Determinantes gen?ticos da hansen?ase em uma popula??o do Rio Grande do Norte

Ara?jo, S?rgio Ricardo Fernandes de

25 August 2008

Made available in DSpace on 2014-12-17T14:03:29Z (GMT). No. of bitstreams: 1 SergioRFA.pdf: 2472351 bytes, checksum: daab3b710d9abca3798e5b5314990137 (MD5) Previous issue date: 2008-08-25 / Coordena??o de Aperfei?oamento de Pessoal de N?vel Superior / Background: Leprosy can cause severe disability and disfigurement and is still a major health in different parts of the world. Only a subset of those individuals exposed to the pathogen will go on to develop clinical disease and there is a broad clinical spectrum amongst leprosy patients. The outcome of infection is in part due to host genes that influence control of the initial infection and the host?s immune response to that infection. Aim: Evaluate if polymorphisms type SNP in the 17q118q21 chromosomic region contribute to development of leprosy in Rio Grande do Norte population. Material and methods: A sample composed of 215 leprosy patients and 229 controls drawn from the same population were genotyped by using a Snapshot assay for eight genes (NOS2A, CCL18, CRLF3, CCL23, TNFAIP1, STAT5B, CCR7 and CSF3) located in chromosomic region 17q118q21. The genotype and allele frequency were measured and statistical analysis was performed by chi-square in SPSS version 15 and graph prism pad version 4 software. Results: Ours results indicated that the markers NOS2A8277, NOS2A8rs16949, CCR78rs11574663 and CSF38rs2227322 presented strong association with leprosy and their risk genotype were GG, TT, AA and GG respectively. The risk genotypes for all markers associated to leprosy presented recessive inheritance standard. When we compared the interaction among the markers in different combination we find that the marker NOS2A8277 associated with CCR78rs11574663 presented highest risk probability to development of leprosy. When we evaluated the haplotype of the risk markers it was found a haplotype associated with increase of the protection (CSF38rs22273228CC, CCR78 rs115746638GA, NOS2A8rs169498CT and NOS2A82778GA). The association of the clinical forms paucibacilary and multibacilary with markers showed that to the markers NOS2A8 2778GG, CCR78rs115746638AA and CSF38rs22273228GG there were a strong influence to migration to multibacilary pole and to marker NOS2A8rs169498TT the high proportion was found to the paucibacilary form. Conclusions: Changes in the genes NOS2A, CCR7 and CSF3 can influence the immune response against Mycobacterium leprae. The combination among these polymorphisms alters the risk probability to develop leprosy. The markers type SNP associated to development of the leprosy also are linked to clinical forms and its severity being the polymorphism NOS2A8rs169498TT associated with paucibacilar form and the polymorphisms NOS2A82778GG, CCR78rs115746638AA and CSF38rs22273228GG associated to multibacilar form / Introdu??o: A hansen?ase ? uma doen?a milenar que pode causar incapacidades f?sicas e desfiguramento, sendo ainda imponente em nosso pa?s, um problema de sa?de p?blica em seis pa?ses incluindo o Brasil. Apenas uma fra??o dos indiv?duos expostos ao Mycobacterium leprae desenvolve sintomas caracter?sticos da hansen?ase. Os fatores relacionados ? evolu??o da infec??o para doen?a depende em parte de caracter?sticas gen?ticas do hospedeiro que influenciam o controle da infec??o e ? progress?o da resposta imune. Objetivo: Avaliar se polimorfismos localizados na regi?o cromoss?mica 17q118q21 est?o associados ? hansen?ase numa popula??o oriunda do Rio Grande do Norte. Material e m?todos: Foram estudados 215 pacientes de hansen?ase e 229 controles sendo genotipados por Snapshot. Foram estudados varia??es em oito genes (NOS2A, CCL18, CRLF3, CCL23, TNFAIP1, STAT5B, CCR7 e CSF3) localizados na regi?o cromoss?mica 17q118q21. As freq??ncias genot?picas e al?licas foram determinadas por contagem direta e as diferen?as na distribui??o dessas entre os casos e os controles foram avaliadas por qui-quadrado usando o pacote estat?stico SPSS vers?o 15, e Graph Prism Pad vers?o 4.0. Resultados: Nossos resultados mostraram que os marcadores NOS2A8277, NOS2A8rs16949, CCR78rs11574663 e CSF38rs2227322 apresentam forte associa??o com a hansen?ase e seus gen?tipos de risco foram GG, TT, AA e GG respectivamente, apresentando todos padr?o de heran?a recessivo. O marcador NOS2A8277 e CCR78rs11574663 indicou maior probabilidade de risco no desenvolvimento a hansen?ase em (OR = 3,92, p = 0,0001). A avalia??o e hapl?tipos mostrou que CSF38rs22273228CC, CCR78rs115746638GA, NOS2A8rs169498CT e NOS2A82778GA est?o relacionados com a prote??o para o desenvolvimento da doen?a. Quando analisamos a distribui??o genot?pica dos marcadores estudados entre as formas cl?nicas paucibacilar e multibacilar, foram encontrados que os marcadores NOS2A82778 GG, CCR78rs115746638AA e CSF38rs22273228GG apresentavam uma forte associa??o com o polo multibacilar enquanto que o marcador NOS2A8rs169498TT foi associado a forma paucibacilar. Conclus?es: Os genes NOS2A, CCR7 e CSF3 possuiram grande import?ncia na resposta imune contra o Mycobacterium leprae e que modifica??es na seq??ncia nucleot?dica desses genes alteram a forma como agem no controle e desenvolvimento da hansen?ase. Os polimorfismos nesses genes possuem uma maior probabilidade de risco quando analisados combinados. A maior susceptibilidade induzida pelos polimorfismos nesses genes est? ligada a forma como evolui a doen?a sendo alguns deles associados a uma doen?a mais severa e outros a forma mais branda. Estes dados validam que o agregado de genes presentes no cromossomo 17 que expressam mol?culas importantes para manuten??o do equil?brio imune e que contribuem de forma intensa para a prote??o contra microorganismos intracelulares como o Mycobacterium leprae podem ter suas fun??es comprometidas por altera??o de suas seq??ncias nucleot?dicas

