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首页> 外文期刊>Evidence-based complementary and alternative medicine: eCAM >iTRAQ-Based Proteomics of Chronic Renal Failure Rats after FuShengong Decoction Treatment Reveals Haptoglobin and Alpha-1-Antitrypsin as Potential Biomarkers
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iTRAQ-Based Proteomics of Chronic Renal Failure Rats after FuShengong Decoction Treatment Reveals Haptoglobin and Alpha-1-Antitrypsin as Potential Biomarkers

机译:富豪通汤治疗后急性肾功能衰竭大鼠的ITRAQ蛋白质组学显示哈帕氟胺和α-1-抗酸血剂作为潜在的生物标志物

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Background. Chronic renal failure (CRF) has become a global health problem and bears a huge economic burden. FuShengong Decoction (FSGD) as traditional Chinese medicine has multiple pharmacological effects. Objectives. To understand the underlying molecular mechanism and signaling pathway involved in the FSGD treatment of CRF and screen differentially expressed proteins in rats with CRF treated with FSGD. Methods, Thirty-three male Sprague-Dawley rats were randomly divided into control group, CRF group, and FSGD group. Differentially expressed proteins were screened by iTRAQ coupled with nanoLC-MS/MS, and these identified proteins were later analyzed by GO, KEGG, and STRING. Additionally, haptoglobin (HP) and alpha-1-antitrypsin (AAT) were finally verified by ELISA, Western blot, and real time PCR. Results. A total of 417 proteins Were identified. Nineteen differentially expressed proteins were identified in the FSGD group compared with the model group, of which 3 proteins were upregulated and 16 proteins were downregulated. Cluster analysis indicated that inflammatory response was associated with these proteins and complement and coagulation cascade pathways were predominantly involved. The validation methods further confirmed that the levels of HP and AAT were significantly increased. Conclusions. HP and AAT maybe the important biomarkers in the pathogenesis of CRF and FSGD therapy.
机译:背景。慢性肾功能衰竭(CRF)已成为全球卫生问题,致力于巨大的经济负担。阜峰汤(FSGD)作为中药有多种药理作用。目标。为了了解CRF和筛网差异表达FSGD的大鼠FSGD处理中涉及的潜在的分子机制和信号通路。方法,三十三只雄性Sprague-Dawley大鼠随机分为对照组,CRF组和FSGD组。 ITRAQ偶联含有差异表达的蛋白质与纳米-SMS / MS滤,通过GO,Kegg和String稍后分析这些鉴定的蛋白质。此外,哈帕替洛蛋白(HP)和α-1-抗酸胆蛋白(AAT)最终通过ELISA,Western印迹和实时PCR验证。结果。共鉴定了共417个蛋白质。与模型组相比,在FSGD组中鉴定了19个差异表达的蛋白质,其中将3个蛋白质上调,并下调16个蛋白质。聚类分析表明,炎症反应与这些蛋白质相关,并且主要涉及凝固级联途径。验证方法进一步证实HP和AAT的水平显着增加。结论。 HP和AAT可能是CRF和FSGD治疗发病机制中的重要生物标志物。

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