首页> 外文期刊>Experimental Biology and Medicine: Journal of the Society for Experimental Biology and Medicine >Haptoglobin as an early serum biomarker of virus-induced autoimmune type 1 diabetes in biobreeding diabetes resistant and LEW1.WR1 rats.
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Haptoglobin as an early serum biomarker of virus-induced autoimmune type 1 diabetes in biobreeding diabetes resistant and LEW1.WR1 rats.

机译:Haptoglobin作为生物诱导的糖尿病抗性和LEW1.WR1大鼠中病毒诱导的自身免疫1型糖尿病的早期血清生物标志物。

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Proteomic profiling of serum is a powerful technique to identify differentially expressed proteins that can serve as biomarkers predictive of disease onset. In this study, we utilized two-dimensional (2D) gel analysis followed by matrix-assisted-laser desorption/ionization time-of-flight mass spectrometry analysis to identify putative serum biomarkers for autoimmune type 1 diabetes (T1D) in biobreeding diabetes resistant (BBDR) rats induced to express the disease. Treatment with toll-like receptor 3 ligand, polyinosinic:polycytidilic acid (pIC), plus infection with Kilham rat virus (KRV), a rat parvovirus, results in nearly 100% of young BBDR rats becoming diabetic within 11-21 d. Sera collected from prediabetic rats at early time points following treatment with pIC + KRV were analyzed by 2D gel electrophoresis and compared with sera from control rats treated with phosphate-buffered saline, pIC alone or pIC + H1, a non-diabetogenic parvovirus. None of the latter three control treatments precipitates T1D. 2D gel analysis revealed that haptoglobin, an acute phase and hemoglobin scavenger protein, was differentially expressed in the sera of rats treated with pIC + KRV relative to control groups. These results were confirmed by Western blot and enzyme-linked immunosorbent assay studies, which further validated haptoglobin levels as being differentially increased in the sera of pIC + KRV-treated rats relative to controls during the first week following infection. Early elevations in serum haptoglobin were also observed in LEW1.WR1 rats that became diabetic following infection with rat cytomegalovirus. The identification and validation of haptoglobin as a putative serum biomarker for autoimmune T1D in rats now affords us the opportunity to test the validity of this protein as a biomarker for human T1D, particularly in those situations where viral infection is believed to precede the onset of disease.
机译:血清的蛋白质组学分析是一种强大的技术,可以鉴定差异表达的蛋白质,这些蛋白质可以用作预测疾病发作的生物标记。在这项研究中,我们利用了二维(2D)凝胶分析,然后进行了基质辅助激光解吸/电离飞行时间质谱分析,从而确定了在具有抗药性的生物繁殖型糖尿病(1)中自身免疫性1型糖尿病(T1D)的假定血清标志物。 BBDR)大鼠被诱导表达这种疾病。用Toll样受体3配体,多肌苷酸:聚胞苷酸(pIC)进行治疗,再加上感染Kilham大鼠病毒(KRV)(一种鼠细小病毒),导致近100%的年轻BBDR大鼠在11-21 d内患有糖尿病。通过2D凝胶电泳分析在pIC + KRV治疗后早期从糖尿病前期大鼠收集的血清,并将其与用磷酸盐缓冲液,单独pIC或pIC + H1(非糖尿病细小病毒)处理的对照组大鼠的血清进行比较。后三种对照处理均未沉淀出T1D。 2D凝胶分析表明,与对照组相比,用pIC + KRV处理的大鼠血清中触珠蛋白(一种急性期和血红蛋白清除剂)差异表达。这些结果通过蛋白质印迹和酶联免疫吸附试验研究得到了证实,该研究进一步证实,在感染后第一周内,pIC + KRV处理的大鼠血清中的触珠蛋白水平相对于对照组有差异地增加。在LEW1.WR1大鼠中也观察到血清触珠蛋白的早期升高,该大鼠在感染大鼠巨细胞病毒后变为糖尿病。鉴定和验证触珠蛋白作为大鼠自身免疫性T1D的推定血清生物标志物,现在使我们有机会测试该蛋白作为人T1D的生物标志物的有效性,特别是在认为病毒感染是在疾病发作之前的那些情况下。

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