Publication | Open Access
COVID-19 patients with high TNF/IFN-γ levels show hallmarks of PANoptosis, an inflammatory cell death
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Citations
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References
2023
Year
TNF and IFN-γ trigger cell damage during SARS CoV-2 infection; these cytokines can induce senescence and a cell death process called PANoptosis. This study included 138 vaccine-naïve COVID-19 patients, who were divided into four groups (Gp) according to the plasma level of TNF and IFN-γ (High [<sup>Hi</sup>] or Normal-Low [<sup>No-Low</sup>]), Gp 1: TNF<sup>Hi</sup>/IFNγ<sup>Hi</sup>; Gp 2: TNF<sup>Hi</sup>/IFNγ<sup>No-Low</sup>; Gp 3: TNF<sup>No-Low</sup>/IFNγ<sup>Hi</sup>; and Gp 4: TNF<sup>No-Low</sup>/IFNγ<sup>No-Low</sup>. Thirty-five apoptosis-related proteins and molecules related to cell death and senescence were evaluated. Our results showed that groups did not display differences in age and comorbidities. However, 81% of the Gp 1 patients had severe COVID-19, and 44% died. Notably, the p21/CDKN1A was increased in Gp 2 and Gp 3. Moreover, Gp 1 showed higher TNFR1, MLKL, RIPK1, NLRP3, Caspase 1, and HMGB-1 levels, suggesting elevated TNF and IFN-γ levels simultaneously activate diverse cell death pathways because it is not observed when only one of these cytokines is increased. Thus, high TNF/IFN-γ levels are predominant in severe COVID-19 status, and patients display cell alterations associated with the activation of diverse cell death pathways, including a possible senescent phenotype.
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