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Pathogen-specific epitopes as epidemiological tools for defining the magnitude of Mycobacterium leprae transmission in areas endemic for leprosy
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نویسنده
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martins m.v.s.b. ,guimarães m.m.s. ,spencer j.s. ,hacker m.a.v.b. ,costa l.s. ,carvalho f.m. ,geluk a. ,van der ploeg-van schip j.j. ,pontes m.a.a. ,gonçalves h.s. ,de morais j.p. ,bandeira t.j.p.g. ,pessolani m.c.v. ,brennan p.j. ,pereira g.m.b.
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منبع
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plos neglected tropical diseases - 2012 - دوره : 6 - شماره : 4
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چکیده
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During recent years,comparative genomic analysis has allowed the identification of mycobacterium leprae-specific genes with potential application for the diagnosis of leprosy. in a previous study,58 synthetic peptides derived from these sequences were tested for their ability to induce production of ifn-γ in pbmc from endemic controls (ec) with unknown exposure to m. leprae,household contacts of leprosy patients and patients,indicating the potential of these synthetic peptides for the diagnosis of sub- or preclinical forms of leprosy. in the present study,the patterns of ifn-γ release of the individuals exposed or non-exposed to m. leprae were compared using an artificial neural network algorithm,and the most promising m. leprae peptides for the identification of exposed people were selected. this subset of m. leprae-specific peptides allowed the differentiation of groups of individuals from sites hyperendemic for leprosy versus those from areas with lower level detection rates. a progressive reduction in the ifn-γ levels in response to the peptides was seen when contacts of multibacillary (mb) patients were compared to other less exposed groups,suggesting a down modulation of ifn-γ production with an increase in bacillary load or exposure to m. leprae. the data generated indicate that an ifn-γ assay based on these peptides applied individually or as a pool can be used as a new tool for predicting the magnitude of m. leprae transmission in a given population. © 2012 martins et al.
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آدرس
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laboratory of cellular microbiology,oswaldo cruz institute,fiocruz,rio de janeiro, Brazil, laboratory of cellular microbiology,oswaldo cruz institute,fiocruz,rio de janeiro, Brazil, department of microbiology,immunology and pathology,colorado state university,fort collins,co, United States, leprosy laboratory,oswaldo cruz institute,fiocruz,rio de janeiro, Brazil, laboratory of medical informatics,school of medical sciences,state university of rio de janeiro,rio de janeiro, Brazil, laboratory of cellular microbiology,oswaldo cruz institute,fiocruz,rio de janeiro, Brazil, department of infectious diseases,leiden university medical center,leiden, Netherlands, department of infectious diseases,leiden university medical center,leiden, Netherlands, dona libânia reference center,fortaleza, Brazil, dona libânia reference center,fortaleza, Brazil, leprosy control program/ser v/fortaleza,fortaleza, Brazil, labpasteur diagnostic medicine/diagnostics of america (dasa),fortaleza, Brazil, laboratory of cellular microbiology,oswaldo cruz institute,fiocruz,rio de janeiro, Brazil, department of microbiology,immunology and pathology,colorado state university,fort collins,co, United States, laboratory of cellular microbiology,oswaldo cruz institute,fiocruz,rio de janeiro,brazil,laboratory of immunopathology,school of medical sciences,state university of rio de janeiro,rio de janeiro, Brazil
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Authors
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