HLA-LINKED GENES ACTING AS ADDITIVE SUSCEPTIBILITY FACTORS IN CELIAC-DISEASE

被引:35
作者
FERNANDEZARQUERO, M [1 ]
FIGUEREDO, MA [1 ]
MALUENDA, C [1 ]
DELACONCHA, EG [1 ]
机构
[1] UNIV COMPLUTENSE MADRID,SAN CARLOS HOSP,DEPT PEDIAT,MADRID,SPAIN
来源
HUMAN IMMUNOLOGY | 1995年 / 42卷 / 04期
关键词
D O I
10.1016/0198-8859(94)00108-3
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Susceptibility to developing CD is widely accepted to be primarily associated with a particular HLA-DQ alpha beta heterodimer encoded by the DQA1(*)0501 and DQB1(*)0201 alleles in cis position on the DR3,DQ2 haplotype or in trans position by DR5,DQ7/DR7,DQ2 heterozygotes. We performed genomic HLA-DR and DQ typing of 100 unrelated Spanish celiac children and 180 ethnically matched controls. As expected, most (92 out of 100) celiac patients carried the HLA-DQ alpha beta heterodimer, and we selected these individuals for further studies. The results corroborate that although the DQA1(*)0501 and DQB1(*)0201 genes in single dosage appear sufficient for conferring disease susceptibility, individuals homozygotes for DQB1(*)0201 show an increased risk. Furthermore, our data also show that those carrying the genotype DR5,DQ7/DR7,DQ2 have a significantly increased risk of developing CD as compared to those that are non-DR7 positive, also carrying the CD-associated HLA-DQ alpha beta heterodimer. This strongly suggests that there is an MHC linked non-HLA-DQ gene primarily associated with CD present on DR7,DQ2 haplotype, which should either be DR7 or in strong linkage disequilibrium with it. Our data also indicate that, as has already been suggested, another HLA-associated CD susceptibility gene may be present on some DR4-carrying haplotypes.
引用
收藏
页码:295 / 300
页数:6
相关论文
共 30 条
[1]   CLONING AND SEQUENCE-ANALYSIS OF THE HUMAN MAJOR HISTOCOMPATIBILITY COMPLEX GENE DC-3-BETA [J].
BOSS, JM ;
STROMINGER, JL .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1984, 81 (16) :5199-5203
[2]  
BRAUTBAR C, 1981, TISSUE ANTIGENS, V17, P313
[3]   A TECHNIQUE FOR RADIOLABELING DNA RESTRICTION ENDONUCLEASE FRAGMENTS TO HIGH SPECIFIC ACTIVITY [J].
FEINBERG, AP ;
VOGELSTEIN, B .
ANALYTICAL BIOCHEMISTRY, 1983, 132 (01) :6-13
[4]   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
[5]   MUTATIONS AND SELECTION IN THE GENERATION OF CLASS-II HISTOCOMPATIBILITY ANTIGEN POLYMORPHISM [J].
GUSTAFSSON, K ;
WIMAN, K ;
EMMOTH, E ;
LARHAMMAR, D ;
BOHME, J ;
HYLDIGNIELSEN, JJ ;
RONNE, H ;
PETERSON, PA ;
RASK, L .
EMBO JOURNAL, 1984, 3 (07) :1655-1661
[6]  
HALDANE JBS, 1955, ANN HUM GENET, V20, P309
[7]   STRUCTURAL-ANALYSIS OF THE HLA-DR, HLA-DQ, AND HLA-DP ALLELES ON THE CELIAC DISEASE-ASSOCIATED HLA-DR3 (DRW17) HAPLOTYPE [J].
KAGNOFF, MF ;
HARWOOD, JI ;
BUGAWAN, TL ;
ERLICH, HA .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (16) :6274-6278
[8]  
KAGNOFF MF, 1992, GASTROENTEROL CLIN N, V21, P405
[9]  
KARR RW, 1986, J IMMUNOL, V137, P2886
[10]   COMPLETE AMINO-ACID-SEQUENCE OF AN HLA-DR ANTIGEN-LIKE BETA-CHAIN AS PREDICTED FROM THE NUCLEOTIDE-SEQUENCE - SIMILARITIES WITH IMMUNOGLOBULINS AND HLA-A, HLA-B, AND HLA-C ANTIGENS [J].
LARHAMMAR, D ;
SCHENNING, L ;
GUSTAFSSON, K ;
WIMAN, K ;
CLAESSON, L ;
RASK, L ;
PETERSON, PA .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1982, 79 (12) :3687-3691
123