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Association of TNF polymorphisms with sarcoidosis, its prognosis and tumour necrosis factor (TNF)-α levels in Asian Indians

机译:TNF多态性与结节病,其预后和亚洲印第安人肿瘤坏死因子(TNF)-α水平的关系

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摘要

Tumour necrosis factor (TNF)-α, an important proinflammatory cytokine, has been implicated in the pathogenesis of sarcoidosis, a multi-systemic granulomatous disorder of unknown aetiology. Here, we report for the first time the association of TNF haplotypes and genotypes with sarcoidosis and its prognosis in the Indian population. Five potentially functional promoter polymorphisms in the TNFA gene and a LTA_NcoI polymorphism (+252 position) of the LTA gene were genotyped in a clinically well-defined cohort of North-Indian patients with sarcoidosis (n = 96) and their regional controls (n = 155). Serum TNF-α (sTNF-α) and serum angiotensin converting enzyme (SACE) levels were measured and correlated with genotypes and haplotypes. The TNFA_-1031 and TNFA_-863 polymorphisms were identified as markers for disease onset (FET P = 0·006 and 0·042 for TNFA_-1031 and TNFA_-863, respectively). Additionally, the allele A of LTA_NcoI polymorphism was shown to be prevalent in the ‘no treatment’ group (FET P = 0·005), while the G allele was associated with frequent relapses on drug withdrawal (P = 0·057). Furthermore, the TNFA-308G>A and the TNFA-238G>A polymorphisms were found to influence sTNF-α (P = 0·054 and 0·0005, respectively) and SACE levels (P = 0·0017 and 0·056, respectively). The haplotype frequencies were significantly different in the patients and the controls (P = 0·0067). The haplotype GTCCGG was identified as the major risk/susceptibility haplotype (P = 0·003) and was associated with increased SACE levels in the patient population. In conclusion, our study suggests an association of TNF polymorphisms with sarcoidosis.
机译:肿瘤坏死因子(TNF)-α,一种重要的促炎细胞因子,与结节病(一种病因不明的多系统性肉芽肿性疾病)的发病机制有关。在这里,我们首次报告TNF单倍型和基因型与结节病及其在印度人口中的预后的关联。在临床上明确定义的北印度结节病患者(n = 96)和他们的区域对照(n = 155)。测量血清TNF-α(sTNF-α)和血清血管紧张素转化酶(SACE)的水平,并与基因型和单倍型相关。 TNFA_-1031和TNFA_-863多态性被确定为疾病发作的标志物(TNFA_-1031和TNFA_-863的FET P分别为0·006和0·042)。此外,LTA_NcoI多态性的等位基因A在“不治疗”组中很普遍(FET P = 0·005),而G等位基因则与戒断频发有关(P = 0·057)。此外,发现TNFA-308G> A和TNFA-238G> A的多态性会影响sTNF-α(分别为P = 0·054和0·0005)和SACE水平(P = 0·0017和0·056,分别)。患者和对照组的单倍型频率显着不同(P = 0·0067)。单倍型GTCCGG被确定为主要的危险/易感性单倍型(P = 0·003),并且与患者群体中SACE水平升高有关。总之,我们的研究表明TNF多态性与结节病有关。

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