Down-regulation of pancreatic transcription factors and incretin receptors in type 2 diabetes 被引量：9

Down-regulation of pancreatic transcription factors and incretin receptors in type 2 diabetes

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摘要 Type 2 diabetes is one of the most prevalent and serious metabolic diseases.Under diabetic conditions,chronic hyperglycemia and subsequent induction of oxidative stress deteriorate pancreaticβ-cell function,which leads to the aggravation of type 2 diabetes.Although such phenomena are well known as glucose toxicity,its molecular mechanism remains unclear.In this review article,we describe the possible molecular mechanism forβ-cell dysfunction found in type 2 diabetes,focusing on(1)oxidative stress,(2)pancreatic transcription factors(PDX-1 and MafA)and(3)incretin receptors(GLP-1 and GIP receptors).Under such conditions,nuclear expression levels of PDX-1 and MafA are decreased,which leads to suppression of insulin biosynthesis and secretion.In addition,expression levels of GLP-1 and GIP receptors are decreased,which likely contributes to the impaired incretin effects found in diabetes.Taken together,it is likely that downregulation of pancreatic transcription factors(PDX-1and MafA)and down-regulation of incretin receptors(GLP-1 and GIP receptors)explain,at least in part,the molecular mechanism forβ-cell dysfunction found in type 2 diabetes. Type 2 diabetes is one of the most prevalent and serious metabolic diseases.Under diabetic conditions,chronic hyperglycemia and subsequent induction of oxidative stress deteriorate pancreaticβ-cell function,which leads to the aggravation of type 2 diabetes.Although such phenomena are well known as glucose toxicity,its molecular mechanism remains unclear.In this review article,we describe the possible molecular mechanism forβ-cell dysfunction found in type 2 diabetes,focusing on(1)oxidative stress,(2)pancreatic transcription factors(PDX-1 and MafA)and(3)incretin receptors(GLP-1 and GIP receptors).Under such conditions,nuclear expression levels of PDX-1 and MafA are decreased,which leads to suppression of insulin biosynthesis and secretion.In addition,expression levels of GLP-1 and GIP receptors are decreased,which likely contributes to the impaired incretin effects found in diabetes.Taken together,it is likely that downregulation of pancreatic transcription factors(PDX-1and MafA)and down-regulation of incretin receptors(GLP-1 and GIP receptors)explain,at least in part,the molecular mechanism forβ-cell dysfunction found in type 2 diabetes.

作者 Hideaki Kaneto Taka-aki Matsuoka

机构地区 Department of Metabolic Medicine

出处《World Journal of Diabetes》 SCIE CAS 2013年第6期263-269,共7页 世界糖尿病杂志（英文版）（电子版）

关键词 Pancreatic &#x003b2 -CELLS Oxidative stress Pancreatic duodenal homeobox-1 MAFA Incretin receptor Pancreatic β-cells Oxidative stress Pancreatic duodenal homeobox-1 MafA Incretin receptor

分类号 R587.1 [医药卫生—内分泌]

