Evaluation of Mannose Binding Lectin Gene Variants in Pediatric Influenza Virus-Related Critical Illness

Background: Mannose-binding lectin (MBL) is an innate immune protein with strong biologic plausibility for protecting against influenza virus-related sepsis and bacterial co-infection. In an autopsy cohort of 105 influenza-infected young people, carriage of the deleterious MBL gene MBL2_Gly54Asp(“B”...

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Autores principales: Levy, Emily R., Yip, Wai-Ki, Super, Michael, Ferdinands, Jill M., Mistry, Anushay J., Newhams, Margaret M., Zhang, Yu, Su, Helen C., McLaughlin, Gwenn E., Sapru, Anil, Loftis, Laura L., Weiss, Scott L., Hall, Mark W., Cvijanovich, Natalie, Schwarz, Adam, Tarquinio, Keiko M., Mourani, Peter M., Randolph, Adrienne G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2019
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6518443/
https://www.ncbi.nlm.nih.gov/pubmed/31139182
http://dx.doi.org/10.3389/fimmu.2019.01005
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author Levy, Emily R.
Yip, Wai-Ki
Super, Michael
Ferdinands, Jill M.
Mistry, Anushay J.
Newhams, Margaret M.
Zhang, Yu
Su, Helen C.
McLaughlin, Gwenn E.
Sapru, Anil
Loftis, Laura L.
Weiss, Scott L.
Hall, Mark W.
Cvijanovich, Natalie
Schwarz, Adam
Tarquinio, Keiko M.
Mourani, Peter M.
Randolph, Adrienne G.
author_facet Levy, Emily R.
Yip, Wai-Ki
Super, Michael
Ferdinands, Jill M.
Mistry, Anushay J.
Newhams, Margaret M.
Zhang, Yu
Su, Helen C.
McLaughlin, Gwenn E.
Sapru, Anil
Loftis, Laura L.
Weiss, Scott L.
Hall, Mark W.
Cvijanovich, Natalie
Schwarz, Adam
Tarquinio, Keiko M.
Mourani, Peter M.
Randolph, Adrienne G.
author_sort Levy, Emily R.
collection PubMed
description Background: Mannose-binding lectin (MBL) is an innate immune protein with strong biologic plausibility for protecting against influenza virus-related sepsis and bacterial co-infection. In an autopsy cohort of 105 influenza-infected young people, carriage of the deleterious MBL gene MBL2_Gly54Asp(“B”) mutation was identified in 5 of 8 individuals that died from influenza-methicillin-resistant Staphylococcus aureus (MRSA) co-infection. We evaluated MBL2 variants known to influence MBL levels with pediatric influenza-related critical illness susceptibility and/or severity including with bacterial co-infections. Methods: We enrolled children and adolescents with laboratory-confirmed influenza infection across 38 pediatric intensive care units from November 2008 to June 2016. We sequenced MBL2 “low-producer” variants rs11003125(“H/L”), rs7096206(“Y/X”), rs1800450(Gly54Asp)(“B”), rs1800451(Gly57Glu)(“C”), rs5030737(Arg52Cys)(“D”) in patients and biologic parents. We measured serum levels and compared complement activity in low-producing homozygotes (“B/B,” “C/C”) to HYA/HYA controls. We used a population control of 1,142 healthy children and also analyzed family trios (PBAT/HBAT) to evaluate disease susceptibility, and nested case-control analyses to evaluate severity. Results: We genotyped 420 patients with confirmed influenza-related sepsis: 159 (38%) had acute lung injury (ALI), 165 (39%) septic shock, and 30 (7%) died. Although bacterial co-infection was diagnosed in 133 patients (32%), only MRSA co-infection (n = 33, 8% overall) was associated with death (p < 0.0001), present in 11 of 30 children that died (37%). MBL2 variants predicted serum levels and complement activation as expected. We found no association between influenza-related critical illness susceptibility and MBL2 variants using family trios (633 biologic parents) or compared to population controls. MBL2 variants were not associated with admission illness severity, septic shock, ALI, or bacterial co-infection diagnosis. Carriage of low-MBL producing MBL2 variants was not a risk factor for mortality, but children that died did have higher carriage of one or more B alleles (OR 2.3; p = 0.007), including 7 of 11 with influenza MRSA-related death (vs. 2 of 22 survivors: OR 14.5, p = 0.0002). Conclusions: MBL2 variants that decrease MBL levels were not associated with susceptibility to pediatric influenza-related critical illness or with multiple measures of critical illness severity. We confirmed a prior report of higher B allele carriage in a relatively small number of young individuals with influenza-MRSA associated death.
