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Labeling of glucagon binding components in hepatocyte plasma membranes.
Authors:M D Bregman  D Levy
Affiliation:Department of Biochemistry University of Southern California School of Medicine Los Angeles, California 90033 USA
Abstract:
A photosensitive derivative of glucagon, 125I-N?-4-azido-2-nitrophenyl-glucagon, has been synthesized and used to specifically label glucagon binding proteins in hepatocyte plasma membranes. Photolysis of the derivative in the presence of a membrane suspension results in the incorporation of radioactivity primarily into membrane components with a molecular weight range of 23,000–25,000. The binding properties of the derivative are essentially identical to that observed for glucagon. The binding of 125I-NAP-glucagon was completely inhibited in the presence of glucagon (3 μM) while greater than 90% of the covalent labeling was also inhibited in the presence of glucagon. These studies suggest that the labeled membrane protein may be a component of the glucagon receptor.
Keywords:NAP-glucagon  To whom correspondence should be directed.
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