Your search keyword '"Araki, E."' showing total 45 results

1. Efficacy, Safety, and Tolerability of Oral Semaglutide Versus Placebo Added to Insulin With or Without Metformin in Patients With Type 2 Diabetes: The PIONEER 8 Trial.

Author

Zinman B, Aroda VR, Buse JB, Cariou B, Harris SB, Hoff ST, Pedersen KB, Tarp-Johansen MJ, and Araki E

Subjects

Adult, Body Weight drug effects, Diabetes Mellitus, Type 2 blood, Double-Blind Method, Drug Therapy, Combination, Female, Glycated Hemoglobin drug effects, Humans, Male, Middle Aged, Nausea chemically induced, Treatment Outcome, Weight Loss drug effects, Diabetes Mellitus, Type 2 drug therapy, Glucagon-Like Peptides administration & dosage, Hypoglycemic Agents administration & dosage, Insulin administration & dosage, Metformin administration & dosage

Abstract

Objective: To investigate the efficacy, safety, and tolerability of oral semaglutide added to insulin with or without metformin., Research Design and Methods: Patients with type 2 diabetes uncontrolled on insulin with or without metformin were randomized to oral semaglutide 3 mg ( N = 184), 7 mg ( N = 182), or 14 mg ( N = 181) or to placebo ( N = 184) in a 52-week, double-blind trial. End points were change from baseline to week 26 in HbA 1c (primary) and body weight (confirmatory secondary). Two estimands were defined: treatment policy (effect regardless of trial product discontinuation or rescue medication) and trial product (effect assuming trial product continuation without rescue medication) in randomized patients., Results: Oral semaglutide was superior to placebo in reducing HbA 1c (estimated treatment difference [ETD] -0.5% [95% CI -0.7, -0.3], -0.9% [-1.1, -0.7], and -1.2% [-1.4, -1.0] for 3, 7, and 14 mg, respectively; P < 0.001) and body weight (ETD -0.9 kg [95% CI -1.8, -0.0], -2.0 kg [-3.0, -1.0], and -3.3 kg [-4.2, -2.3]; P = 0.0392 for 3 mg, P ≤ 0.0001 for 7 and 14 mg) at week 26 (treatment policy estimand). Significantly greater dose-dependent HbA 1c and body weight reductions versus placebo were achieved with oral semaglutide at weeks 26 and 52 (both estimands). The most frequent adverse event with oral semaglutide was nausea (11.4-23.2% of patients vs. 7.1% with placebo; mostly mild to moderate)., Conclusions: Oral semaglutide was superior to placebo in reducing HbA 1c and body weight when added to insulin with or without metformin in patients with type 2 diabetes. The safety profile was consistent with other glucagon-like peptide 1 receptor agonists., (© 2019 by the American Diabetes Association.)

Published

2019

2. FoxK1 and FoxK2 in insulin regulation of cellular and mitochondrial metabolism.

Author

Sakaguchi M, Cai W, Wang CH, Cederquist CT, Damasio M, Homan EP, Batista T, Ramirez AK, Gupta MK, Steger M, Wewer Albrechtsen NJ, Singh SK, Araki E, Mann M, Enerbäck S, and Kahn CR

Subjects

Animals, Cell Line, Cell Proliferation, Cell Survival, Forkhead Transcription Factors metabolism, Glycogen Synthase Kinase 3 metabolism, Humans, Mice, Signal Transduction, TOR Serine-Threonine Kinases metabolism, Forkhead Transcription Factors physiology, Insulin metabolism, Mitochondria metabolism

Abstract

A major target of insulin signaling is the FoxO family of Forkhead transcription factors, which translocate from the nucleus to the cytoplasm following insulin-stimulated phosphorylation. Here we show that the Forkhead transcription factors FoxK1 and FoxK2 are also downstream targets of insulin action, but that following insulin stimulation, they translocate from the cytoplasm to nucleus, reciprocal to the translocation of FoxO1. FoxK1/FoxK2 translocation to the nucleus is dependent on the Akt-mTOR pathway, while its localization to the cytoplasm in the basal state is dependent on GSK3. Knockdown of FoxK1 and FoxK2 in liver cells results in upregulation of genes related to apoptosis and down-regulation of genes involved in cell cycle and lipid metabolism. This is associated with decreased cell proliferation and altered mitochondrial fatty acid metabolism. Thus, FoxK1/K2 are reciprocally regulated to FoxO1 following insulin stimulation and play a critical role in the control of apoptosis, metabolism and mitochondrial function.

Published

2019

3. Pharmacokinetics and pharmacodynamics of dapagliflozin in combination with insulin in Japanese patients with type 1 diabetes.

