MAJOR HISTOCOMPATIBILITY COMPLEX HAPLOTYPES AND COMPLEMENT-C4 ALLELES IN SYSTEMIC LUPUS-ERYTHEMATOSUS - RESULTS OF A MULTICENTER STUDY

被引：132

作者：

HARTUNG, K

BAUR, MP

COLDEWEY, R

FRICKE, M

KALDEN, JR

LAKOMEK, HJ

PETER, HH

SCHENDEL, D

SCHNEIDER, PM

SEUCHTER, SA

STANGEL, W

DEICHER, HRG

机构：

[1] UNIV HANNOVER, W-3000 HANNOVER, GERMANY

[2] UNIV FREIBURG, W-7800 FREIBURG, GERMANY

[3] UNIV ERLANGEN NURNBERG, W-8520 ERLANGEN, GERMANY

[4] UNIV DUSSELDORF, W-4000 DUSSELDORF 1, GERMANY

[5] UNIV BONN, W-5300 BONN, GERMANY

[6] UNIV MAINZ, W-6500 MAINZ, GERMANY

[7] UNIV MUNICH, W-8000 MUNICH 2, GERMANY

来源：

JOURNAL OF CLINICAL INVESTIGATION | 1992年 / 90卷 / 04期

关键词：

SYSTEMIC LUPUS ERYTHEMATOSUS; GENETICS; HLA; FAMILY STUDIES; AUTOIMMUNITY;

D O I：

10.1172/JCI116000

中图分类号：

R-3 [医学研究方法]; R3 [基础医学];

学科分类号：

1001 ;

摘要：

In a multicenter study more than 300 central European systemic lupus erythematosus (SLE) patients were examined for HLA-B, HLA-DR, and complement C4 phenotypes. For 174 SLE patients MHC haplotypes were determined by family segregation analysis, and for 155 patients C4 gene deletions were determined by TaqI restriction fragment length polymorphism. Two haplotypes, B8-C4AQ0-C4B1-DR3 and B7-C4A3-C4B1-DR2, were identified as risk factors for SLE. These findings were confirmed by applying the haplotype frequency difference (HFD) method, which uses nontransmitted haplotypes from the family study as internal controls. Furthermore, only HLA-DR2, but not DR3, B7, or B8, was significantly increased in SLE patients independently of the two risk haplotypes. C4A gene deletions, but not silent C4AQ0 alleles, were increased in SLE patients and neither C4BQ0 alleles nor C4B gene deletions were increased. The observed frequencies of homozygosity and heterozygosity for the two haplotypes and the frequencies of homozygotes for C4AQ0. and C4A deletions did not differ from the expected values, indicating that the risk for SLE is conveyed by single allele effects. In conclusion, there are two MHC-linked susceptibility factors for Caucasian SLE patients carried by the haplotypes B7-DR2 and B8-DR3. The results argue against C4Q0 alleles being the decisive factors increasing susceptibility to SLE.

引用

页码：1346 / 1351

页数：6

共 52 条

[41] STURFELT G, 1988, SCAND J REHEUMATOL S, V72, P35
[42] HLA GENOTYPE DISTRIBUTION AND GENETIC MODELS OF INSULIN-DEPENDENT DIABETES-MELLITUS
SVEJGAARD, A
RYDER, LP
[J]. ANNALS OF HUMAN GENETICS, 1981, 45 (JUL) : 293 - 298
[43] SPECIAL ARTICLE - THE 1982 REVISED CRITERIA FOR THE CLASSIFICATION OF SYSTEMIC LUPUS-ERYTHEMATOSUS
TAN, EM
COHEN, AS
FRIES, JF
MASI, AT
MCSHANE, DJ
ROTHFIELD, NF
SCHALLER, JG
TALAL, N
WINCHESTER, RJ
[J]. ARTHRITIS AND RHEUMATISM, 1982, 25 (11): : 1271 - 1277
[44] ASSOCIATION BETWEEN A T-CELL RECEPTOR RESTRICTION-FRAGMENT-LENGTH-POLYMORPHISM AND SYSTEMIC LUPUS-ERYTHEMATOSUS
TEBIB, JG
ALCOCERVARELA, J
ALARCONSEGOVIA, D
SCHUR, PH
[J]. JOURNAL OF CLINICAL INVESTIGATION, 1990, 86 (06) : 1961 - 1967
[45] Terasaki P., 1965, HISTOCOMPATIBILITY T
[46] TIWARI J, 1985, HLA DISEASE ASS
[47] A MOLECULAR-BASIS FOR MHC CLASS-II - ASSOCIATED AUTOIMMUNITY
TODD, JA
ACHAORBEA, H
BELL, JI
CHAO, N
FRONEK, Z
JACOB, CO
MCDERMOTT, M
SINHA, AA
TIMMERMAN, L
STEINMAN, L
MCDEVITT, HO
[J]. SCIENCE, 1988, 240 (4855) : 1003 - 1009
[48] WELCH TR, 1988, DIS MARKERS, V6, P247
[49] WHITTINGHAM S, 1983, TISSUE ANTIGENS, V21, P50
[50] MODE OF INHERITANCE OF DECREASED C3B RECEPTORS ON ERYTHROCYTES OF PATIENTS WITH SYSTEMIC LUPUS-ERYTHEMATOSUS
WILSON, JG
WONG, WW
SCHUR, PH
FEARON, DT
[J]. NEW ENGLAND JOURNAL OF MEDICINE, 1982, 307 (16) : 981 - 986

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