MBL deficiency-causing B allele (rs1800450) as a risk factor for severe COVID-19

Speletas, Matthaios; Dadouli, Katerina; Syrakouli, Argyro; Gatselis, Nikolaos; Mouchtouri, Varvara A.; Koulas, Ioannis; Samakidou, Anna; Nikolaidou, Anastasia; Stefos, Aggelos; Mimtsoudis, Iordanis; Hatzianastasiou, Sophia; Koureas, Michalis; Anagnostopoulos, Lemonia; Tseroni, Maria; Tsinti, Gerasimina; Metallidis, Symeon; Dalekos, George Ν.; Hadjichristodoulou, Christos

doi:10.1016/j.imbio.2021.152136

Cited by 17 publications

(19 citation statements)

References 32 publications

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“…This supports the association of the MBL2 B allele with a lower level of serum MBL following infection by SARS-CoV-2. The MBL2 B allele was demonstrated to be a risk factor for severe COVID-19 in some previous studies, and hence MBL2 gene variants are thought to play a very important role in COVID-19 susceptibility and disease severity [ 21 , 22 ]. Speletas et al [ 21 ] demonstrated that the presence of the MBL deficiency-causing B allele ( rs1800450 ) was associated with an almost 2-fold increased risk of developing pneumonia and requiring hospitalization, suggesting its utility as a molecular predictor of disease severity in individuals with COVID-19.…”

Section: Discussionmentioning

confidence: 99%

Association of the Mannose-Binding Lectin 2 BB Genotype with COVID-19-Related Mortality

Kashiwagi

Suzuki

Takahashi

et al. 2023

Life

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Mannose-binding lectin (MBL) is crucial in first-line immune defenses. There are still many unknown factors regarding the mechanisms causing variability in the clinical course of coronavirus disease 2019 (COVID-19). In Japan, there have been few reports to date regarding the association between MBL and COVID-19. It has been demonstrated that the MBL2 gene B variant at codon 54 (rs1800450) is associated with variabilities in the clinical course of COVID-19. We aimed to investigate how the level of serum MBL and the codon 54 variant of MBL (rs1800450) affect the disease severity of COVID-19. A total of 59 patients from the fourth wave and 49 patients from the fifth wave in Japan were analyzed based on serum MBL levels using ELISA and the genotype of MBL2 codon 54 using PCR reaction. There was no significant association between serum MBL levels and age. MBL2 genotype was independent of age, there was no significant difference in different COVID-19 severities, MBL genotypes, and serum MBL levels. Binary logistic regression analysis to identify predisposing factors for severe COVID-19 symptoms demonstrated that patients with the BB genotype had a higher risk of death from COVID-19. Our results quantitatively demonstrated that the BB genotype might be a factor associated with death from COVID-19.

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Section: Discussionmentioning

confidence: 99%

Association of the Mannose-Binding Lectin 2 BB Genotype with COVID-19-Related Mortality

Kashiwagi

Suzuki

Takahashi

et al. 2023

Life

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“…[7,17] PKR plays a role in the course of COVID-19 infection, including a regulatory role [6,18] in the virus-induced stress response and induces possible insulin resistance, [6] contributing to the progression of pathophysiological processes in COVID-19 patients with comorbid diabetes. MBL2 gene polymorphisms [19] are thought to be associated with the severity of COVID-19 infection, and the presence of the B allele (rs1800450) [20] due to MBL deficiency is associated with poorer clinical presentation of patients, including the need for hospitalization and the need for ventilator use. [20] Certain genetic polymorphisms [21][22][23] in INFL4 may contribute to population susceptibility to COVID-19, but its association with disease severity still requires additional animal studies or clinical studies to reveal.…”

Section: Discussionmentioning

confidence: 99%

IFNL4, ACE1, PKR, IFNG, MBL2 genetic polymorphisms and severe COVID-19

Bao

2022

Medicine

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Background: Corona virus disease 2019 (COVID-19) is caused by SARS-CoV-2, the pathogenic process of SARS-Cov-2 is related to the angiotensin-2 converting enzyme (ACE-2) on host cells. The genetic polymorphisms among different populations may influence the progression of COVID-19. However, the effects of IFNL4, ACE1, PKR, IFNG, and MBL2 in severe COVID-19 have not been systematically assessed.Methods: We will include all relevant English and Chinese studies by searching the following electronic databases: PubMed, MEDLINE, Embase, Web of Science, Scopus, the Cochrane Library, and Google Scholar before March 31, 2022. Two researchers will independently screen and extract the literature. The methodological quality of the included studies will be evaluated by the Cochrane Handbook for Systematic Reviews of Interventions.Result: This systematic review and meta-analysis will summarize the association of IFNL4, ACE1, PKR, IFNG, MBL2 genetic polymorphisms, and severe COVID-19. The results will be submitted to a peer-reviewed journal once completed. Conclusion:The conclusion of our study will provide evidence for the early prevention of severe COVID-19.

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“…Gavriilaki et al used targeted next-generation sequencing and identified C3 variants as independent predictors of disease severity, ICU admission, and/or mortality, strengthening the hypothesis of genetic susceptibility in severe COVID-19[ 39 , 40 ]. Other genetic polymorphisms associated with severe disease include the mannose binding lectin gene 2 (rs1800450)[ 41 , 42 ] and the chromosome 3 rs11385942 G>GA variant that has been associated with complement overactivation (formation of C5a and MAC)[ 43 ].…”

Section: Complement Activation In Severe Covid-19mentioning

confidence: 99%

“…Common side effects include headache, upper respiratory infection, fatigue, nausea, vomiting, diarrhea, hypokalemia, neutropenia and fever[ 108 , 109 ]. A recently identified variant in the MBL gene 2 (rs1800450) has been associated with the need for hospitalization, severe disease, ICU admission, and development of pneumonia potentially suggesting a new therapeutic target[ 41 , 42 ].…”

Section: Complement Inhibition As An Effective Target With Therapeuti...mentioning

confidence: 99%

Complement-mediated microvascular injury and thrombosis in the pathogenesis of severe COVID-19: A review

Gianni

Goldin

Ngu

et al. 2022

WJEM

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Coronavirus disease 2019 (COVID-19) causes acute microvascular thrombosis in both venous and arterial structures which is highly associated with increased mortality. The mechanisms leading to thromboembolism are still under investigation. Current evidence suggests that excessive complement activation with severe amplification of the inflammatory response (cytokine storm) hastens disease progression and initiates complement-dependent cytotoxic tissue damage with resultant prothrombotic complications. The concept of thromboinflammation, involving overt inflammation and activation of the coagulation cascade causing thrombotic microangiopathy and end-organ damage, has emerged as one of the core components of COVID-19 pathogenesis. The complement system is a major mediator of the innate immune response and inflammation and thus an appealing treatment target. In this review, we discuss the role of complement in the development of thrombotic microangiopathy and summarize the current data on complement inhibitors as COVID-19 therapeutics.

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MBL deficiency-causing B allele (rs1800450) as a risk factor for severe COVID-19

Cited by 17 publications

References 32 publications

Association of the Mannose-Binding Lectin 2 BB Genotype with COVID-19-Related Mortality

Association of the Mannose-Binding Lectin 2 BB Genotype with COVID-19-Related Mortality

IFNL4, ACE1, PKR, IFNG, MBL2 genetic polymorphisms and severe COVID-19

Complement-mediated microvascular injury and thrombosis in the pathogenesis of severe COVID-19: A review

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