Author

Watada H, Shiramoto M, Ueda S, Tang W, Asano M, Thorén F, Kim H, Yajima T, Boulton DW, and Araki E

Subjects

Adult, Benzhydryl Compounds pharmacology, Dose-Response Relationship, Drug, Drug Therapy, Combination, Female, Glucosides pharmacology, Glucuronides blood, Glycosuria urine, Humans, Japan, Male, Middle Aged, Sodium-Glucose Transporter 2 Inhibitors pharmacology, Benzhydryl Compounds pharmacokinetics, Diabetes Mellitus, Type 1 drug therapy, Glucosides pharmacokinetics, Hypoglycemic Agents therapeutic use, Insulin therapeutic use, Sodium-Glucose Transporter 2 Inhibitors pharmacokinetics

Abstract

Aims: To assess the pharmacokinetics/pharmacodynamics (PK/PD) of dapagliflozin, a sodium-glucose co-transporter 2 inhibitor that increases urinary glucose excretion (UGE) and its major metabolite, dapagliflozin-3-O-glucuronide (D3OG), in Japanese patients with type 1 diabetes (T1D) and inadequate glycaemic control (HbA1c 7%-10%)., Materials and Methods: Japanese patients (18-65 years) with inadequately controlled T1D were randomized 1:1:1 to dapagliflozin 5 mg, 10 mg or placebo (n = 14 each) once daily for 7 days, with adjustable insulin. The PK/PD characteristics of dapagliflozin and D3OG were assessed on Day 7. Patients underwent follow-up evaluation on Days 8 and 14. Adverse events (AEs), hypoglycaemic episodes and events of diabetic ketoacidosis (DKA) were recorded over the treatment and follow-up periods., Results: A total of 42 randomized patients received dapagliflozin or placebo. PK variables increased in a dose-dependent manner. D3OG was generated rapidly, with a median time to maximum plasma concentration of 2.0 hours (1.0-3.0). The dapagliflozin dose-UGE relationship was attenuated, with larger insulin dose reductions than anticipated. Mean percent (standard error) changes in total daily insulin dose from baseline to Day 7 were - 36.86% (3.32), -39.13% (2.68) and - 4.97% (5.28) for dapagliflozin 5 mg and 10 mg and for placebo, respectively. No DKA was reported. AEs were consistent with the established dapagliflozin safety profile. There was no increase in hypoglycaemia., Conclusions: The PK and safety profiles of dapagliflozin in Japanese patients with T1D were consistent with previous studies, but with an unanticipated attenuation of the PD dose-response measured as UGE., (© 2018 The Authors. Diabetes, Obesity and Metabolism published by John Wiley & Sons Ltd.)

Published

2019

4. Impact of hepatic HSP72 on insulin signaling.

Author

Kitano S, Kondo T, Matsuyama R, Ono K, Goto R, Takaki Y, Hanatani S, Sakaguchi M, Igata M, Kawashima J, Motoshima H, Matsumura T, Kai H, and Araki E

Subjects

Animals, Diet, High-Fat, Endoplasmic Reticulum Stress genetics, Glucose metabolism, Insulin Resistance genetics, Insulin Secretion genetics, Mice, Mice, Knockout, Signal Transduction, Adipose Tissue, White metabolism, Diabetes Mellitus, Type 2 metabolism, Gluconeogenesis genetics, HSP72 Heat-Shock Proteins genetics, Insulin metabolism, Insulin-Secreting Cells metabolism, Liver metabolism

Abstract

Heat shock protein 72 (HSP72) is a major inducible molecule in the heat shock response that enhances intracellular stress tolerance. Decreased expression of HSP72 is observed in type 2 diabetes, which may contribute to the development of insulin resistance and chronic inflammation. We used HSP72 knockout (HSP72-KO) mice to investigate the impact of HSP72 on glucose metabolism and endoplasmic reticulum (ER) stress, particularly in the liver. Under a high-fat diet (HFD) condition, HSP72-KO mice showed glucose intolerance, insulin resistance, impaired insulin secretion, and enhanced hepatic gluconeogenic activity. Furthermore, activity of the c-Jun NH 2 -terminal kinase (JNK) was increased and insulin signaling suppressed in the liver. Liver-specific expression of HSP72 by lentivirus (lenti) in HFD-fed HSP72-KO mice ameliorated insulin resistance and hepatic gluconeogenic activity. Furthermore, increased adipocyte size and hepatic steatosis induced by the HFD were suppressed in HSP72-KO lenti-HSP72 mice. Increased JNK activity and ER stress upon HFD were suppressed in the liver as well as the white adipose tissue of HSP72-KO lenti-HSP72 mice. Thus, HSP72 KO caused a deterioration in glucose metabolism, hepatic gluconeogenic activity, and β-cell function. Moreover, liver-specific recovery of HSP72 restored glucose homeostasis. Therefore, hepatic HSP72 may play a critical role in the pathogenesis of type 2 diabetes.

Published

2019

5. One-hour oral glucose tolerance test plasma glucose at gestational diabetes diagnosis is a common predictor of the need for insulin therapy in pregnancy and postpartum impaired glucose tolerance.

