Receptor binding and biological activity of [SerB24]-insulin, an abnormal mutant insulin |
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Authors: | M Kobayashi M Haneda H Maegawa N Watanabe Y Takada Y Shigeta K Inouye |
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Affiliation: | 1. Third Department of Medicine, Shiga University of Medical Science, Ohtsu, Japan;2. Shionogi Research Laboratories, Osaka, Japan |
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Abstract: | [SerB24]-insulin, the second structurally abnormal mutant insulin, and [SerB25]-insulin were semisynthesized and were studied for receptor binding and biological activity. Receptor binding and biological activity determined by its ability to increase 2-deoxy-glucose uptake in rat adipocytes were 0.7-3% of native insulin for [SerB24]-insulin and 3-8% for [SerB25]-insulin. Negative cooperative effect of these analogues was also markedly decreased. Immunoreactivity of [SerB24]-insulin was decreased whereas that of [SerB25]-insulin was normal. Markedly decreased receptor binding of [SerB24]-insulin appeared to be due to substitution of hydrophobic amino acid, Phe, with a polar amino acid, Ser, at B24. |
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