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首页> 外文期刊>Journal of Radiation Research >Purified PEGylated human glucagon-like peptide-2 reduces the severity of irradiation-induced acute radiation enteritis in rats
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Purified PEGylated human glucagon-like peptide-2 reduces the severity of irradiation-induced acute radiation enteritis in rats

机译:纯化的PEG化人胰高血糖素样肽2可降低大鼠辐射诱发的急性放射性肠炎的严重程度

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摘要

Radiation-induced acute intestinal injury after abdominal and pelvic irradiation is a common and serious problem in the clinical setting. Glucagon-like peptide-2 (GLP-2), a 33-amino acid peptide, exerts diverse effects related to the regulation of gastrointestinal growth and function. However, GLP-2 is relatively unstable in vivo. The aim of the present study was to improve GLP-2 stability in vivo and to evaluate its therapeutic effect on acute radiation enteritis. We generated long-lasting intestinal protection peptides by conjugating human GLP-2 (hGLP-2) peptides to polyethyleneglycol (PEG) to produce mPEGylation hGLP-2 (Mono-PEG-hGLP-2) through an enzymatic site-specific transglutamination reaction. Mono-PEG-hGLP-2 synthesized under optimal reaction conditions and separated by one-step ion-exchange chromatography was found to be resistant to degradation in vitro. Pretreatment with Mono-PEG-hGLP-2 reduced the severity of radiation-induced intestinal injury, oxidative stress, and the expression of NF-κB in rats with irradiation-induced acute radiation enteritis. The enhanced biological potency of Mono-PEG-hGLP-2 highlights its potential as a therapeutic agent for intestinal diseases.
机译:在腹部和骨盆照射后,辐射诱发的急性肠道损伤是临床中常见且严重的问题。胰高血糖素样肽2(GLP-2)是一种33个氨基酸的肽,具有与胃肠道生长和功能调节相关的多种作用。但是,GLP-2在体内相对不稳定。本研究的目的是改善体内GLP-2的稳定性,并评估其对急性放射性肠炎的治疗效果。我们通过将人GLP-2(hGLP-2)肽与聚乙二醇(PEG)结合以通过酶促位点特异性转谷氨酰胺化反应产生mPEG化hGLP-2(Mono-PEG-hGLP-2),从而产生了持久的肠道保护肽。发现在最佳反应条件下合成并通过一步离子交换色谱分离的Mono-PEG-hGLP-2具有体外抗降解能力。 Mono-PEG-hGLP-2预处理可降低辐射诱发的急性放射性肠炎大鼠的辐射诱发的肠损伤,氧化应激和NF-κB的表达。 Mono-PEG-hGLP-2的增强的生物效能突出了其作为肠道疾病治疗剂的潜力。

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