Author

Nishikawa T, Ono K, Hashimoto S, Kinoshita H, Watanabe T, Araki H, Otsu K, Sakamoto W, Harada M, Toyonaga T, Kawakami S, Fukuda J, Haga Y, Kukidome D, Takahashi T, and Araki E

Subjects

Adult, Blood Glucose analysis, Female, Gestational Age, Glucose Intolerance complications, Humans, Japan, Postpartum Period, Pregnancy, Retrospective Studies, Risk Factors, Diabetes, Gestational diagnosis, Diabetes, Gestational drug therapy, Glucose Intolerance diagnosis, Glucose Intolerance drug therapy, Glucose Tolerance Test methods, Hypoglycemic Agents therapeutic use, Insulin therapeutic use

Abstract

Aims/introduction: Gestational diabetes mellitus (GDM) is a risk for adverse perinatal outcomes, and patients with a history of GDM have an increased risk of impaired glucose tolerance (IGT). Here, we carried out two non-interventional and retrospective studies of GDM patients in Japan., Materials and Methods: In the first study, we enrolled 529 GDM patients and assessed predictors of the need for insulin therapy. In the second study, we enrolled 185 patients from the first study, and assessed predictors of postpartum IGT., Results: In the first study, gestational weeks at GDM diagnosis and history of pregnancy were significantly lower, and pregestational body mass index, family history of diabetes mellitus, 1- and 2-h glucose levels in a 75-g oral glucose tolerance test (OGTT), the number of abnormal values in a 75-g OGTT, and glycated hemoglobin were significantly higher in participants receiving insulin therapy. In the second study, 1- and 2-h glucose levels in a 75-g OGTT, the number of abnormal values in a 75-g OGTT, glycated hemoglobin, and ketone bodies in a urine test were significantly higher in participants with OGT. Logistic regression analysis showed that gestational weeks at GDM diagnosis, 1-h glucose levels in a 75-g OGTT and glycated hemoglobin were significant predictors of the need for insulin therapy, and 1-h glucose levels in a 75-g OGTT at diagnosis and ketone bodies in a urine test were significant predictors for postpartum IGT., Conclusions: Antepartum 1-h glucose levels in a 75-g OGTT was a predictor of the need for insulin therapy in pregnancy and postpartum IGT., (© 2018 The Authors. Journal of Diabetes Investigation published by Asian Association for the Study of Diabetes (AASD).)

Published

2018

6. Semaglutide Added to Basal Insulin in Type 2 Diabetes (SUSTAIN 5): A Randomized, Controlled Trial.

Author

Rodbard HW, Lingvay I, Reed J, de la Rosa R, Rose L, Sugimoto D, Araki E, Chu PL, Wijayasinghe N, and Norwood P

Subjects

Adult, Aged, Aged, 80 and over, Blood Glucose, Diabetes Mellitus, Type 2 blood, Double-Blind Method, Drug Therapy, Combination, Female, Humans, Male, Middle Aged, Treatment Outcome, Young Adult, Diabetes Mellitus, Type 2 drug therapy, Glucagon-Like Peptides therapeutic use, Glycated Hemoglobin analysis, Hypoglycemic Agents therapeutic use, Insulin therapeutic use

Abstract

Context: Combination therapy with insulin and glucagon-like peptide-1 receptor agonists (GLP-1RAs) is important for treating type 2 diabetes (T2D). This trial assesses the efficacy and safety of semaglutide, a GLP-1RA, as an add-on to basal insulin., Objective: To demonstrate the superiority of semaglutide vs placebo on glycemic control as an add-on to basal insulin in patients with T2D., Design: Phase 3a, double-blind, placebo-controlled, 30-week trial., Setting: This study included 90 sites in five countries., Patients: We studied 397 patients with uncontrolled T2D receiving stable therapy with basal insulin with or without metformin., Interventions: Subcutaneous semaglutide 0.5 or 1.0 mg once weekly or volume-matched placebo., Main Outcome Measures: Primary endpoint was change in glycated Hb (HbA1c) from baseline to week 30. Confirmatory secondary endpoint was change in body weight from baseline to week 30., Results: At week 30, mean HbA1c reductions [mean baseline value, 8.4% (67.9 mmol/mol)] with semaglutide 0.5 and 1.0 mg were 1.4% (15.8 mmol/mol) and 1.8% (20.2 mmol/mol) vs 0.1% (1.0 mmol/mol) with placebo [estimated treatment difference (ETD) vs placebo, -1.35 (14.8 mmol/mol); 95% CI, -1.61 to -1.10 and ETD, -1.75% (19.2 mmol/mol); 95% CI, -2.01 to -1.50; both P < 0.0001]. Severe or blood glucose-confirmed hypoglycemic episodes were reported in 11 patients (17 events) and 14 patients (25 events) with semaglutide 0.5 and 1.0 mg, respectively, vs seven patients (13 events) with placebo (estimated rate ratio vs placebo, 2.08; 95% CI, 0.67 to 6.51 and estimated rate ratio vs placebo, 2.41; 95% CI, 0.84 to 6.96 for 0.5 and 1.0 mg; both P = nonsignificant). Mean body weight decreased with semaglutide 0.5 and 1.0 mg vs placebo from baseline to end of treatment: 3.7, 6.4, and 1.4 kg (ETD, -2.31; 95% CI, -3.33 to -1.29 and ETD, -5.06; 95% CI, -6.08 to -4.04 kg; both P < 0.0001). Premature treatment discontinuation due to adverse events was higher for semaglutide 0.5 and 1.0 mg vs placebo (4.5%, 6.1%, and 0.8%), mainly due to gastrointestinal disorders., Conclusions: Semaglutide, added to basal insulin, significantly reduced HbA1c and body weight in patients with uncontrolled T2D vs placebo.

