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利用灌注大鼠肠道来表征葡萄糖刺激后释放到浆膜分泌物中的胰高血糖素样免疫活性。

The use of perfused rat intestine to characterise the glucagon-like immunoreactivity released into serosal secretions following stimulation by glucose.

作者信息

O'Connor F A, Conlon J M, Buchanan K D, Murphy R F

出版信息

Horm Metab Res. 1979 Jan;11(1):19-23. doi: 10.1055/s-0028-1092674.

Abstract

Isolated perfused intestine of rat was used to demonstrate the glucose-stimulated release of glucagon-like immunoreactivity (GLI) into serosal secretions. The released GLI was characterised using immunoaffinity chromatography on columns of immobilised antibodies specific for the N (residues 1 to 18) and for the C (residues 19-29) terminal portions of glucagon followed by gel-filtration. The immunoreactivity was present in a variety of molecular species. These include a large GLI which has a molecular weight about 12000 and binds to antibodies specific for the N-terminal portion of glucagon and two polypeptide fractions with molecular weight closer to that of glucagon. While one fraction of the small GLI boun both to antibodies specific for the C-terminal and N-terminal portions of glucagon the other bound only to the former antibodies. The relevance of these findings to the origins of circulating GLI and the possible precursor relationship between large and other forms of GLI is discussed.

摘要

采用大鼠离体灌注肠段来证明葡萄糖刺激下胰高血糖素样免疫活性物质(GLI)释放到浆膜分泌物中。利用固定化抗体柱上的免疫亲和层析对释放的GLI进行表征,这些抗体分别针对胰高血糖素的N端(第1至18位氨基酸残基)和C端(第19 - 29位氨基酸残基),随后进行凝胶过滤。免疫活性存在于多种分子形式中。这些包括一种大分子GLI,其分子量约为12000,能与针对胰高血糖素N端的抗体结合,以及两种分子量更接近胰高血糖素的多肽组分。小GLI的一个组分既能与针对胰高血糖素C端和N端的抗体结合,另一个组分则仅能与前者抗体结合。讨论了这些发现与循环中GLI来源的相关性以及大分子GLI与其他形式GLI之间可能的前体关系。

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