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Proteomics in gastroparesis: unique and overlapping protein signatures in diabetic and idiopathic gastroparesis

机译:胃术中的蛋白质组学:糖尿病和特发性胃病的独特和重叠蛋白签名

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Macrophage-based immune dysregulatlon plays a critical role in development of delayed gastric emptying in diabetic mice. Loss of anti-inflammatory macrophages and increased expression of genes associated with pro-inflammatory macrophages has been reported in full-thickness gastric biopsies from gastroparesis patients. We aimed to determine broader protein expression (proteomics) and protein-based signaling pathways in gastric biopsies of diabetic (DG) and idiopathic gastroparesis (IG) patients. Additionally, we determined correlations between protein expressions, gastric emptying, and symptoms. Full-thickness gastric antrum biopsies were obtained from nine DG patients, seven IG patients, and five nondiabetic controls. Aptamer-based SomaLogic tissue scan that quantitatively identifies 1,305 human proteins was used. Protein fold changes were computed, and differential expressions were calculated using Limma. Ingenuity pathway analysis and correlations were carried out. Multiple-testing corrected P < 0.05 was considered statistically significant. Seventy-three proteins were differentially expressed in DG, 132 proteins were differentially expressed in IG, and 40 proteins were common to DG and IG.
机译:基于巨噬细胞的免疫抑制蛋白酶在糖尿病小鼠延迟胃排空的发展中起着重要作用。胃流血患者的全厚胃活组织检查报道了抗炎巨噬细胞的丧失和与促炎巨噬细胞相关的基因的增加。我们旨在确定糖尿病(DG)和特发性胃病(IG)患者的胃活组织检查中的更广泛的蛋白质表达(蛋白质组学)和基于蛋白质的信号通路。另外,我们确定蛋白质表达,胃排空和症状之间的相关性。从九种DG患者,七名IG患者和五个非糖尿病对照中获得全厚的胃窦活组织检查。基于Aptamer的微观组织扫描,定量识别1,305个人蛋白。计算蛋白质折叠变化,并使用雷玛计算差异表达。进行熟练的途径分析和相关性。多次测试校正P <0.05被认为是统计学上显着的。在DG中差异表达七十三种蛋白质,132个蛋白质以Ig差异表达,40个蛋白质对DG和Ig常见。

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