Published

2018

7. Efficacy and safety of dapagliflozin over 1 year as add-on to insulin therapy in Japanese patients with type 2 diabetes: the DAISY (Dapagliflozin Added to patients under InSulin therapY) trial.

Author

Araki E, Onishi Y, Asano M, Kim H, and Yajima T

Subjects

Adult, Benzhydryl Compounds adverse effects, Blood Glucose drug effects, Diabetes Mellitus, Type 2 blood, Double-Blind Method, Drug Therapy, Combination, Female, Glucosides adverse effects, Glycated Hemoglobin drug effects, Humans, Hypoglycemia chemically induced, Hypoglycemia epidemiology, Hypoglycemic Agents adverse effects, Japan epidemiology, Male, Time Factors, Treatment Outcome, Benzhydryl Compounds administration & dosage, Diabetes Mellitus, Type 2 drug therapy, Glucosides administration & dosage, Hypoglycemic Agents administration & dosage, Insulin administration & dosage

Abstract

Aims: To evaluate the efficacy and safety of dapagliflozin as add-on to insulin in Japanese patients with type 2 diabetes., Materials and Methods: Insulin-treated Japanese patients were randomized to 5 mg dapagliflozin or placebo during a 16-week double-blind treatment period. Both groups then received dapagliflozin 5 or 10 mg (the dose was increased at or after week 24 if glycated haemoglobin [HbA1c] at the previous visit was >7.5%) during a 36-week open-label extension period. The exploratory efficacy endpoint was to assess the maintenance efficacy of 5/10 mg dapagliflozin + insulin over 52 weeks of treatment. Safety was assessed in terms of adverse events, laboratory variables and vital signs., Results: The changes in HbA1c from baseline to weeks 16 and 52 were -0.62% and -0.74%, respectively, in the dapagliflozin group, vs -0.08% and -0.83%, respectively, in the placebo-dapagliflozin group. Body weight decreased at both time points in the dapagliflozin group and after switching to open-label dapagliflozin in the placebo-dapagliflozin group. The total insulin dose decreased slightly after starting dapagliflozin. Adverse events occurred in 82.9% and 71.7% of patients in the dapagliflozin and placebo-dapagliflozin groups, respectively. Hypoglycaemia occurred in 35.0% and 41.7% of patients in the dapagliflozin and placebo-dapagliflozin groups, respectively, but the incidence was not increased by use of dapagliflozin in either trial period. Genital/urinary tract infections, renal impairment/failure, volume depletion, fracture and hepatic disorders occurred in ≤5% of patients., Conclusion: This trial showed that administration of dapagliflozin as an add-on to insulin therapy was effective, was well tolerated and had insulin-sparing effects in Japanese patients with type 2 diabetes., (© 2016 John Wiley & Sons Ltd.)

Published

2017

8. Efficacy and safety of dapagliflozin in addition to insulin therapy in Japanese patients with type 2 diabetes: Results of the interim analysis of 16-week double-blind treatment period.

Author

Araki E, Onishi Y, Asano M, Kim H, Ekholm E, Johnsson E, and Yajima T

Subjects

Aged, Asian People, Benzhydryl Compounds adverse effects, Blood Glucose drug effects, Body Weight drug effects, Diabetes Mellitus, Type 2 metabolism, Double-Blind Method, Drug Therapy, Combination, Female, Glucosides adverse effects, Glycated Hemoglobin analysis, Humans, Hypoglycemic Agents adverse effects, Insulin adverse effects, Japan, Male, Middle Aged, Treatment Outcome, Benzhydryl Compounds therapeutic use, Diabetes Mellitus, Type 2 drug therapy, Glucosides therapeutic use, Hypoglycemic Agents therapeutic use, Insulin therapeutic use