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1Satoshi Kawashima,Taka-aki Matsuoka,Hideaki Kaneto,Yoshihiro Tochino,Ken Kato,Kaoru Yamamoto,Tsunehiko Yamamoto,Munehide Matsuhisa,Iichiro Shimomura.Effect of alogliptin, pioglitazone and glargine on pancreatic β-cells in diabetic db/db mice[J]. Biochemical and Biophysical Research Communications . 2010 (1)
2H. Wang,T. Brun,K. Kataoka,A. J. Sharma,C. B. Wollheim.MAFA controls genes implicated in insulin biosynthesis and secretion[J]. Diabetologia . 2007 (2)
3Domenico Accili,Karen C Arden.FoxOs at the Crossroads of Cellular Metabolism, Differentiation, and Transformation[J]. Cell . 2004 (4)
4Koji Sakai,Kazuya Matsumoto,Takeshi Nishikawa,Mihoshi Suefuji,Kazuhiko Nakamaru,Yoshiaki Hirashima,Junji Kawashima,Tetsuya Shirotani,Kenshi Ichinose,Michael Brownlee,Eiichi Araki.Mitochondrial reactive oxygen species reduce insulin secretion by pancreatic β-cells[J]. Biochemical and Biophysical Research Communications . 2003 (1)
5Shin-ichi Gorogawa,Yoshitaka Kajimoto,Yutaka Umayahara,Hideaki Kaneto,Hirotaka Watada,Akio Kuroda,Dan Kawamori,Tetsuyuki Yasuda,Munehide Matsuhisa,Yoshimitsu Yamasaki,Masatsugu Hori.Probucol preserves pancreatic β-cell function through reduction of oxidative stress in type 2 diabetes[J]. Diabetes Research and Clinical Practice . 2002 (1)
6Kataoka, Kohsuke,Han, Song-iee,Shioda, Setsuko,Hirai, Momoki,Nishizawa, Makoto,Handa, Hiroshi.MafA is a glucose-regulated and pancreatic β-cell-specific transcriptional activator for the insulin gene. Journal of Biological Chemistry . 2002
7Carlsson C,Borg LAH,Welsh N.Sodium palmitate induces partial mitochondrial uncoupling and reactive oxygen species in rat pancreatic islets in vitro. The Journal of Endocrinology . 1999
8Joseph Jamie W,Koshkin Vasilij,Saleh Monique C,Sivitz William I,Zhang Chen-Yu,Lowell Bradford B,Chan Catherine B,Wheeler Michael B.Free fatty acid-induced beta-cell defects are dependent on uncoupling protein 2 expression. Journal of Biological Chemistry . 2004
9Oprescu Andrei I,Bikopoulos George,Naassan Anthony,Allister Emma M,Tang Christine,Park Edward,Uchino Hiroshi,Lewis Gary F,Fantus I George,Rozakis-Adcock Maria,Wheeler Michael B,Giacca Adria.Free fatty acid-induced reduction in glucose-stimulated insulin secretion: evidence for a role of oxidative stress in vitro and in vivo. Diabetes . 2007
10Shimabukuro M,Ohneda M,Lee Y,et al.Role of nitric oxide in obesity-induced beta cell disease. Journal of Clinical Investigation, The . 1997

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1Zhi-Wen Yu , Dan Li , Wen-Hua Ling , Tian-Ru Jin.Role of nuclear factor (erythroid-derived 2)-like 2 in metabolic homeostasis and insulin action: A novel opportunity for diabetes treatment?[J].World Journal of Diabetes,2012,3(1):19-28. 被引量：5
2Kai-Ming Yang , Wang Yong , Ai-Dong Li , Hui-Jun Yang.Insulin-producing cells are bi-potential and differentiatorsprior to proliferation in early human development[J].World Journal of Diabetes,2011,2(4):54-58. 被引量：4
3Javier Espino,José A Pariente,Ana B Rodríguez.Role of melatonin on diabetes-related metabolic disorders[J].World Journal of Diabetes,2011,2(6):82-91. 被引量：11
4Brigitte Reusens,Nicolas Theys,Claude Remacle.Alteration of mitochondrial function in adult rat offspring of malnourished dams[J].World Journal of Diabetes,2011,2(9):149-157. 被引量：2
5Hirofumi Noguchi.Pancreatic islet transplantation[J].World Journal of Gastrointestinal Surgery,2009,1(1):16-20. 被引量：7
6Hirofumi Noguchi.Recent advances in stem cell research for the treatment of diabetes[J].World Journal of Stem Cells,2009,1(1):36-42.
7Zahra Niki Boroujeni,Ahmad Aleyasin.Insulin producing cells established using non-integrated lentiviral vector harboring PDX1 gene[J].World Journal of Stem Cells,2013,5(4):217-228. 被引量：3
8Yang, Chuang,Wang, Ji-Ming,Du, Cheng-You,Xue, Dong.Expression of stem cell markers CK-19 and PDX-1mRNA in pancreatic islet samples of different purity from rats[J].Hepatobiliary & Pancreatic Diseases International,2007,6(5):544-548. 被引量：3

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