Molecular Immunogenetics Group, National Institute of Immunology, New Delhi, 110067, India.
Systems Biology Group, CSIR - Institute of Genomics and Integrative Biology, New Delhi, 110025, India.
Br J Dermatol. 2018 Feb;178(2):482-491. doi: 10.1111/bjd.15391. Epub 2017 Oct 9.
Vitiligo is a multifactorial, autoimmune, depigmenting disorder of the skin where aberrant presentation of autoantigens may have a role.
To study the association of two antigen-processing genes, PSMB8 and PSMB9, with vitiligo.
In total 1320 cases of vitiligo (1050 generalized and 270 localized) and 752 healthy controls were studied for the PSMB9 exon 3 G/A single-nucleotide polymorphism (SNP), PSMB8 exon 2 C/A SNP and PSMB8 intron 6 G/T SNP at site 37 360 using polymerase chain reaction (PCR)-restriction fragment length polymorphism. Real-time PCR was used for transcriptional expression of PSMB8 and cytokines. Expression of ubiquitinated proteins and phosphorylated-p38 (P-p38) was studied by Western blotting.
Significant increases in PSMB8 exon 2 allele A (P < 2.07 × 10 , odds ratio 1·93) and genotypes AA (P < 1.03 × 10 , odds ratio 2·51) and AC (P < 1.29 × 10 , odds ratio 1·63) were observed in patients with vitiligo. Interferon-γ stimulation induced lower expression of PSMB8 in peripheral blood mononuclear cells of cases compared with controls, suggesting impaired antigen processing, which was confirmed by accumulation of ubiquitinated proteins in both lesional and nonlesional skin of patients with vitiligo. Expression of proinflammatory cytokines - interleukin (IL)-6, IL-1β and IL-8 - was higher in the lesional skin. P-p38 expression was variable but correlated with the amount of ubiquitinated proteins in the lesional and nonlesional skin, suggesting that the inflammatory cytokine responses in lesional skin could be a result of both P-p38-dependent and -independent pathways.
The PSMB8 exon 2 SNP is significantly associated with vitiligo. Accumulation of ubiquitinated proteins in skin of cases of vitiligo suggests their aberrant processing, which may promote the development of the disease.
白癜风是一种多因素自身免疫性脱色素疾病,其自身抗原的异常表达可能起作用。
研究两个抗原加工基因 PSMB8 和 PSMB9 与白癜风的相关性。
采用聚合酶链反应(PCR)-限制性片段长度多态性技术,对 1320 例白癜风(1050 例泛发性和 270 例局限性)和 752 例健康对照者的 PSMB9 外显子 3 G/A 单核苷酸多态性(SNP)、PSMB8 外显子 2 C/A SNP 和 PSMB8 内含子 6 G/T SNP 位点 37360 进行研究。采用实时 PCR 检测 PSMB8 和细胞因子的转录表达。通过 Western 印迹法研究泛素化蛋白和磷酸化-p38(P-p38)的表达。
白癜风患者 PSMB8 外显子 2 等位基因 A(P<2.07×10-8,优势比 1.93)和基因型 AA(P<1.03×10-8,优势比 2.51)和 AC(P<1.29×10-8,优势比 1.63)显著增加。与对照组相比,干扰素-γ刺激后白癜风患者外周血单个核细胞中 PSMB8 的表达降低,提示抗原加工受损,这在白癜风患者的皮损和非皮损皮肤中泛素化蛋白的积累中得到证实。皮损中促炎细胞因子白细胞介素(IL)-6、IL-1β和 IL-8 的表达较高。P-p38 的表达是可变的,但与皮损和非皮损皮肤中泛素化蛋白的量相关,表明皮损中炎症细胞因子的反应可能是 P-p38 依赖性和非依赖性途径的结果。
PSMB8 外显子 2 SNP 与白癜风显著相关。白癜风患者皮肤中泛素化蛋白的积累表明其异常加工,这可能促进疾病的发展。