Abstract

Introduction: Dapagliflozin treatment when added to insulin therapy in Japanese patients with type 2 diabetes remains to be evaluated., Materials and Methods: This was a multicenter, randomized, double-blind, parallel-group, placebo-controlled study to evaluate efficacy (at 16 weeks) and long-term safety (at 52 weeks) of dapagliflozin in addition to insulin therapy. The interim analysis was carried out at week 16 to assess the efficacy and safety profiles. The patients receiving insulin (n = 182) were randomized to either dapagliflozin 5 mg or a placebo at a 2:1 ratio. The primary efficacy end-point was the change in hemoglobin A1c (HbA1c) from baseline at week 16., Results: Patients in the dapagliflozin group showed an adjusted decrease in HbA1c of -0.55% from baseline, whereas the placebo showed a marginal increase of 0.05%. The placebo-corrected mean change of HbA1c from baseline to week 16 in dapagliflozin was -0.60% (P < 0.0001). In addition, the placebo-corrected mean change of fasting plasma glucose and bodyweight from baseline to week 16 in the dapagliflozin group was -22.7 mg/dL (P < 0.0001) and -1.21 kg (P < 0.0001), respectively. The placebo-corrected mean daily insulin dose in the dapagliflozin group was numerically decreased (treatment difference: -0.72 IU/day; P = 0.0743). No major episodes or discontinuations as a result of hypoglycemia were reported during the study period., Conclusions: Dapagliflozin used as add-on treatment to insulin therapy showed significantly greater reduction of HbA1c, fasting plasma glucose and bodyweight without severe hypoglycemia compared with the placebo at week 16. These results show the clinical benefit of prescribing dapagliflozin for Japanese patients with insufficient glycemic control even with insulin therapy., (© 2015 The Authors. Journal of Diabetes Investigation published by Asian Association for the Study of Diabetes (AASD) and John Wiley & Sons Australia, Ltd.)

Published

2016

9. Effects of combination therapy with vildagliptin and valsartan in a mouse model of type 2 diabetes.

Author

Miyagawa K, Kondo T, Goto R, Matsuyama R, Ono K, Kitano S, Kawasaki S, Igata M, Kawashima J, Matsumura T, Motoshima H, and Araki E

Subjects

Adamantane pharmacology, Adamantane therapeutic use, Adiponectin metabolism, Angiotensin II Type 1 Receptor Blockers therapeutic use, Animals, Blood Glucose metabolism, Cytokines drug effects, Dipeptidyl-Peptidase IV Inhibitors therapeutic use, Disease Models, Animal, Drug Therapy, Combination, Fatty Liver, Homeodomain Proteins drug effects, Homeodomain Proteins metabolism, Inflammation, Insulin Resistance, Insulin Secretion, Mice, Mice, Inbred C57BL, Nitriles therapeutic use, Phlorhizin pharmacology, Pyrrolidines therapeutic use, Tetrazoles therapeutic use, Trans-Activators drug effects, Trans-Activators metabolism, Valine pharmacology, Valine therapeutic use, Valsartan, Vildagliptin, Adamantane analogs & derivatives, Angiotensin II Type 1 Receptor Blockers pharmacology, Blood Glucose drug effects, Diabetes Mellitus, Experimental drug therapy, Diabetes Mellitus, Type 2 drug therapy, Dipeptidyl-Peptidase IV Inhibitors pharmacology, Insulin metabolism, Insulin-Secreting Cells drug effects, Nitriles pharmacology, Pyrrolidines pharmacology, Tetrazoles pharmacology, Valine analogs & derivatives

Abstract

Background: Dipeptidyl peptidase-4 (DPP-4) inhibitors modulate incretin hormones and exert anti-diabetic effects in type 2 diabetes mellitus. Treatment with angiotensin II type 1 receptor blockers (ARB) is a proven successful intervention for hypertension with type 2 diabetes. The present study investigated the combined effects of the DPP-4 inhibitor vildagliptin and the ARB valsartan in a mouse model of type 2 diabetes., Methods: C57BL/6 J mice fed with high-fat diet (HFD) or db/db mice were treated with placebo, phloridzin (PHZ), vildagliptin alone (ViL), valsartan alone (VaL) or ViL with VaL (ViLVaL) for 8 weeks., Results: Glucose metabolism was improved in response to PHZ, ViL and ViLVaL in both HFD and db/db mice. Upon glucose challenge, ViLVaL showed the greatest suppression of blood glucose excursions, with increased insulin secretion, in db/db mice. ViLVaL treatment also showed an improvement of insulin sensitivity in db/db mice. Serum inflammatory cytokines were significantly decreased, and adiponectin was highest, in the ViLVaL group. ViLVaL improved insulin signaling and attenuated stress signaling in liver with amelioration of hepatic steatosis due to activated fatty acid oxidation in db/db mice. Furthermore, immunohistochemical analysis of the pancreas revealed that the combination treatment resulted in an increased expression of insulin and PDX-1, and increased insulin content., Conclusions: The combination therapy of ViL and VaL improves both pancreatic beta-cell function and insulin sensitivity, with a reduction of the inflammatory and cell stress milieu in mouse models of T2DM. Our results suggest that this combination therapy exerts additive or even synergistic benefits to treat T2DM.