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spelling pubmed-65184432019-05-28 Evaluation of Mannose Binding Lectin Gene Variants in Pediatric Influenza Virus-Related Critical Illness Levy, Emily R. Yip, Wai-Ki Super, Michael Ferdinands, Jill M. Mistry, Anushay J. Newhams, Margaret M. Zhang, Yu Su, Helen C. McLaughlin, Gwenn E. Sapru, Anil Loftis, Laura L. Weiss, Scott L. Hall, Mark W. Cvijanovich, Natalie Schwarz, Adam Tarquinio, Keiko M. Mourani, Peter M. Randolph, Adrienne G. Front Immunol Immunology Background: Mannose-binding lectin (MBL) is an innate immune protein with strong biologic plausibility for protecting against influenza virus-related sepsis and bacterial co-infection. In an autopsy cohort of 105 influenza-infected young people, carriage of the deleterious MBL gene MBL2_Gly54Asp(“B”) mutation was identified in 5 of 8 individuals that died from influenza-methicillin-resistant Staphylococcus aureus (MRSA) co-infection. We evaluated MBL2 variants known to influence MBL levels with pediatric influenza-related critical illness susceptibility and/or severity including with bacterial co-infections. Methods: We enrolled children and adolescents with laboratory-confirmed influenza infection across 38 pediatric intensive care units from November 2008 to June 2016. We sequenced MBL2 “low-producer” variants rs11003125(“H/L”), rs7096206(“Y/X”), rs1800450(Gly54Asp)(“B”), rs1800451(Gly57Glu)(“C”), rs5030737(Arg52Cys)(“D”) in patients and biologic parents. We measured serum levels and compared complement activity in low-producing homozygotes (“B/B,” “C/C”) to HYA/HYA controls. We used a population control of 1,142 healthy children and also analyzed family trios (PBAT/HBAT) to evaluate disease susceptibility, and nested case-control analyses to evaluate severity. Results: We genotyped 420 patients with confirmed influenza-related sepsis: 159 (38%) had acute lung injury (ALI), 165 (39%) septic shock, and 30 (7%) died. Although bacterial co-infection was diagnosed in 133 patients (32%), only MRSA co-infection (n = 33, 8% overall) was associated with death (p < 0.0001), present in 11 of 30 children that died (37%). MBL2 variants predicted serum levels and complement activation as expected. We found no association between influenza-related critical illness susceptibility and MBL2 variants using family trios (633 biologic parents) or compared to population controls. MBL2 variants were not associated with admission illness severity, septic shock, ALI, or bacterial co-infection diagnosis. Carriage of low-MBL producing MBL2 variants was not a risk factor for mortality, but children that died did have higher carriage of one or more B alleles (OR 2.3; p = 0.007), including 7 of 11 with influenza MRSA-related death (vs. 2 of 22 survivors: OR 14.5, p = 0.0002). Conclusions: MBL2 variants that decrease MBL levels were not associated with susceptibility to pediatric influenza-related critical illness or with multiple measures of critical illness severity. We confirmed a prior report of higher B allele carriage in a relatively small number of young individuals with influenza-MRSA associated death. Frontiers Media S.A. 2019-05-08 /pmc/articles/PMC6518443/ /pubmed/31139182 http://dx.doi.org/10.3389/fimmu.2019.01005 Text en Copyright © 2019 Levy, Yip, Super, Ferdinands, Mistry, Newhams, Zhang, Su, McLaughlin, Sapru, Loftis, Weiss, Hall, Cvijanovich, Schwarz, Tarquinio, Mourani, PALISI PICFLU Investigators and Randolph. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Levy, Emily R.
Yip, Wai-Ki
Super, Michael
Ferdinands, Jill M.
Mistry, Anushay J.
Newhams, Margaret M.
Zhang, Yu
Su, Helen C.
McLaughlin, Gwenn E.
Sapru, Anil
Loftis, Laura L.
Weiss, Scott L.
Hall, Mark W.
Cvijanovich, Natalie
Schwarz, Adam
Tarquinio, Keiko M.
Mourani, Peter M.
Randolph, Adrienne G.
Evaluation of Mannose Binding Lectin Gene Variants in Pediatric Influenza Virus-Related Critical Illness
title Evaluation of Mannose Binding Lectin Gene Variants in Pediatric Influenza Virus-Related Critical Illness
title_full Evaluation of Mannose Binding Lectin Gene Variants in Pediatric Influenza Virus-Related Critical Illness
title_fullStr Evaluation of Mannose Binding Lectin Gene Variants in Pediatric Influenza Virus-Related Critical Illness
title_full_unstemmed Evaluation of Mannose Binding Lectin Gene Variants in Pediatric Influenza Virus-Related Critical Illness
title_short Evaluation of Mannose Binding Lectin Gene Variants in Pediatric Influenza Virus-Related Critical Illness
title_sort evaluation of mannose binding lectin gene variants in pediatric influenza virus-related critical illness
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6518443/
https://www.ncbi.nlm.nih.gov/pubmed/31139182
http://dx.doi.org/10.3389/fimmu.2019.01005
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