Association and linkage of leprosy phenotypes with HLA class II and tumour necrosis factor genes

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2001xmlui.dri2xhtml.METS-1.0.item-files-viewOpen
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http://patua.iec.gov.br/handle/iec/1046xmlui.dri2xhtml.METS-1.0.item-author
Shaw, M. A
Donaldson, I. J
Collins, A
Peacock, C. S
Lins-Lainson, Zéa Constante
Shaw, Jeffrey Jon
Ramos, Francisco Lúzio de Paula
Silveira, Fernando Tobias
Blackwell, J. M
xmlui.dri2xhtml.METS-1.0.item-abstract
Previous analyses indicate major gene control of susceptibility to leprosy per se and the HLA class II region has been
implicated in determining susceptibility and control of clinical phenotype. Segregation analysis using data from 76 Brazilian
leprosy multi-case pedigrees (1166 individuals) supported a two locus model as the best fit: a recessive major gene and a
recessive modifier gene(s) (single locus vs two locus model, P = 0.0007). Combined segregation and linkage analysis to
the major locus, showed strong linkage to HLA class II (HLA-DQB1 P = 0.000002, HLA-DQA1 P = 0.000002, HLA-DRB1
P = 0.0000003) and tumour necrosis factor genes (TNF P = 0.00002, LTA P = 0.003). Extended transmission disequilibrium
testing, using multiple affected family members, demonstrated that the common allele TNF*1 of the −308 promoter region
polymorphism showed linkage and/or association with disease per se, at a high level of significance (P , 0.0001). Two
locus transmission disequilibrium testing suggested susceptibility (TNF*1/LTA*2) and protective (TNF*2/LTA*2) haplotypes
in the class III region. Taken together the segregation and HLA analyses suggest the possibility of more than one
susceptibility locus in the MHC
xmlui.dri2xhtml.METS-1.0.item-citation
SHAW, M. A. et al. Association and linkage of leprosy phenotypes with HLA class II and tumour necrosis factor genes. Genes and Immunity, v. 2, n. 4 , p. 196-204, 2001xmlui.dri2xhtml.METS-1.0.item-decsPrimary
Hanseníase / genéticaPredisposição Genética para Doença
Ligação Genética
Genes Classe II do Complexo de Histocompatibilidade (MHC)
Receptores do Fator de Necrose Tumoral
Polimorfismo Genético