Published

2013

10. The impact of Ca²⁺/calmodulin-dependent protein kinase II on insulin gene expression in MIN6 cells.

Author

Suefuji M, Furukawa N, Matsumoto K, Oiso H, Shimoda S, Yoshinaga T, Matsuyama R, Miyagawa K, Kondo T, Kawashima J, Tsuruzoe K, and Araki E

Subjects

Animals, Calcium-Calmodulin-Dependent Protein Kinase Type 2 genetics, Cell Line, Tumor, Cyclic AMP Response Element-Binding Protein genetics, Down-Regulation, Gene Knockdown Techniques, Mice, Phosphorylation, Promoter Regions, Genetic, Serine genetics, Serine metabolism, CREB-Binding Protein metabolism, Calcium-Calmodulin-Dependent Protein Kinase Type 2 metabolism, Cyclic AMP Response Element-Binding Protein metabolism, Gene Expression Regulation, Insulin genetics

Abstract

Ca(2+)/calmodulin-dependent protein kinase II (CaMKII) is expressed in insulin-secreting β cells. However, the effects of CaMKII on insulin synthesis are unknown. Although Ser133 phosphorylation of cyclic AMP-responsive element-binding protein (CREB) typically increases CREB transcriptional activity, CaMKII phosphorylates CREB at Ser142 and at Ser133 to exert a dominant inhibitory effect. Our objective was to characterize the role of CaMKII in insulin gene expression. In MIN6 cells, insulin gene promoter activity was significantly down-regulated by wild-type (WT) CaMKIIδ2, but was significantly upregulated after small interfering RNA (siRNA) knockdown of CaMKIIδ expression. These results were independent of glucose concentrations and membrane depolarization. Insulin mRNA levels were also decreased by WT CaMKIIδ2 and increased by CaMKIIδ siRNA. Downregulation of insulin gene promoter activity by WT CaMKIIδ2 was partly mediated via cyclic AMP-responsive element 2 (CRE2). WT CaMKIIδ2 significantly increased CREB phosphorylation at Ser142 and significantly decreased binding to CREB binding protein (CBP), whereas kinase dead CaMKIIδ2 did not. Our results indicate that CaMKIIδ2 downregulates insulin gene expression by Ser142 phosphorylation of CREB and reducing binding of CREB to CBP., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

11. Voltage-gated K+ channel KCNQ1 regulates insulin secretion in MIN6 β-cell line.

Author

Yamagata K, Senokuchi T, Lu M, Takemoto M, Fazlul Karim M, Go C, Sato Y, Hatta M, Yoshizawa T, Araki E, Miyazaki J, and Song WJ

Subjects

Animals, Cell Line, Glucagon-Like Peptide 1 metabolism, Insulin Secretion, KCNQ1 Potassium Channel genetics, Mice, Mice, Inbred C57BL, Retroviridae, Transfection, Insulin metabolism, Insulin-Secreting Cells metabolism, KCNQ1 Potassium Channel metabolism

Abstract

KCNQ1, located on 11p15.5, encodes a voltage-gated K(+) channel with six transmembrane regions, and loss-of-function mutations in the KCNQ1 gene cause hereditary long QT syndrome. Recent genetic studies have identified that single nucleotide polymorphisms located in intron 15 of the KCNQ1 gene are strongly associated with type 2 diabetes and impaired insulin secretion. In order to understand the role of KCNQ1 in insulin secretion, we introduced KCNQ1 into the MIN6 mouse β-cell line using a retrovirus-mediated gene transfer system. In KCNQ1 transferred MIN6 cells, both the density of the KCNQ1 current and the density of the total K(+) current were significantly increased. In addition, insulin secretion by glucose, pyruvate, or tolbutamide was significantly impaired by KCNQ1-overexpressing MIN6 cells. These results suggest that increased KCNQ1 protein expression limits insulin secretion from pancreatic β-cells by regulating the potassium channel current., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

12. CHOP deletion does not impact the development of diabetes but suppresses the early production of insulin autoantibody in the NOD mouse.

Author

Satoh T, Abiru N, Kobayashi M, Zhou H, Nakamura K, Kuriya G, Nakamura H, Nagayama Y, Kawasaki E, Yamasaki H, Yu L, Eisenbarth GS, Araki E, Mori M, Oyadomari S, and Eguchi K

Subjects

Adoptive Transfer, Animals, Apoptosis, Autoantibodies immunology, CD8-Positive T-Lymphocytes immunology, Endoplasmic Reticulum genetics, Endoplasmic Reticulum pathology, Gene Expression Regulation, In Situ Nick-End Labeling, Insulin-Secreting Cells metabolism, Insulin-Secreting Cells pathology, Lymphocyte Depletion, Mice, Mice, Inbred NOD, Peroxidase metabolism, Spleen immunology, Stress, Physiological genetics, Transcription Factor CHOP metabolism, Autoantibodies biosynthesis, Gene Deletion, Insulin immunology, Prediabetic State immunology, Prediabetic State pathology, Transcription Factor CHOP genetics