Polimorfismos

Hansen?ase

SNP

Susceptibilidade gen?tica

Polymorphisms

Genetic

Susceptibility

Leprosy

SNP

CNPQ::CIENCIAS BIOLOGICAS::BIOQUIMICA

Estudo dos genes do complexo do ant?geno leucocit?rio humano (hla) associados ? susceptibilidade ao diabetes mellitus tipo 1

Silva, Heglayne Pereira Vital da

27 March 2013

Made available in DSpace on 2014-12-17T14:16:34Z (GMT). No. of bitstreams: 1 HeglaynePVS_DISSERT.pdf: 2645894 bytes, checksum: da2c7ec39b2e87b75a199511857a4e83 (MD5) Previous issue date: 2013-03-27 / Conselho Nacional de Desenvolvimento Cient?fico e Tecnol?gico / Of all of the genes associated with the development of Diabetes mellitus type 1 (T1D), the largest contribution comes from the genes in the Human Leukocyte Antigen (HLA) region, mostly the class II DR e DQ genes. Specific combinations of alleles DRB1, DQA1 and DQB1 constituting haplotypes, and further, a combination of more than one haplotype, providing multilocus genotypes are associated with susceptibility, protection and neutrality to DM1. Thus, the aim of present study was to verified the association of polymorphisms of HLA genes class II with susceptibility to type 1 diabetes mellitus (T1D). Ninety-two patients with T1D and 100 individuals normoglycemics (NG) aged between 6 and 20 years were studied. Genomic DNA was obtained from peripheral whole blood, collected in EDTA tube, using the extraction kit Illustra Triple Prep?, GE Healthcare. For HLA typing was used DNA LABType system by One Lambda kit applying Luminex? technology to the method of PCRSSO typing reverse. The alleles DRB1*03:01, *04:05, *04:01, *04:02, DQA1*03:01g, *05:01g, DQB1*02:01g, *03:02, the haplotypes DRB1*03:01-DQA1*05:01-DQB1*02:01, DRB1*04:05-DQA1*03:01g-DQB1*03:02, DRB1*04:02-DQA1*03:01g-DQB1*03:02, DRB1*04:01-DQA1*03:01g-DQB1*03:02 and DR3-DQ2/DR4-DQ8 genotype were significantly associated with the chance of developing T1D. The alleles DRB1*11:01, *15:03, *15:01, *13:01, DQA1*01:02, *04:01g, *01:03, DQB1*06:02, *03:01g, *06:03, *04:02, the haplotypes DRB1*11:01-DQA1*05:01-DQB1*03:01, DRB1*13:01-DQA1*01:03-DQB1*06:03 and DRX-DQX/DRX-DQX genotype, formed by other than the DR3-DQ2 or DR4-DQ8 haplotypes, were significantly associated with T1D protection Despite the major racial Brazilian, even at the regional level, these results are similar to the majority of alleles, genotypes and haplotypes of HLA class II-related susceptibility or resistance to T1D, extensively described in the literature for Caucasian population. Children with age at diagnosis less than 5 years of age had significantly higher frequency of the heterozygous genotype DR3-DQ2/DR4-DQ8 compared to children with age at diagnosis than 5 years old. These results also demonstrate strong association of the genetic profile of the class II HLA for this age group, possibly associated