HLA CLASS-II ASSOCIATIONS WITH IDIOPATHIC NEPHROTIC SYNDROME IN CHILDREN

被引：29

作者：

KONRAD, M

MYTILINEOS, J

BOUISSOU, F

SCHERER, S

GULLI, MP

MEISSNER, I

CAMBONTHOMSEN, A

OPELZ, G

SCHARER, K

机构：

[1] UNIV HEIDELBERG,KINDERKLIN,DIV PEDIAT NEPHROL,INF 150,D-69120 HEIDELBERG,GERMANY

[2] UNIV HEIDELBERG,DIV TRANSPLANTAT IMMUNOL,W-6900 HEIDELBERG,GERMANY

[3] HOP PURPAN,DIV PEDIAT,NEPHROL,TOULOUSE,FRANCE

[4] HOP PURPAN,CRPC,CNRS,UPR 8291,TOULOUSE,FRANCE

来源：

TISSUE ANTIGENS | 1994年 / 43卷 / 05期

关键词：

MAJOR HISTOCOMPATIBILITY COMPLEX; NEPHROTIC SYNDROME; RESTRICTION FRAGMENT LENGTH POLYMORPHISM; CHILDREN;

D O I：

10.1111/j.1399-0039.1994.tb02340.x

中图分类号：

Q2 [细胞生物学];

学科分类号：

071009 ; 090102 ;

摘要：

The occasional familial occurrence of idiopathic nephrotic syndrome (NS) points to a genetic predisposition. Reports on associations with certain HLA class II antigens support this hypothesis. In order to define the immunogenetic background of NS more precisely, HLA class II allele frequencies in 161 children with NS were studied by restriction fragment length polymorphism (RFLP) typing. The patient cohorts consisted of 87 children from Southwest-France and 74 from Southwest-Germany. The control group consisted of 118 French and 101 German unrelated individuals from the same geographical areas. HLA alleles were defined in patients with steroid-sensitive (SS) and steroid-resistant (SR) NS and in controls. RFLP typing revealed that the previously reported association between SSNS and HLA-DR7 is confined to the RFLP split 7.1 (DRB1*07) with a combined relative risk (RRcomb) of 6.2. HLA-DQB typing showed an increased frequency of the allele DQB2b (DQB1*0201) (RRcomb=7.8). HLA-DQA typing showed an association of SSNS with DQA3 (DQA1*0201,0301,0302) (RRcomb=4.1). The highest RR (16.5) for SSNS was found in German patients who carried the two DRB1 specificities 17.1 (DRB1*0301) and 7.1 (DRB1*07). All associations were stronger in SS patients with frequent relapses or steroid dependency than in non- or infrequent relapsers. SR patients exhibited no significant associations with HLA class II alleles.

引用

页码：275 / 280

页数：6

共 34 条

[1] ABE K, 1991, 11TH INT HIST WORKSH
[2] ALFILER CA, 1980, CLIN NEPHROL, V14, P71
[3] [Anonymous], 1979, Lancet, V1, P401
[4] CDNA CLONE FOR THE HEAVY-CHAIN OF THE HUMAN B-CELL ALLOANTIGEN DC1 - STRONG SEQUENCE HOMOLOGY TO THE HLA-DR HEAVY-CHAIN
AUFFRAY, C
KORMAN, AJ
ROUXDOSSETO, M
BONO, R
STROMINGER, JL
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1982, 79 (20): : 6337 - 6341
[5] DNA-RFLP ANALYSIS AND GENOTYPING OF HLA-DR AND DQ ANTIGENS
BIDWELL, J
[J]. IMMUNOLOGY TODAY, 1988, 9 (01): : 18 - 23
[6] HLA-DR ALLOGENOTYPING USING EXON-SPECIFIC CDNA PROBES AND APPLICATION OF RAPID MINIGEL METHODS
BIDWELL, JL
JARROLD, EA
[J]. MOLECULAR IMMUNOLOGY, 1986, 23 (10) : 1111 - 1116
[7] A DNA-RFLP TYPING SYSTEM THAT POSITIVELY IDENTIFIES SEROLOGICALLY WELL-DEFINED AND ILL-DEFINED HLA-DR AND DQ ALLELES, INCLUDING DRW10
BIDWELL, JL
BIDWELL, EA
SAVAGE, DA
MIDDLETON, D
KLOUDA, PT
BRADLEY, BA
[J]. TRANSPLANTATION, 1988, 45 (03) : 640 - 646
[8] CAMBONTHOMSEN A, 1986, PATHOL BIOL, V34, P725
[9] GENES ENCODING THE BETA-CHAINS OF HLA-DR7 AND HLA-DQW2 DEFINE MAJOR SUSCEPTIBILITY DETERMINANTS FOR IDIOPATHIC NEPHROTIC SYNDROME
CLARK, AGB
VAUGHAN, RW
STEPHENS, HAF
CHANTLER, C
WILLIAMS, DG
WELSH, KI
[J]. CLINICAL SCIENCE, 1990, 78 (04) : 391 - 397
[10] DEMARCHI M, 1979, TISSUE ANTIGENS, V14, P309

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