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Titlebook: Glucagon I; Pierre J. Lefèbvre (Professor of Medicine, Guest P Book 1983 Springer-Verlag Berlin Heidelberg 1983 Drogen.Glucagon.Hormone.Hy

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https://doi.org/10.1007/978-3-322-89477-9ume by B. (Chap. 1) and B. (Chap. 3) respectively. As emphasized by B. (Chap. 1), the primary structures of porcine, bovine, and human glucagon are identical, but different primary structures have been reported for guinea pig, avian, and piscine glucagons. The present chapter will summarize the prod
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Johannes Brombach,Michael Leisganguent refinement of this tool has enabled major strides to be made in describing the sources and functions of an array of substances related to glucagon and interpreting their roles in fuel homeostasis. It is now clear that glucagon is not only synthesized and released from the pancreatic A-cell, but
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https://doi.org/10.1007/978-3-658-13969-8ome of these forms, as in the case of many other polypeptide hormones, may be related to glucagon biosynthesis (see Chaps. 6 and 7). At present, it is not clearly established whether the glucagon heterogeneity found in plasma is merely a reflection of that found in pancreatic or extrapancreatic tiss
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Einführung von Lean Six Sigma bei Xeroxjor site of gluconeogenesis, although the kidney becomes important during prolonged starvation. The most important function of gluconeogenesis is the maintenance of blood glucose levels during times when food intake is restricted and/or glycogen stores are depleted. For example, the rate of gluconeo
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Chemical Characteristics of GlucagonThe object of this chapter is to describe the covalent chemistry of pancreatic glucagon to provide a background for subsequent chapters. Modifications of the primary structure are considered with respect to biologic activity, but not immunologic activity which is discussed in Chap. 9. Conformation and function are considered in Chap. 3.
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