Candidate Human Genetic Polymorphisms and Severe Malaria in a Tanzanian Population

Human genetic background strongly influences susceptibility to malaria infection and progression to severe disease and death. Classical genetic studies identified haemoglobinopathies and erythrocyte-associated polymorphisms, as protective against severe disease. High throughput genotyping by mass sp...

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Autores principales: Manjurano, Alphaxard, Clark, Taane G., Nadjm, Behzad, Mtove, George, Wangai, Hannah, Sepulveda, Nuno, Campino, Susana G., Maxwell, Caroline, Olomi, Raimos, Rockett, Kirk R., Jeffreys, Anna, Riley, Eleanor M., Reyburn, Hugh, Drakeley, Christopher
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3483265/
https://www.ncbi.nlm.nih.gov/pubmed/23144702
http://dx.doi.org/10.1371/journal.pone.0047463
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author Manjurano, Alphaxard
Clark, Taane G.
Nadjm, Behzad
Mtove, George
Wangai, Hannah
Sepulveda, Nuno
Campino, Susana G.
Maxwell, Caroline
Olomi, Raimos
Rockett, Kirk R.
Jeffreys, Anna
Riley, Eleanor M.
Reyburn, Hugh
Drakeley, Christopher
author_facet Manjurano, Alphaxard
Clark, Taane G.
Nadjm, Behzad
Mtove, George
Wangai, Hannah
Sepulveda, Nuno
Campino, Susana G.
Maxwell, Caroline
Olomi, Raimos
Rockett, Kirk R.
Jeffreys, Anna
Riley, Eleanor M.
Reyburn, Hugh
Drakeley, Christopher
author_sort Manjurano, Alphaxard
collection PubMed
description Human genetic background strongly influences susceptibility to malaria infection and progression to severe disease and death. Classical genetic studies identified haemoglobinopathies and erythrocyte-associated polymorphisms, as protective against severe disease. High throughput genotyping by mass spectrometry allows multiple single nucleotide polymorphisms (SNPs) to be examined simultaneously. We compared the prevalence of 65 human SNP's, previously associated with altered risk of malaria, between Tanzanian children with and without severe malaria. Five hundred children, aged 1–10 years, with severe malaria were recruited from those admitted to hospital in Muheza, Tanzania and compared with matched controls. Genotyping was performed by Sequenom MassArray, and conventional PCR was used to detect deletions in the alpha-thalassaemia gene. SNPs in two X-linked genes were associated with altered risk of severe malaria in females but not in males: heterozygosity for one or other of two SNPs in the G6PD gene was associated with protection from all forms of severe disease whilst two SNPs in the gene encoding CD40L were associated with respiratory distress. A SNP in the adenyl cyclase 9 (ADCY9) gene was associated with protection from acidosis whilst a polymorphism in the IL-1α gene (IL1A) was associated with an increased risk of acidosis. SNPs in the genes encoding IL-13 and reticulon-3 (RTN3) were associated with increased risk of cerebral malaria. This study confirms previously known genetic associations with protection from severe malaria (HbS, G6PD). It identifies two X-linked genes associated with altered risk of severe malaria in females, identifies mutations in ADCY9, IL1A and CD40L as being associated with altered risk of severe respiratory distress and acidosis, both of which are characterised by high serum lactate levels, and also identifies novel genetic associations with severe malaria (TRIM5) and cerebral malaria(IL-13 and RTN3). Further studies are required to test the generality of these associations and to understand their functional consequences.
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spelling pubmed-34832652012-11-09 Candidate Human Genetic Polymorphisms and Severe Malaria in a Tanzanian Population Manjurano, Alphaxard Clark, Taane G. Nadjm, Behzad Mtove, George Wangai, Hannah Sepulveda, Nuno Campino, Susana G. Maxwell, Caroline Olomi, Raimos Rockett, Kirk R. Jeffreys, Anna Riley, Eleanor M. Reyburn, Hugh Drakeley, Christopher PLoS One Research Article Human genetic background strongly influences susceptibility to malaria infection and progression to severe disease and death. Classical genetic studies identified haemoglobinopathies and erythrocyte-associated polymorphisms, as protective against severe disease. High throughput genotyping by mass spectrometry allows multiple single nucleotide polymorphisms (SNPs) to be examined simultaneously. We compared the prevalence of 65 human SNP's, previously associated with altered risk of malaria, between Tanzanian children with and without severe malaria. Five hundred children, aged 1–10 years, with severe malaria were recruited from those admitted to hospital in Muheza, Tanzania and compared with matched controls. Genotyping was performed by Sequenom MassArray, and conventional PCR was used to detect deletions in the alpha-thalassaemia gene. SNPs in two X-linked genes were associated with altered risk of severe malaria in females but not in males: heterozygosity for one or other of two SNPs in the G6PD gene was associated with protection from all forms of severe disease whilst two SNPs in the gene encoding CD40L were associated with respiratory distress. A SNP in the adenyl cyclase 9 (ADCY9) gene was associated with protection from acidosis whilst a polymorphism in the IL-1α gene (IL1A) was associated with an increased risk of acidosis. SNPs in the genes encoding IL-13 and reticulon-3 (RTN3) were associated with increased risk of cerebral malaria. This study confirms previously known genetic associations with protection from severe malaria (HbS, G6PD). It identifies two X-linked genes associated with altered risk of severe malaria in females, identifies mutations in ADCY9, IL1A and CD40L as being associated with altered risk of severe respiratory distress and acidosis, both of which are characterised by high serum lactate levels, and also identifies novel genetic associations with severe malaria (TRIM5) and cerebral malaria(IL-13 and RTN3). Further studies are required to test the generality of these associations and to understand their functional consequences. Public Library of Science 2012-10-29 /pmc/articles/PMC3483265/ /pubmed/23144702 http://dx.doi.org/10.1371/journal.pone.0047463 Text en © 2012 Manjurano et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Manjurano, Alphaxard
Clark, Taane G.
Nadjm, Behzad
Mtove, George
Wangai, Hannah
Sepulveda, Nuno
Campino, Susana G.
Maxwell, Caroline
Olomi, Raimos
Rockett, Kirk R.
Jeffreys, Anna
Riley, Eleanor M.
Reyburn, Hugh
Drakeley, Christopher
Candidate Human Genetic Polymorphisms and Severe Malaria in a Tanzanian Population
title Candidate Human Genetic Polymorphisms and Severe Malaria in a Tanzanian Population
title_full Candidate Human Genetic Polymorphisms and Severe Malaria in a Tanzanian Population
title_fullStr Candidate Human Genetic Polymorphisms and Severe Malaria in a Tanzanian Population
title_full_unstemmed Candidate Human Genetic Polymorphisms and Severe Malaria in a Tanzanian Population
title_short Candidate Human Genetic Polymorphisms and Severe Malaria in a Tanzanian Population
title_sort candidate human genetic polymorphisms and severe malaria in a tanzanian population
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3483265/
https://www.ncbi.nlm.nih.gov/pubmed/23144702
http://dx.doi.org/10.1371/journal.pone.0047463
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