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MOLECULAR CHARACTERIZATION OF HLA CLASS-II GENES IN CELIAC-DISEASE PATIENTS OF LATIN-AMERICAN CAUCASIAN ORIGIN

被引:22
作者
HERRERA, M
THEILER, G
AUGUSTOVSKI, F
CHERTKOFF, L
FAINBOIM, L
DEROSA, S
COWAN, EP
SATZ, ML
机构
[1] UNIV BUENOS AIRES,HOSP CLIN,FAC MED,INMUNOGENET LAB,BUENOS AIRES,ARGENTINA
[2] UNIV BUENOS AIRES,FAC MED,DEPT MICROBIOL,BUENOS AIRES,ARGENTINA
[3] HOSP NACL PEDIAT JP GARRAHAM,GASTROENTEROL SERV,BUENOS AIRES,DF,ARGENTINA
[4] NINCDS,NEUROIMMUNOL BRANCH,BETHESDA,MD 20892
来源
TISSUE ANTIGENS | 1994年 / 43卷 / 02期
关键词
HLA CLASS II GENES; CELIAC DISEASE;
D O I
10.1111/j.1399-0039.1994.tb02305.x
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
In the present study, the polymorphic domain of HLA class II genes present in a pediatric population of Argentinian celiac disease patients was analyzed by hybridization to sequence-specific oligonucleotides and DNA sequencing. Sixteen out of 16 DR5/7 heterozygous patients bore the DQA1*0501 and DQB1*0201 alleles implicated in the DQ2 risk specificity. The second exon of DQA1, DQB1 and DRB1 genes from 2 DR5/7 patients was characterized by DNA sequencing. The following alleles were found in both patients: DRB1*1101 and DRB1*0701; DQB1*0301 and DQB1*0201; DQA1*0501 and DQA1*0201. Previous serological analysis in this population had shown the presence of DQ2 in 95% of the patients (40% in controls) and a negative association with DQ1 haplotypes, suggesting the presence of other ''permissive'' or neutral alleles. The following HLA-DQB1 alleles, besides DQB1*0201, were identified in 31 CD patients: DQB1*0301, 0302, 0401 and 0402. All these alleles share a common pattern of residues between positions 84 and 90, and distinct from that present in DQ1-related alleles.
引用
收藏
页码:83 / 87
页数:5
相关论文
共 33 条
[1]   A FAMILY STUDY CONFIRMS THAT THE HLA-DP ASSOCIATIONS WITH CELIAC-DISEASE ARE THE RESULT OF AN EXTENDED HLA-DR3 HAPLOTYPE [J].
BOLSOVER, WJ ;
HALL, MA ;
VAUGHAN, RW ;
WELSH, KI ;
CICLITIRA, PJ .
HUMAN IMMUNOLOGY, 1991, 31 (02) :100-108
[2]   3-DIMENSIONAL STRUCTURE OF THE HUMAN CLASS-II HISTOCOMPATIBILITY ANTIGEN HLA-DR1 [J].
BROWN, JH ;
JARDETZKY, TS ;
GORGA, JC ;
STERN, LJ ;
URBAN, RG ;
STROMINGER, JL ;
WILEY, DC .
NATURE, 1993, 364 (6432) :33-39
[3]   A COMBINATION OF A PARTICULAR HLA-DP-BETA ALLELE AND AN HLA-DQ HETERODIMER CONFERS SUSCEPTIBILITY TO CELIAC-DISEASE [J].
BUGAWAN, TL ;
ANGELINI, G ;
LARRICK, J ;
AURICCHIO, S ;
FERRARA, GB ;
ERLICH, HA .
NATURE, 1989, 339 (6224) :470-473
[4]   REASSESSMENT OF HLA ASSOCIATION WITH CELIAC-DISEASE IN SPECIAL REFERENCE TO THE DP ASSOCIATION [J].
COLONNA, M ;
MANTOVANI, W ;
CORAZZA, GR ;
BARBONI, P ;
GASBARRINI, G ;
FERRARA, GB ;
TOSI, R ;
TANIGAKI, N .
HUMAN IMMUNOLOGY, 1990, 29 (04) :263-274
[5]   HLA-DR AND HLA-DQ ALLELIC SEQUENCES IN MULTIPLE-SCLEROSIS PATIENTS ARE IDENTICAL TO THOSE FOUND IN THE GENERAL-POPULATION [J].
COWAN, EP ;
PIERCE, ML ;
MCFARLAND, HF ;
MCFARLIN, DE .
HUMAN IMMUNOLOGY, 1991, 32 (03) :203-210
[6]  
DEMARCHI M, 1984, HISTOCOMPATIBILITY T
[7]   ALLELES AT 4 HLA CLASS-II LOCI DETERMINED BY OLIGONUCLEOTIDE HYBRIDIZATION AND THEIR ASSOCIATIONS IN 5 ETHNIC-GROUPS [J].
FERNANDEZVINA, MA ;
GAO, XJ ;
MORAES, ME ;
MORAES, JR ;
SALATIEL, I ;
MILLER, S ;
TSAI, J ;
SUN, YP ;
AN, JB ;
LAYRISSE, Z ;
GAZIT, E ;
BRAUTBAR, C ;
STASTNY, P .
IMMUNOGENETICS, 1991, 34 (05) :299-312
[8]   OLIGOTYPING OF ITALIAN CELIAC PATIENTS WITH THE 11TH INTERNATIONAL HISTOCOMPATIBILITY WORKSHOP REAGENTS [J].
FERRANTE, P ;
PETRONZELLI, F ;
MARIANI, P ;
BONAMICO, M ;
MAZZILLI, MC .
TISSUE ANTIGENS, 1992, 39 (01) :38-39
[9]  
HAMAGUCHI K, 1992, HLA 1991, V2, P488
[10]   RESTRICTION FRAGMENT LENGTH POLYMORPHISM IN HLA CLASS-II GENES OF LATIN-AMERICAN CAUCASIAN CELIAC-DISEASE PATIENTS [J].
HERRERA, M ;
CHERTKOFF, L ;
PALAVECINO, E ;
MOTA, A ;
GUALA, MD ;
FAINBOIM, L ;
SATZ, ML .
HUMAN IMMUNOLOGY, 1989, 26 (04) :272-280
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