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胰腺大胰高血糖素的纯化及生物学特性

The purification and biological properties of pancreatic big glucagon.

作者信息

O'Connor K J, Lazarus N R

出版信息

Biochem J. 1976 May 15;156(2):265-77. doi: 10.1042/bj1560265.

Abstract
  1. Big glucagon was present in extracts of ox, dog, rat and turkey pancreas, representing 10-15% of the glucagon immunoreactivity, and was shown to be of islet origin by its presence in extracts of isolated pigeon islets. 2. Big glucagon was homogeneous by immunoassay after polyacrylamide-gel electrophoresis and was more electronegative than little glucagon. 3. Big glucagon was purified from bovine pancreas, and its apparent molecular weight was estimated by gel filtration as 8200+/-9%. 4. Limited tryptic proteolysis of the molecule produced an immunoreactive component slightly smaller than little glucagon. 5. Linear dilution curves were obtained with mammalian big glucagons by using both enteroglucagon cross-reacting and 'little-glucagon-carboxyl-end-specific' antisera. 6. The half-times for the disappearance of the immunoreactivity of big and little glucagon that had been injected into the rat circulation were 6.9 and 3.2min respectively. 7. Big glucagon was approximately one-sixth as effective as little glucagon in displacing radioactive little glucagon from its liver membrane receptor. 8. Big glucagon was equipotent on a molar basis with little glucagon in the stimulation of the mouse islet adenylate cyclase, an indicator of insulinogenic activity. 9. On a molar basis, big glucagon inhibited basal liver adenylate cyclase activity to the same extent that little glucagon stimulated the enzyme. 10. Big glucagon was without effect on blood glucose concentration in the rat in doses up to 5mug/kg. 11. Big glucagon was equipotent, on a molar basis, with little glucagon in stimulating lipolysis in isolated chicken fat-cells.
摘要
  1. 大胰高血糖素存在于牛、狗、大鼠和火鸡的胰腺提取物中,占胰高血糖素免疫反应性的10 - 15%,通过其在分离的鸽胰岛提取物中的存在表明其来源于胰岛。2. 经聚丙烯酰胺凝胶电泳后,大胰高血糖素通过免疫测定呈均一性,且比小胰高血糖素更具电负性。3. 从牛胰腺中纯化出大胰高血糖素,通过凝胶过滤估计其表观分子量为8200±9%。4. 该分子经有限的胰蛋白酶水解产生一种免疫反应性成分,略小于小胰高血糖素。5. 使用肠胰高血糖素交叉反应和“小胰高血糖素羧基末端特异性”抗血清,获得了哺乳动物大胰高血糖素的线性稀释曲线。6. 注入大鼠循环中的大胰高血糖素和小胰高血糖素免疫反应性消失的半衰期分别为6.9分钟和3.2分钟。7. 在从其肝膜受体置换放射性小胰高血糖素方面,大胰高血糖素的效力约为小胰高血糖素的六分之一。8. 在刺激小鼠胰岛腺苷酸环化酶(胰岛素生成活性的指标)方面,大胰高血糖素在摩尔基础上与小胰高血糖素等效。9. 在摩尔基础上,大胰高血糖素抑制基础肝腺苷酸环化酶活性的程度与小胰高血糖素刺激该酶的程度相同。10. 剂量高达5μg/kg时,大胰高血糖素对大鼠血糖浓度无影响。11. 在刺激分离的鸡脂肪细胞中的脂肪分解方面,大胰高血糖素在摩尔基础上与小胰高血糖素等效。

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