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首页> 外文期刊>The Journal of trauma >Intestinal trefoil factor produced in Escherichia coli promotes the healing of rat burn-induced acute gastric mucosal lesions.
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Intestinal trefoil factor produced in Escherichia coli promotes the healing of rat burn-induced acute gastric mucosal lesions.

机译:大肠杆菌中产生的肠三叶因子促进大鼠烧伤诱导的急性胃粘膜病变的愈合。

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BACKGROUND: Intestinal trefoil factor (ITF), a member of the trefoil factor family, plays an important role in protecting the epithelial layer of the gastrointestinal tract from damage and repairing epithelium after injury. This study aims to produce ITF by Escherichia coli expression system and explore its role in the treatment of burn-induced acute gastric mucosal lesions. METHODS: Human ITF (hITF) gene encoding mature peptide was obtained by RT-PCR, and then inserted into the expression vector pET32a to construct the recombinant pET32a-hITF. After confirmation by gene sequencing, pET32a-hITF was transformed into E. coli Origami B(DE3), and TrxA-hITF fusion protein was expressed by conventional isopropyl-beta-d-thiogalactopyranoside induction in shake flask and analyzed with sodium dodecyl sulfate-polyacrylamide gel electorphoresis (SDS-PAGE) and Western-blot. Subsequently, TrxA-hITF was isolated by Nickel-nitrilotriacetic acid affinity chromatography, and ultrafiltration. Finally, a burn-induced rat gastric injury model was established, TrxA-hITF was administered orally and macroscopic and microscopic changes in gastric mucosa were observed. RESULTS: The correctness and integrity of hITF gene were identified by restriction digestion and gene sequencing. TrxA-hITF fusion protein was successfully expressed to 50 mg/L and its purity was above 95% after purification. SDS-PAGE and Western-blot analyses showed that the fusion protein presented as a single band with a molecular weight of 32 kDa, a little larger than the calculated value, 30 kDa. Lesion score and histologic examination revealed that TrxA-hITF alleviated rat gastric injury significantly. CONCLUSIONS: This study lays foundation for the commercial production of hITF and suggests a new way to treat burn-induced gastric lesions.
机译:背景:肠三叶因子(ITF)是三叶因子家族的成员,在保护胃肠道上皮层免受损伤和损伤后修复上皮中起着重要作用。本研究旨在通过大肠杆菌表达系统生产ITF,并探讨其在烧伤诱发的急性胃粘膜病变中的作用。方法:采用逆转录-聚合酶链反应(RT-PCR)获得编码成熟肽段的人ITF(hITF)基因,然后将其插入表达载体pET32a中,构建重组pET32a-hITF。经基因测序确认后,将pET32a-hITF转化到大肠杆菌Origami B(DE3)中,并通过常规异丙基-β-d-硫代吡喃半乳糖苷在摇瓶中诱导表达TrxA-hITF融合蛋白,并用十二烷基硫酸钠-聚丙烯酰胺进行分析凝胶电泳(SDS-PAGE)和Western印迹。随后,通过镍-三氮三乙酸亲和色谱和超滤分离TrxA-hITF。最后建立烧伤致大鼠胃损伤模型,口服TrxA-hITF,观察胃黏膜的宏观和微观变化。结果:通过限制性酶切和基因测序鉴定hITF基因的正确性和完整性。 TrxA-hITF融合蛋白成功表达至50 mg / L,纯化后纯度高于95%。 SDS-PAGE和Western-blot分析表明,融合蛋白呈一条分子量为32 kDa的单条带,比计算值30 kDa略大。病变评分和组织学检查显示,TrxA-hITF明显减轻了大鼠胃损伤。结论:本研究为hITF的商业化生产奠定了基础,并提出了治疗烧伤引起的胃部病变的新方法。

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