Abstract

C/EBP homologous protein (CHOP) has been proposed as a key transcription factor for endoplasmic reticulum (ER) stress-mediated β-cell death induced by inflammatory cytokines in vitro. However, the contribution of CHOP induction to the pathogenesis of type 1 diabetes is not yet clear. To evaluate the relevance of CHOP in the pathogenesis of type 1 diabetes in vivo, we generated CHOP-deficient non-obese diabetic (NOD.Chop (-/-)) mice. CHOP deficiency did not affect the development of insulitis and diabetes and apoptosis in β-cells. Interestingly, NOD.Chop (-/-) mice exhibited a delayed appearance of insulin autoantibodies compared to wild-type (wt) mice. Adoptive transfer with the diabetogenic, whole or CD8(+)-depleted splenocytes induced β-cell apoptosis and the rapid onset of diabetes in the irradiated NOD.Chop (-/-) recipients with similar kinetics as in wt mice. Expression of ER stress-associated genes was not significantly up-regulated in the islets from NOD.Chop (-/-) compared to those from wt mice or NOD-scid mice. These findings suggest that CHOP expression is independent of the development of insulitis and diabetes but might affect the early production of insulin autoantibodies in the NOD mouse.

Published

2011

13. Mild electrical stimulation with heat shock ameliorates insulin resistance via enhanced insulin signaling.

Author

Morino S, Kondo T, Sasaki K, Adachi H, Suico MA, Sekimoto E, Matsuda T, Shuto T, Araki E, and Kai H

Subjects

Animals, Blood Glucose metabolism, Electric Stimulation, HSP72 Heat-Shock Proteins metabolism, Hepatocytes metabolism, Humans, Hyperglycemia metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Inbred Strains, Phenotype, Phosphatidylinositol 3-Kinases metabolism, Phosphorylation, Proto-Oncogene Proteins c-akt metabolism, Heat-Shock Response physiology, Insulin metabolism, Insulin Resistance physiology, Signal Transduction

Abstract

Low-intensity electrical current (or mild electrical stimulation; MES) influences signal transduction and activates phosphatidylinositol-3 kinase (PI3K)/Akt pathway. Because insulin resistance is characterized by a marked reduction in insulin-stimulated PI3K-mediated activation of Akt, we asked whether MES could increase Akt phosphorylation and ameliorate insulin resistance. In addition, it was also previously reported that heat shock protein 72 (Hsp72) alleviates hyperglycemia. Thus, we applied MES in combination with heat shock (HS) to in vitro and in vivo models of insulin resistance. Here we show that 10-min treatment with MES at 5 V (0.1 ms pulse duration) together with HS at 42 degrees C increased the phosphorylation of insulin signaling molecules such as insulin receptor substrate (IRS) and Akt in HepG2 cells maintained in high-glucose medium. MES (12 V)+mild HS treatment of high fat-fed mice also increased the phosphorylation of insulin receptor beta subunit (IRbeta) and Akt in mice liver. In high fat-fed mice and db/db mice, MES+HS treatment for 10 min applied twice a week for 12-15 weeks significantly decreased fasting blood glucose and insulin levels and improved insulin sensitivity. The treated mice showed significantly lower weight of visceral and subcutaneous fat, a markedly improved fatty liver and decreased size of adipocytes. Our findings indicated that the combination of MES and HS alleviated insulin resistance and improved fat metabolism in diabetes mouse models, in part, by enhancing the insulin signaling pathway.

Published

2008

14. Possible relevance of alpha lipoic acid contained in a health supplement in a case of insulin autoimmune syndrome.

Author

Furukawa N, Miyamura N, Nishida K, Motoshima H, Taketa K, and Araki E

Subjects

Adult, Autoimmune Diseases blood, Blood Glucose analysis, Female, HLA-DR Antigens blood, HLA-DRB1 Chains, Humans, Autoimmune Diseases etiology, Dietary Supplements, Insulin blood, Thioctic Acid adverse effects

Abstract

The insulin autoimmune syndrome is characterized as producing polyclonal or monoclonal anti-insulin autoantibodies in a patient with no previous history of exposure to exogenous insulin. The patient is 44-year-old Japanese woman and she had symptoms of hypoglycaemia without exposure to exogenous insulin. The patient was considered to have IAS because high titre of anti-insulin autoantibodies (96-98%: bound/total) were found in her serum. Her HLA DR beta1 DNA sequences analysis revealed that she has the DRB1(*)0406 and DRB1(*)0901. Our patient have been taken alpha lipoic acid (ALA) before onset. SH group compounds are known to play an important role in the pathogenesis of IAS, and ALA contains SH. From these data, we propose the possibility of the correlation between pathogenesis of IAS and ALA, and it will be important to pay attention for ALA as a cause of hypoglycemia in such cases.

