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Ampks6k1 Signaling Pathway As A Target For Treating Hepatic Insulin Resistance 1st Edition Sang Geon Kim Je Cho Hee Yeon Kay

  • SKU: BELL-51356408
Ampks6k1 Signaling Pathway As A Target For Treating Hepatic Insulin Resistance 1st Edition Sang Geon Kim Je Cho Hee Yeon Kay
$ 31.00 $ 45.00 (-31%)

4.1

10 reviews

Ampks6k1 Signaling Pathway As A Target For Treating Hepatic Insulin Resistance 1st Edition Sang Geon Kim Je Cho Hee Yeon Kay instant download after payment.

Publisher: Nova Science Publishers, Incorporated
File Extension: PDF
File size: 2.6 MB
Pages: 69
Author: Sang Geon Kim; Je Cho; Hee Yeon Kay
ISBN: 9781617614576, 1617614572
Language: English
Year: 2010
Edition: 1

Product desciption

Ampks6k1 Signaling Pathway As A Target For Treating Hepatic Insulin Resistance 1st Edition Sang Geon Kim Je Cho Hee Yeon Kay by Sang Geon Kim; Je Cho; Hee Yeon Kay 9781617614576, 1617614572 instant download after payment.

Hepatic insulin resistance and altered insulin metabolism, as characterized by the desensitization of hepatic parenchymal cells to insulin, play a role in the pathogenesis of liver disease, particularly resulting in steatosis and steatohepatitis. By the same token, type II diabetic patients are at higher risk for developing liver diseases, including steatosis, hepatitis, cirrhosis, and hepatocellular carcinoma. On the other hand, established liver disease from any cause leads to glucose intolerance and peripheral insulin resistance systemically. The link between insulin resistance and liver pathology reviewed in this book suggests that insulin resistance is closely related with a variety of liver diseases. Recent evidence indicates that the AMP activating protein kinase (AMPK) in conjunction with p70 ribosomal S6 kinase 1 (S6K1) serves as a key signaling pathway regulating insulin-dependent physiological functions; thus, this pathway serves as a target for the therapy of diseases associated with insulin resistance. In this chapter, the regulatory role of the AMPK-S6K1 pathway is discussed in terms of enhancing insulin receptor signaling with insulin receptor substrate-1/2 and phosphatidylinositol phosphate kinase activity, which may contribute to preventing and/or treating insulin resistance in the liver.

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