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HMOX1 gene promoter alleles and high HO-1 levels are associated with severe malaria in Gambian children
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نویسنده
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walther m. ,de caul a. ,aka p. ,njie m. ,amambua-ngwa a. ,walther b. ,predazzi i.m. ,cunnington a. ,deininger s. ,takem e.n. ,ebonyi a. ,weis s. ,walton r. ,rowland-jones s. ,sirugo g. ,williams s.m. ,conway d.j.
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منبع
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plos pathogens - 2012 - دوره : 8 - شماره : 3
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چکیده
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Heme oxygenase 1 (ho-1) is an essential enzyme induced by heme and multiple stimuli associated with critical illness. in humans,polymorphisms in the hmox1 gene promoter may influence the magnitude of ho-1 expression. in many diseases including murine malaria,ho-1 induction produces protective anti-inflammatory effects,but observations from patients suggest these may be limited to a narrow range of ho-1 induction,prompting us to investigate the role of ho-1 in malaria infection. in 307 gambian children with either severe or uncomplicated p. falciparum malaria,we characterized the associations of hmox1 promoter polymorphisms,hmox1 mrna inducibility,ho-1 protein levels in leucocytes (flow cytometry),and plasma (elisa) with disease severity. the (gt)n repeat polymorphism in the hmox1 promoter was associated with hmox1 mrna expression in white blood cells in vitro,and with severe disease and death,while high ho-1 levels were associated with severe disease. neutrophils were the main ho-1-expressing cells in peripheral blood,and hmox1 mrna expression was upregulated by heme-moieties of lysed erythrocytes. we provide mechanistic evidence that induction of hmox1 expression in neutrophils potentiates the respiratory burst,and propose this may be part of the causal pathway explaining the association between short (gt)n repeats and increased disease severity in malaria and other critical illnesses. our findings suggest a genetic predisposition to higher levels of ho-1 is associated with severe illness,and enhances the neutrophil burst leading to oxidative damage of endothelial cells. these add important information to the discussion about possible therapeutic manipulation of ho-1 in critically ill patients.
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آدرس
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medical research council laboratories,fajara,banjul,gambia,national institute of allergy and infectious diseases,national institutes of health,rockville,md, United States, medical research council laboratories,fajara,banjul, Gambia, medical research council laboratories,fajara,banjul, Gambia, medical research council laboratories,fajara,banjul, Gambia, medical research council laboratories,fajara,banjul, Gambia, medical research council laboratories,fajara,banjul, Gambia, vanderbilt medical center,division of human genomics and center for human genetics research,nashville,tn, United States, medical research council laboratories,fajara,banjul,gambia,department of immunology and infection,faculty of infectious and tropical diseases,london school of hygiene and tropical medicine,london, United Kingdom, medical research council laboratories,fajara,banjul,gambia,institute of medical microbiology,immunology and parasitology,university clinic bonn,bonn, Germany, medical research council laboratories,fajara,banjul, Gambia, medical research council laboratories,fajara,banjul, Gambia, department of internal medicine,neurology and dermatology,university of leipzig,leipzig, Germany, medical research council laboratories,fajara,banjul,gambia,institute of health sciences education,barts and the london school of medicine and dentistry,queen mary university,london, United Kingdom, medical research council laboratories,fajara,banjul,gambia,weatherall institute of molecular medicine,john radcliffe hospital,oxford, United Kingdom, centro di genetica,centro di ricerca scientifica,ospedale san pietro fbf,rome, Italy, vanderbilt medical center,division of human genomics and center for human genetics research,nashville,tn, United States, medical research council laboratories,fajara,banjul,gambia,department of immunology and infection,faculty of infectious and tropical diseases,london school of hygiene and tropical medicine,london, United Kingdom
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Authors
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