The tumor necrosis factor polymorphism TNF (-308) is associated with susceptibility to meningococcal sepsis, but not with lethality
The tumor necrosis factor polymorphism TNF (-308) is associated with susceptibility to meningococcal sepsis, but not with lethality
OBJECTIVE: To determine whether the promoter polymorphism tumor necrosis factor (TNF) (-308) is associated with susceptibility to or death from meningococcal sepsis. DESIGN, SETTING, PATIENTS, AND PARTICIPANTS: Association study involving 1321 patients with microbiologically proven invasive meningococcal disease presenting to hospitals throughout United Kingdom during 1998-2001, among whom 134 died. Controls were derived from 1280 northern English blood donors.
MEASUREMENTS: DNA from patients and controls was genotyped at TNF (-308). After analysis, DNA was subsequently genotyped at eight other markers in strong linkage disequilibrium with TNF (-308); these markers were IkappaBL (-62), BAT3, LST1, NOTCH4 (+1297), NOTCH4 (+3061), CCHCR1 (+436), CCHCR1 (+2271), and LTalpha. To confirm functional relevance of TNF (-308) in the context of meningococcal disease, TNF secretion by, and TNF messenger RNA expression of macrophages derived from volunteers with known TNF (-308) genotype after exposure to Neisseria meningitidis were measured.
MAIN RESULTS: Among cases of meningococcal disease, likelihood of death was shown to be influenced by the age of the affected individual and also with the infecting serogroup, but was not influenced by genotype at TNF (-308) or the other linked markers. However, patients with meningococcal disease, irrespective of whether they died, were more likely to be homozygous for the rare allele at TNF (-308) (odds ratio = 1.93, 95% confidence interval 1.08-3.46), and less likely to be heterozygous for this marker (odds ratio = 0.79, 95% confidence interval 0.64-0.97), compared with the control cohort. There was no association of susceptibility to disease with the other markers studied. Macrophages derived from volunteers homozygous for the rare allele at TNF (-308) expressed higher levels of TNF messenger RNA and secreted higher concentrations of TNF compared with common homozygotes after exposure to N. meningitidis.
CONCLUSIONS: Genotype at TNF (-308) modifies cellular TNF secretion in response to N. meningitidis and may influence susceptibility to meningococcal disease, but does not influence the likelihood of death after infection.
Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Female, Genetic Predisposition to Disease, Genotype, Humans, Infant, Male, Meningococcal Infections, Middle Aged, Polymorphism, Genetic, Sepsis, Tumor Necrosis Factor-alpha, Young Adult, Journal Article, Research Support, Non-U.S. Gov't
1237-1243
Read, Robert C.
b5caca7b-0063-438a-b703-7ecbb6fc2b51
Teare, Dawn M.
a1107526-ed90-40bf-b11c-010260bef7cb
Pridmore, Alison C.
b704c202-afcc-4fde-9169-48e51f9fa0b0
Naylor, Simone C.
d0233f03-8cc1-445d-ad95-9d4bacb16f6c
Timms, James M.
4c480af8-7dd7-404f-b051-edf13b64f112
Kaczmarski, Edward B.
b64d93b8-aaee-44f6-a7a3-715f8971d3b3
Borrow, Raymond
dd28679e-2072-4639-9d68-851ada2eeea3
Wilson, Anthony G.
64a82514-8d20-40b5-ac71-56a26751a714
April 2009
Read, Robert C.
b5caca7b-0063-438a-b703-7ecbb6fc2b51
Teare, Dawn M.
a1107526-ed90-40bf-b11c-010260bef7cb
Pridmore, Alison C.
b704c202-afcc-4fde-9169-48e51f9fa0b0
Naylor, Simone C.
d0233f03-8cc1-445d-ad95-9d4bacb16f6c
Timms, James M.
4c480af8-7dd7-404f-b051-edf13b64f112
Kaczmarski, Edward B.
b64d93b8-aaee-44f6-a7a3-715f8971d3b3
Borrow, Raymond
dd28679e-2072-4639-9d68-851ada2eeea3
Wilson, Anthony G.
64a82514-8d20-40b5-ac71-56a26751a714
Read, Robert C., Teare, Dawn M., Pridmore, Alison C., Naylor, Simone C., Timms, James M., Kaczmarski, Edward B., Borrow, Raymond and Wilson, Anthony G.
(2009)
The tumor necrosis factor polymorphism TNF (-308) is associated with susceptibility to meningococcal sepsis, but not with lethality.
Critical Care Medicine, 37 (4), .
(doi:10.1097/CCM.0b013e31819c39bc).
(PMID:19318832)
Abstract
OBJECTIVE: To determine whether the promoter polymorphism tumor necrosis factor (TNF) (-308) is associated with susceptibility to or death from meningococcal sepsis. DESIGN, SETTING, PATIENTS, AND PARTICIPANTS: Association study involving 1321 patients with microbiologically proven invasive meningococcal disease presenting to hospitals throughout United Kingdom during 1998-2001, among whom 134 died. Controls were derived from 1280 northern English blood donors.
MEASUREMENTS: DNA from patients and controls was genotyped at TNF (-308). After analysis, DNA was subsequently genotyped at eight other markers in strong linkage disequilibrium with TNF (-308); these markers were IkappaBL (-62), BAT3, LST1, NOTCH4 (+1297), NOTCH4 (+3061), CCHCR1 (+436), CCHCR1 (+2271), and LTalpha. To confirm functional relevance of TNF (-308) in the context of meningococcal disease, TNF secretion by, and TNF messenger RNA expression of macrophages derived from volunteers with known TNF (-308) genotype after exposure to Neisseria meningitidis were measured.
MAIN RESULTS: Among cases of meningococcal disease, likelihood of death was shown to be influenced by the age of the affected individual and also with the infecting serogroup, but was not influenced by genotype at TNF (-308) or the other linked markers. However, patients with meningococcal disease, irrespective of whether they died, were more likely to be homozygous for the rare allele at TNF (-308) (odds ratio = 1.93, 95% confidence interval 1.08-3.46), and less likely to be heterozygous for this marker (odds ratio = 0.79, 95% confidence interval 0.64-0.97), compared with the control cohort. There was no association of susceptibility to disease with the other markers studied. Macrophages derived from volunteers homozygous for the rare allele at TNF (-308) expressed higher levels of TNF messenger RNA and secreted higher concentrations of TNF compared with common homozygotes after exposure to N. meningitidis.
CONCLUSIONS: Genotype at TNF (-308) modifies cellular TNF secretion in response to N. meningitidis and may influence susceptibility to meningococcal disease, but does not influence the likelihood of death after infection.
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Published date: April 2009
Keywords:
Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Female, Genetic Predisposition to Disease, Genotype, Humans, Infant, Male, Meningococcal Infections, Middle Aged, Polymorphism, Genetic, Sepsis, Tumor Necrosis Factor-alpha, Young Adult, Journal Article, Research Support, Non-U.S. Gov't
Organisations:
Clinical & Experimental Sciences
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Local EPrints ID: 346813
URI: http://eprints.soton.ac.uk/id/eprint/346813
ISSN: 0090-3493
PURE UUID: 75889af7-b562-4cc0-8a20-80af3646a6ca
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Date deposited: 10 Jan 2013 14:48
Last modified: 15 Mar 2024 03:42
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Author:
Dawn M. Teare
Author:
Alison C. Pridmore
Author:
Simone C. Naylor
Author:
James M. Timms
Author:
Edward B. Kaczmarski
Author:
Raymond Borrow
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