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Relationship between Angiotensin-Converting Enzyme Insertion/Deletion Polymorphism and the Risk of COVID-19: A Meta-Analysis

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Introduction. Research shows the correlation between angiotensin-converting enzyme (ACE) deletion and insertion (D/I) polymorphism and COVID-19 risk; yet, conclusive evidence is still lacking. Thus, a meta-analysis of relevant articles was performed to more accurately estimate the relationship of ACE I/D polymorphism with the risk of COVID-19. Material and Methods. Relevant literature from the PubMed database was systematically reviewed, and odds ratios (ORs) and associated 95% confidence intervals (CIs) were measured. Additionally, the metapackage from Stata version 15.0 was used for statistical analysis. Results. The meta-analysis eventually contained 8 studies, including 1362 COVID-19 cases and 4312 controls. Based on the data, the ACE I/D polymorphism did not show an association with COVID-19 risk (D vs. I: [Formula: see text], 95% [Formula: see text]; DD vs. II: [Formula: see text], 95% [Formula: see text]; DI vs. II: [Formula: see text], 95% [Formula: see text]; dominant model: [Formula: see text], 95% [Formula: see text]; and recessive model: [Formula: see text], 95% [Formula: see text]). Further, subgroup analyses stratified based on case proved that the ACE D allele demonstrated an association with increasing risk of COVID-19 severity (D vs. I: [Formula: see text], 95% [Formula: see text]; DD vs. II: [Formula: see text], 95% [Formula: see text]; DI vs. II: [Formula: see text], 95% [Formula: see text]; dominant model: [Formula: see text], 95% [Formula: see text]; and recessive model: [Formula: see text], 95% [Formula: see text]). Conclusions. The ACE D allele was clearly related to an enhanced risk of COVID-19 severity. Hence, it is imperative to take into account the influence of genetic factors during the development of future vaccines.
Title: Relationship between Angiotensin-Converting Enzyme Insertion/Deletion Polymorphism and the Risk of COVID-19: A Meta-Analysis
Description:
Introduction.
Research shows the correlation between angiotensin-converting enzyme (ACE) deletion and insertion (D/I) polymorphism and COVID-19 risk; yet, conclusive evidence is still lacking.
Thus, a meta-analysis of relevant articles was performed to more accurately estimate the relationship of ACE I/D polymorphism with the risk of COVID-19.
Material and Methods.
Relevant literature from the PubMed database was systematically reviewed, and odds ratios (ORs) and associated 95% confidence intervals (CIs) were measured.
Additionally, the metapackage from Stata version 15.
0 was used for statistical analysis.
Results.
The meta-analysis eventually contained 8 studies, including 1362 COVID-19 cases and 4312 controls.
Based on the data, the ACE I/D polymorphism did not show an association with COVID-19 risk (D vs.
I: [Formula: see text], 95% [Formula: see text]; DD vs.
II: [Formula: see text], 95% [Formula: see text]; DI vs.
II: [Formula: see text], 95% [Formula: see text]; dominant model: [Formula: see text], 95% [Formula: see text]; and recessive model: [Formula: see text], 95% [Formula: see text]).
Further, subgroup analyses stratified based on case proved that the ACE D allele demonstrated an association with increasing risk of COVID-19 severity (D vs.
I: [Formula: see text], 95% [Formula: see text]; DD vs.
II: [Formula: see text], 95% [Formula: see text]; DI vs.
II: [Formula: see text], 95% [Formula: see text]; dominant model: [Formula: see text], 95% [Formula: see text]; and recessive model: [Formula: see text], 95% [Formula: see text]).
Conclusions.
The ACE D allele was clearly related to an enhanced risk of COVID-19 severity.
Hence, it is imperative to take into account the influence of genetic factors during the development of future vaccines.

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