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Mechanistic understanding of insulin receptor modulation: Implications for the development of anti-diabetic drugs SCIE SCOPUS

Title
Mechanistic understanding of insulin receptor modulation: Implications for the development of anti-diabetic drugs
Authors
Na-Oh YunnJaeyoon KimYoundong KimIngo LeibigerPer-Olof BerggrenRYU, SUNG HO
Date Issued
2018-05
Publisher
PERGAMON-ELSEVIER SCIENCE LTD
Abstract
The insulin receptor is an important regulator of metabolic processes in the body, and in particular of glucose homeostasis, including glucose uptake into peripheral tissues. Thus, insulin administration is an effective treatment for diabetes, which is characterized by chronic elevation of blood glucose. However, insulin is not only a metabolic regulator, but also functions as a growth hormone. Accordingly, studies of long-term insulin administration and of the hyperinsulinemia associated with type 2 diabetes have raised concerns about possible increases in the risks of cancer and atherosclerosis, due to excessive stimulation of cell proliferation. Interestingly, some insulin receptor ligands that have been developed based on a peptide, an antibody, and an aptamer selectively have metabolic effects exerted through the insulin receptor but do not cause significant cellular proliferation. Although these ligands therefore have potential as anti-diabetic drugs for advanced diabetes care, the mechanism whereby they specifically activate the insulin receptor is still unclear. Recently, studies of the structure of the insulin receptor have progressed considerably, and have provided further mechanistic understanding of insulin receptor activation. Based on this progress, we propose a mechanistic model of this specificity and discuss the potential for the development of novel anti-diabetic drugs that would not have the adverse effects caused by excessive mitogenic action.
Keywords
antidiabetic agent; aptamer; insulin; insulin derivative; insulin receptor; insulin receptor antibody; peptide derivative; allosteric site; antidiabetic activity; cancer risk; carboxy terminal sequence; cardiovascular disease; cardiovascular risk; cell growth; complex formation; diabetes mellitus; diabetic complication; dimerization; drug binding site; human; hyperinsulinemia; insulin binding; insulin treatment; malignant neoplasm; mitogenesis; nonhuman; priority journal; protein function; receptor binding; Review
URI
https://oasis.postech.ac.kr/handle/2014.oak/50111
DOI
10.1016/j.pharmthera.2017.12.005
ISSN
0163-7258
Article Type
Article
Citation
PHARMACOLOGY & THERAPEUTICS, vol. 185, page. 86 - 98, 2018-05
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류성호RYU, SUNG HO
Dept of Life Sciences
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