Association of HLA loci alleles and antigens in Saudi patients with vitiligo

被引：26

作者：

Abanmi, Abdullah ^{[1
]}

Al Harthi, Fahad ^{[1
]}

Al Baqami, Riyadh ^{[1
]}

Al Assaf, Saleh ^{[1
]}

Zouman, Abdulrahman ^{[1
]}

Arfin, Misbahul ^{[1
]}

Tariq, Mohammad ^{[1
]}

机构：

[1] Armed Forces Hosp, Dept Dermatol, Riyadh 11159, Saudi Arabia

来源：

ARCHIVES OF DERMATOLOGICAL RESEARCH | 2006年 / 298卷 / 07期

关键词：

vitiligo; HLA; Saudi;

D O I：

10.1007/s00403-006-0699-4

中图分类号：

R75 [皮肤病学与性病学];

学科分类号：

100206 ;

摘要：

HLA complex is composed of several closely linked loci, each containing several alleles, yielding a high expression of polymorphism. Vitiligo, a commonly acquired dermatological disorder, has been associated with different HLA antigens in different ethnic groups. In this study, HLA classes I (HLA-A, B, and C) and II (HLA-DR, DQ) antigens/alleles were analyzed in a group of 80 Saudi subjects consisting of vitiligo patients (40) and matched controls (40). The frequency of antigens of various HLA loci was tested using two-stage microcytotoxicity assays, while the frequency of alleles of HLA-DR was screened by polymerase chain reaction/sequence specific primers (PCR/SSP) method. The frequencies of HLA-B7, B15, Bw6, Cw6, Cw7, and DRB4*010101 were found to be significantly higher in vitiligo patients compared to controls [P = 0.029, 0.015, 0.033, 0.009, 0.043, and 0.015, respectively, with relative risk (RR) >= 3, etiologic fraction (EF) >= 0.4]. On the other hand, HLA-A9, B5, DQ1, and DRB3*010101 were significantly decreased in vitiligo patients compared to healthy Saudis [P = 0.008, 0.004, 0.028, and 0.04, respectively, with RR < 1 and preventive fraction (PF) < 0.5]. Among the patients, the highest allele frequency was noted for DRB4*010101(70%), while in controls it was for DRB3*010101 (72.5%). These results for antigens and allele frequency of various HLA Loci in vitiligo patients and control subjects suggested that HLA-B7, Bw6, Cw6, Cw7, and DRB4*010101 could be susceptible to vitiligo, while HLA-A9, B5, DQ1, and DRB3*010101 might be negatively associated with the development of vitiligo in Saudis.

引用

页码：347 / 352

页数：6

共 36 条

[1] STUDY OF HLA CLASS-I/II AND T-LYMPHOCYTE SUBSETS IN KUWAITI VITILIGO PATIENTS [J].

ALFOUZAN, A ;

ALARBASH, M ;

FOUAD, F ;

KAABA, SA ;

MOUSA, MA ;

ALHARBI, SA .

EUROPEAN JOURNAL OF IMMUNOGENETICS, 1995, 22 (02) :209-213

[2] GENETIC POLYMORPHISM IN HUMAN GLYCINE-RICH BETA-GLYCOPROTEIN [J].

ALPER, CA ;

BOENISCH, T ;

WATSON, L .

JOURNAL OF EXPERIMENTAL MEDICINE, 1972, 135 (01) :68-&

[3]

AMOS DB, 1980, MANUAL CLIN IMMUNOLO, P978

[4] DIFFERENCE IN CLINICAL-FEATURES AND HLA ANTIGENS BETWEEN FAMILIAL AND NONFAMILIAL VITILIGO OF NON-SEGMENTAL TYPE [J].

ANDO, I ;

CHI, HI ;

NAKAGAWA, H ;

OTSUKA, F .

BRITISH JOURNAL OF DERMATOLOGY, 1993, 129 (04) :408-410

[5] Vitiligo: complex segregation and linkage disequilibrium analyses with respect to microsatellite loci spanning the HLA [J].

Arcos-Burgos, M ;

Parodi, E ;

Salgar, M ;

Bedoya, E ;

Builes, JJ ;

Jaramillo, D ;

Ceballos, G ;

Uribe, A ;

Rivera, N ;

Rivera, D ;

Fonseca, I ;

Camargo, M ;

Palacio, LG .

HUMAN GENETICS, 2002, 110 (04) :334-342

[6]

Buc M, 1996, FOLIA BIOL-PRAGUE, V42, P23

[7]

Buc M, 1998, EUR J DERMATOL, V8, P13

[8] IDENTIFICATION OF PIGMENT CELL ANTIGENS DEFINED BY VITILIGO ANTIBODIES [J].

CUI, J ;

HARNING, R ;

HENN, M ;

BYSTRYN, JC .

JOURNAL OF INVESTIGATIVE DERMATOLOGY, 1992, 98 (02) :162-165

[9] PIGMENTARY PROBLEMS IN THE TROPICS [J].

DOMINGUEZSOTO, L ;

HOJYOTOMOKA, MT ;

VEGAMEMIJE, E ;

ARENAS, R ;

CORTESFRANCO, R .

DERMATOLOGIC CLINICS, 1994, 12 (04) :777-&

[10] VITILIGO IS ASSOCIATED WITH HLA-DR4 IN BLACK PATIENTS - A PRELIMINARY-REPORT [J].

DUNSTON, GM ;

HALDER, RM .

ARCHIVES OF DERMATOLOGY, 1990, 126 (01) :56-60

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