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Quantifying Protein-Specific N-Glycome Profiles by Focused Protein and Immunoprecipitation Glycomics

机译:通过聚焦蛋白和免疫沉淀糖量定量蛋白质特异性的N-Glycome曲线

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Serum N-glycans have been reported to be potential diagnostic and therapeutic biomarkers for many diseases and conditions, such as inflammation, fibrosis, and cancer progression. We previously described the focused protein glycomic analysis (FPG) from gel-separated serum proteins. With this methodology, we sought novel glycan biomarkers for nonalcoholic steatohepatitis (NASH) and successfully identified some N-glycans that were significantly elevated in NASH patients compared to nonalcoholic fatty liver patients. Among them, trisialylated monofucosylated triantennary glycan (A3F) of alpha-1 antitrypsin showed the most dynamic change. For rapid identification of N-glycans on the focused proteins, we constructed a simplified method called immunoprecipitation glycomics (IPG), where the target proteins were immunoprecipitated with affinity beads and subsequently subjected to glycomic analysis by MALDI-TOF MS. Focusing on alpha-1 antitrypsin and ceruloplasmin as the target proteins, we compared the values of N-glycans determined by FPG and IPG. The quantified values of each N-glycan by these two methods showed a statistically significant correlation, indicating that high throughput and quantitative N-glycomics of targeted proteins can be achieved by the simplified IPG method. Thus, an analytical strategy combining FPG and IPG can be adapted to general biomarker discovery and validation in appropriate disease areas.
机译:据报道,血清N-聚糖是许多疾病和病症的潜在诊断和治疗生物标志物,如炎症,纤维化和癌症进展。我们之前描述了来自凝胶分离的血清蛋白的聚焦蛋白质糖分比分析(FPG)。通过这种方法,我们寻求新的聚糖生物标志物用于非酒精性脱脂性(NASH),并成功地确定了与非酒精性脂肪肝患者相比在纳什患者中显着升高的一些N-Glycans。其中,α-1抗胰蛋白酶的三种状糖化的单藻糖基化三糖甘油(A3F)显示出最动力的变化。为了在聚焦蛋白上的快速鉴定N-聚糖,我们构建了一种称为免疫沉淀糖精(IPG)的简化方法,其中靶蛋白质用亲和力珠免疫,随后通过MALDI-TOF MS进行含量进行糖分分析。专注于α-1抗胰蛋白酶和刺激子作为靶蛋白,我们比较了由FPG和IPG测定的N-聚糖的值。通过这两种方法的每种N-聚糖的量化值显示出统计学上显着的相关性,表明通过简化的IPG方法可以实现靶向蛋白的高通量和定量N-糖。因此,组合FPG和IPG的分析策略可以适应在适当的疾病区域中的一般生物标志物发现和验证。

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