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Identification of TPIT and other novel autoantigens in lymphocytic hypophysitis; immunoscreening of a pituitary cDNA library and development of immunoprecipitation assays

机译:淋巴细胞垂体炎中TPIT和其他新型自身抗原的鉴定;脑垂体cDNA文库的免疫筛选和免疫沉淀测定法的发展

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摘要

Background: Lymphocytic hypophysitis is an organ-specific autoimmune disease of the pituitary gland. A specific and sensitive serological test currently does not exist to aid in the diagnosis. Objective: To identify target autoantigens in lymphocytic hypophysitis and develop a diagnostic assay for these proteins. Design/methods: A pituitary cDNA expression library was immunoscreened using sera from four patients with lymphocytic hypophysitis. Relevant cDNA clones from screening, along with previously identified autoantigens pituitary gland-specific factor 1a and 2 (PGSF1a and PGSF2) and neuron-specific enolase (NSE) were tested in an in vitro transcription and translation immunoprecipitation assay. The corticotroph-specific transcription factor, TPIT, was investigated separately as a candidate autoantigen. Results: Significantly positive autoantibody reactivity against TPIT was found in 9/86 hypophysitis patients vs 1/90 controls (P=0.018). The reactivity against TPIT was not specific for lymphocytic hypophysitis with autoantibodies detectable in the sera from patients with other autoimmune endocrine diseases. Autoantibodies were also detected against chromodomain-helicase-DNA binding protein 8, presynaptic cytomatrix protein (piccolo), Ca²⁺-dependent secretion activator, PGSF2 and NSE in serum samples from patients with lymphocytic hypophysitis, but at a frequency that did not differ from healthy controls. Importantly, 8/86 patients with lymphocytic hypophysitis had autoantibodies against any two autoantigens in comparison with 0/90 controls (P=0.0093). Conclusions: TPIT, a corticotroph-specific transcription factor, was identified as a target autoantigen in 10.5% of patients with lymphocytic hypophysitis. Further autoantigens related to vesicle processing were also identified as potential autoantigens with different immunoreactivity patterns in patients and controls.
机译:背景:淋巴细胞性垂体炎是垂体的一种器官特异性自身免疫性疾病。目前尚不存在特异性和灵敏的血清学检查以帮助诊断。目的:鉴定淋巴细胞性垂体炎中的靶自身抗原,并开发出针对这些蛋白的诊断方法。设计/方法:使用来自四名淋巴细胞性垂体炎患者的血清对垂体cDNA表达文库进行免疫筛选。在体外转录和翻译免疫沉淀试验中,对来自筛选的相关cDNA克隆以及先前确定的自身抗原垂体特异性因子1a和2(PGSF1a和PGSF2)和神经元特异性烯醇化酶(NSE)进行了测试。皮质激素特异性转录因子TPIT作为候选自身抗原被单独研究。结果:9/86垂体炎患者相对于1/90对照患者发现针对TPIT的自身抗体显着阳性(P = 0.018)。对TPIT的反应性并非特异性针对淋巴细胞性垂体炎,其自身抗体可从患有其他自身免疫性内分泌疾病的患者血清中检出。还从淋巴细胞性垂体炎患者的血清样品中检测到了针对染色体结构域解旋酶-DNA结合蛋白8,突触前细胞基质蛋白(piccolo),Ca 2+依赖性分泌激活剂,PGSF2和NSE的自身抗体,但频率与健康人并无差异控件。重要的是,与0/90对照相比,患有淋巴细胞性垂体炎的8/86患者具有针对任何两种自身抗原的自身抗体(P = 0.0093)。结论:糖皮质激素特异性转录因子TPIT被确定为10.5%的淋巴细胞性垂体炎患者的目标自身抗原。与囊泡加工有关的其他自身抗原也被鉴定为患者和对照中具有不同免疫反应模式的潜在自身抗原。

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