with the severity and rapid progression to the onset of T1D. The knowledge of HLA class II genes may be useful in genetic screens that allow the prediction of T1D / De todos os genes j? relacionados com o desenvolvimento do Diabetes mellitus tipo 1 (DM1), a maior contribui??o vem da regi?o do genoma onde est?o localizados os genes do Ant?geno Leucocit?rio Humano (HLA), sobretudo os genes da classe II do HLA: DR e DQ. Espec?ficas combina??es de alelos DRB1, DQA1 e DQB1 formando hapl?tipos, e ainda, a combina??o de mais de um hapl?tipo, formando gen?tipos multilocus s?o associados com a susceptibilidade, neutralidade e prote??o ao DM1. Dessa forma, o objetivo do estudo foi verificar a associa??o dos polimorfismos dos genes do complexo HLA classe II com a susceptibilidade ao DM1, em pacientes do Rio Grande do Norte. Foram estudados 92 indiv?duos com DM1 e 100 indiv?duos normoglic?micos (NG), com idade entre 6 e 20 anos. O DNA gen?mico foi obtido a partir do sangue total perif?rico, coletado em tubo com EDTA, utilizando o kit de extra??o Illustra Triple Prep?, GE Healthcare. Para a tipagem do HLA foi utilizado o sistema DNA LABType atrav?s de kits One Lambda, que aplica a tecnologia Luminex? ao m?todo de tipagem por PCR-SSO reverso. Os alelos DRB1*03:01, *04:05, *04:01, *04:02; DQA1*03:01g, 05:01g; DQB1*02:01g, *03:02; os hapl?tipos DRB1*03:01-DQA1*05:01-DQB1*02:01, DRB1*04:05-DQA1*03:01g- DQB1*03:02, DRB1*04:02-DQA1*03:01g-DQB1*03:02, DRB1*04:01-DQA1*03:01g- DQB1*03:02 e o gen?tipo heterozigoto, DR3-DQ2/DR4-DQ8 foram significativamente associados com a chance de desenvolvimento do DM1. J? os alelos DRB1*11:01, *15:03, *15:01, *13:01; DQA1*01:02, *04:01g, *01:03; DQB1*06:02, *03:01g, *06:03, *04:02; os hapl?tipos DRB1*11:01-DQA1*05:01-DQB1*03:01, DRB1*13:01-DQA1*01:03-DQB1*06:03 e o gen?tipo DRX-DQX/DRX-DQX, formado por outros hapl?tipos que n?o DR3-DQ2 ou DR4-DQ8, foram significativamente associados a prote??o ao DM1. Apesar da grande miscigena??o racial brasileira, at? em n?vel regional, estes resultados s?o semelhantes a maioria dos alelos, hapl?tipos e gen?tipos de HLA classe II relacionados ? susceptibilidade ou prote??o ao DM1, extensivamente descritos na literatura para a popula??o caucasiana. Crian?as com idade ao diagn?stico inferior a 5 anos de idade apresentaram significativamente maior frequ?ncia do gen?tipo heterozigoto DR3-DQ2/DR4-DQ8, quando comparada ?s crian?as com idade ao diagn?stico superior a 5 anos de idade. Esses resultados demonstram tamb?m forte envolvimento do perfil gen?tico da classe II do HLA para esta faixa et?ria, que estaria relacionada possivelmente com a gravidade e a r?pida progress?o para o in?cio do DM1. O conhecimento dos genes HLA de classe II pode ser ?til em triagens gen?ticas que possibilitem a predi??o do DM1

CNPQ::CIENCIAS BIOLOGICAS::FARMACOLOGIA