CCR5 genotypes and progression to HIV disease in perinatally infected children
Autor: | Wilton S. Freire, Regina Célia de Menezes Succi, Daisy Maria Machado, Daniela Souza Araújo de Angelis, Cláudio Sérgio Pannuti |
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Jazyk: | angličtina |
Rok vydání: | 2007 |
Předmět: |
Microbiology (medical)
Male Heterozygote Adolescent Genotype Receptors CCR5 viruses Population CCR5 co-receptor lcsh:QR1-502 HIV Infections Biology Polymerase Chain Reaction lcsh:Microbiology law.invention lcsh:Infectious and parasitic diseases Pathogenesis Gene Frequency law Humans lcsh:RC109-216 Allele education Child Allele frequency Polymerase chain reaction Electrophoresis Agar Gel education.field_of_study Homozygote Wild type virus diseases Heterozygote advantage Virology Infectious Diseases Child Preschool Immunology Mutation Disease Progression HIV-1 HIV disease progression Female perinatally infected children |
Zdroj: | Brazilian Journal of Infectious Diseases, Volume: 11, Issue: 2, Pages: 196-198, Published: APR 2007 Brazilian Journal of Infectious Diseases v.11 n.2 2007 Brazilian Journal of Infectious Diseases Brazilian Society of Infectious Diseases (BSID) instacron:BSID Brazilian Journal of Infectious Diseases, Vol 11, Iss 2, Pp 196-198 |
Popis: | The CCR5 molecule, a chemokine receptor, is the most important co-receptor for macrophage-tropic HIV-1. A 32-bp deletion in the gene encoding CCR5 (CCR5-del32) confers nearly complete resistance to HIV-1 infection in homozygotes, and slows the rate of progression to AIDS in heterozygous adults. The aim of this study was to describe the CCR5 genotypes and the characteristics of HIV disease progression in perinatally infected children. From a total of 51 children analyzed for the CCR5-del32 mutation, 18 (35%) were considered to be rapid progressors, 28 (55%) were moderate progressors and 5 (10%) were slow progressors. A portion of the CCR5 gene was amplified by PCR from genomic DNA followed by agarose gel electrophoresis. Forty-nine children (96%) carried the homozygous wild type genotype for CCR5 while 2 (4%) carried the heterozygous wt/del32 genotype. In the population studied, the CCR5 genotype was unable to account for the differences in pattern of the disease progression among the three groups (rapid, moderate and slow progressors), and the allele frequency of CCR5-del32 was too low to allow statistical comparisons with adequate resolving power. Studies on larger populations may help to further elucidate the role of this allele and other host factors in the regulation of HIV-1 pathogenesis in children. |
Databáze: | OpenAIRE |
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