac and cytotoxic CD8(+) T cells in severe COVIDâ€19 patients, which in turn may impact the development of MDR.
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