Author: Parackova, Zuzana; Bloomfield, Marketa; Klocperk, Adam; Sediva, Anna
Title: Neutrophils mediate Th17 promotion in COVIDâ€19 patients Cord-id: ol7gl7wm Document date: 2020_12_2
ID: ol7gl7wm
Snippet: From the beginning of 2020, an urgent need to understand the pathophysiology of SARSâ€CoVâ€2 disease (COVIDâ€19), much of which is due to dysbalanced immune responses, resonates across the world. COVIDâ€19â€associated neutrophilia, increased neutrophilâ€toâ€lymphocyte ratio, aberrant neutrophil activation, and infiltration of neutrophils into lungs suggest that neutrophils are important players in the disease immunopathology. The main objective of this study was to assess the phenotypic a
Document: From the beginning of 2020, an urgent need to understand the pathophysiology of SARSâ€CoVâ€2 disease (COVIDâ€19), much of which is due to dysbalanced immune responses, resonates across the world. COVIDâ€19â€associated neutrophilia, increased neutrophilâ€toâ€lymphocyte ratio, aberrant neutrophil activation, and infiltration of neutrophils into lungs suggest that neutrophils are important players in the disease immunopathology. The main objective of this study was to assess the phenotypic and functional characteristics of neutrophils in COVIDâ€19 patients, with particular focus on the interaction between neutrophils and T cells. We hypothesize that the altered functional characteristics of COVIDâ€19 patientâ€derived neutrophils result in skewed Th1/Th17 adaptive immune response, thus contributing to disease pathology. The expansion of Gâ€MDSC and immature forms of neutrophils was shown in the COVIDâ€19 patients. In the COVIDâ€19 neutrophil/T cell cocultures, neutrophils caused a strong polarity shift toward Th17, and, conversely, a reduction of IFNγâ€producing Th1 cells. The Th17 promotion was NOS dependent. Neutrophils, the known modulators of adaptive immunity, skew the polarization of T cells toward the Th17 promotion and Th1 suppression in COVIDâ€19 patients, contributing to the discoordinated orchestration of immune response against SARSâ€CoVâ€2. As ILâ€17 and other Th17â€related cytokines have previously been shown to correlate with the disease severity, we suggest that targeting neutrophils and/or Th17 represents a potentially beneficial therapeutic strategy for severe COVIDâ€19 patients.
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