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Association between inflammatory cytokines/chemokines, clinical laboratory parameters, disease severity and in-hospital mortality in critical and mild COVID-19 patients without comorbidities or immune-mediated diseases.
Document Type
Article
Author
Hamza, MuaawiaAlhujaily, MuhanadAlosaimi, BandarEl Bakkouri, KarimAlDughaim, Mohammed S.Alonazi, MonaAlanazi, Mona AwadAbbass, BasmaAlshehri, AbdulsalamAl-Shouli, Samia T.Alturaiki, WaelAwadalla, Maaweya
Source
Journal of Immunoassay & Immunochemistry. 2023, Vol. 44 Issue 1, p13-30. 18p.
Subject
*COVID-19
*INFLAMMATORY mediators
*CHEMOKINES
*HUMORAL immunity
*HOSPITAL mortality
*PATHOLOGICAL laboratories
Language
ISSN
1532-1819
Abstract
There are limited data on inflammatory cytokines and chemokines; the humoral immune response; and main clinical laboratory parameters as indicators for disease severity and mortality in patients with critical and mild COVID-19 without comorbidities or immune-mediated diseases in Saudi Arabia. We determined the expression levels of major proinflammatory cytokines and chemokines; C-reactive protein (CRP); procalcitonin; SARS-CoV-2 IgM antibody and twenty-two clinical laboratory parameters and assessed their usefulness as indicators of disease severity and in-hospital death. Our results showed a significant increase in the expression levels of SARS-CoV-2 IgM antibody; IL1-β; IL-6; IL-8; TNF-α and CRP in critical COVID-19 patients; neutrophil count; urea; creatinine and troponin were also increased. The elevation of these biomarkers was significantly associated and positively correlated with in-hospital death in critical COVID-19 patients. Our results suggest that the levels of IL1-β; IL-6; IL-8; TNF-α; and CRP; neutrophil count; urea; creatinine; and troponin could be used to predict disease severity in COVID-19 patients without comorbidities or immune-mediated diseases. These inflammatory mediators could be used as predictive early biomarkers of COVID-19 disease deterioration; shock and death among COVID-19 patients without comorbidities or immune-mediated diseases. [ABSTRACT FROM AUTHOR]

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