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猪胃肠道胰高血糖素样免疫活性物质的提取、凝胶过滤图谱及受体结合情况

Extraction, gel filtration pattern, and receptor binding of porcine gastrointestinal glucagon-like immunoreactivity.

作者信息

Holst J J

出版信息

Diabetologia. 1977 Apr;13(2):159-69. doi: 10.1007/BF00745145.

Abstract

Different techniques for the extraction and initial purification of porcine gastrointestinal glucagon-like immunoreactivity (GLI) were compared with reference to yield, and preservation of number and pattern of GLI components. The conventional acid-ethanol technique combined with ethanol-ether purification gave high yields and a reproducible pattern of components. Large amounts of tissue were more easily extracted using another technique, based on extraction by boiling, extraction and precipitation with acetone, and--if necessary--salting out. By means of the latter two techniques mucosal tissue from all of the porcine gastrointestinal tract was extracted and subjected to gel filtration. Glucagon-like peptides were searched for using: 1. a radioimmunoassay which quantifies gut type glucagon (GTG), as well as pancreatic type glucagon (PTG), 2. a radioimmunoassay highly specific for pancreatic type glucagon (PTG), and 3. a radioreceptor assay based on binding of glucagon to porcine liver cell membranes. The oesophageal, the fundic, and the antro-pyloric parts of the gastric mucosa contained very small amounts of GLI. The cardiac gland region contained small amounts of a peptide indistinguishable from "true" glucagon. The duodenal mucosa contained small amounts of "true" glucagon and may be a smaller, glucagon-like peptide. The mucosa of the small intestine contained large amounts of both high and low molecular weight GTG and, in addition, PTG of high molecular weight and "true" glucagon. The colon also contained these components with "true" glucagon in high concentrations. Only small GTG and "true" glucagon were receptor-active, the former with less than its immunometric potency.

摘要

比较了猪胃肠道胰高血糖素样免疫活性物质(GLI)提取和初步纯化的不同技术,涉及产量以及GLI成分数量和模式的保留情况。传统的酸 - 乙醇技术结合乙醇 - 乙醚纯化可获得高产率和可重复的成分模式。使用另一种基于煮沸提取、丙酮提取和沉淀以及必要时盐析的技术,可以更轻松地提取大量组织。通过后两种技术,对猪整个胃肠道的黏膜组织进行了提取并进行凝胶过滤。使用以下方法寻找胰高血糖素样肽:1. 一种放射免疫测定法,可定量肠道型胰高血糖素(GTG)以及胰腺型胰高血糖素(PTG);2. 一种对胰腺型胰高血糖素(PTG)具有高度特异性的放射免疫测定法;3. 一种基于胰高血糖素与猪肝细胞膜结合的放射受体测定法。胃黏膜的食管、胃底和胃窦 - 幽门部分含有极少量的GLI。贲门腺区含有少量与“真”胰高血糖素无法区分的肽。十二指肠黏膜含有少量的“真”胰高血糖素和一种较小的、类似胰高血糖素的肽。小肠黏膜含有大量高分子量和低分子量的GTG,此外还含有高分子量的PTG和“真”胰高血糖素。结肠也含有这些成分,其中“真”胰高血糖素浓度较高。只有小分子量的GTG和“真”胰高血糖素具有受体活性,前者的受体活性低于其免疫测定效力。

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