Published

2007

15. Impact of mitochondrial reactive oxygen species and apoptosis signal-regulating kinase 1 on insulin signaling.

Author

Imoto K, Kukidome D, Nishikawa T, Matsuhisa T, Sonoda K, Fujisawa K, Yano M, Motoshima H, Taguchi T, Tsuruzoe K, Matsumura T, Ichijo H, and Araki E

Subjects

Animals, Carcinoma, Hepatocellular, Carrier Proteins pharmacology, Cell Line, Tumor, Humans, Ion Channels, Liver Neoplasms, Membrane Proteins pharmacology, Mitochondria drug effects, Mitochondrial Proteins, Rats, Superoxide Dismutase genetics, Superoxide Dismutase pharmacology, Uncoupling Agents pharmacology, Uncoupling Protein 1, Insulin pharmacology, MAP Kinase Kinase Kinase 5 metabolism, Mitochondria physiology, Reactive Oxygen Species, Signal Transduction physiology, Tumor Necrosis Factor-alpha pharmacology

Abstract

Tumor necrosis factor (TNF)-alpha inhibits insulin action; however, the precise mechanisms are unknown. It was reported that TNF-alpha could increase mitochondrial reactive oxygen species (ROS) production, and apoptosis signal-regulating kinase 1 (ASK1) was reported to be required for TNF-alpha-induced apoptosis. Here, we examined roles of mitochondrial ROS and ASK1 in TNF-alpha-induced impaired insulin signaling in cultured human hepatoma (Huh7) cells. Using reduced MitoTracker Red probe, we confirmed that TNF-alpha increased mitochondrial ROS production, which was suppressed by overexpression of either uncoupling protein-1 (UCP)-1 or manganese superoxide dismutase (MnSOD). TNF-alpha significantly activated ASK1, increased serine phosphorylation of insulin receptor substrate (IRS)-1, and decreased insulin-stimulated tyrosine phosphorylation of IRS-1 and serine phosphorylation of Akt, and all of these effects were inhibited by overexpression of either UCP-1 or MnSOD. Similar to TNF-alpha, overexpression of wild-type ASK1 increased serine phosphorylation of IRS-1 and decreased insulin-stimulated tyrosine phosphorylation of IRS-1, whereas overexpression of dominant-negative ASK1 ameliorated these TNF-alpha-induced events. In addition, TNF-alpha activated c-jun NH(2)-terminal kinases (JNKs), and this observation was partially inhibited by overexpression of UCP-1, MnSOD, or dominant-negative ASK1. These results suggest that TNF-alpha increases mitochondrial ROS and activates ASK1 in Huh7 cells and that these TNF-alpha-induced phenomena contribute, at least in part, to impaired insulin signaling.

Published

2006

16. A case of insulin autoimmune syndrome with HLA DRB1*0404: impact on the hypothesis for the molecular pathogenesis involving DRB1 molecules.

Author

Miyamura N, Murata Y, Taketa K, Ichihara Y, Matsumura T, Tokunaga H, Matsumoto K, Sakakida M, and Araki E

Subjects

Female, HLA-DR Antigens genetics, HLA-DRB1 Chains, Humans, Linkage Disequilibrium genetics, Middle Aged, Syndrome, Autoimmune Diseases immunology, HLA-DR Antigens immunology, Insulin immunology

Published

2006

17. [Regulation of insulin signaling and its disorder].

Author

Araki E and Kondo T

Subjects

Active Transport, Cell Nucleus, Animals, Appetite, DNA-Binding Proteins metabolism, Humans, Hypothalamus, Insulin Receptor Substrate Proteins, Insulin Resistance, Intracellular Signaling Peptides and Proteins, Leptin physiology, Phosphatidylinositol 3-Kinases metabolism, Phosphatidylinositol Phosphates metabolism, Phosphoproteins physiology, Receptor, Insulin genetics, Receptor, Insulin physiology, STAT3 Transcription Factor, Signal Transduction physiology, Trans-Activators metabolism, Insulin physiology, Signal Transduction genetics

Published

2005

18. Comparison between closed-loop portal and peripheral venous insulin delivery systems for an artificial endocrine pancreas.

Author

Sekigami T, Shimoda S, Nishida K, Matsuo Y, Ichimori S, Ichinose K, Shichiri M, Sakakida M, and Araki E

Subjects

Algorithms, Animals, Blood Glucose analysis, Disease Models, Animal, Dogs, Infusions, Intravenous, Insulin administration & dosage, Portal System drug effects, Probability, Random Allocation, Sensitivity and Specificity, Blood Glucose metabolism, Infusions, Parenteral, Insulin pharmacology, Insulin Infusion Systems, Portal Vein

Abstract

To establish the ideal insulin delivery route for an artificial endocrine pancreas, we examined the effectiveness of closed-loop portal insulin delivery. We investigated the effects of the route of insulin delivery on net hepatic glucose balance (NHGB) in dogs under pancreatic clamp conditions with somatostatin plus basal glucagon and insulin infusions. A constant rate of suprabasal insulin was infused via the portal vein or a peripheral vein, and glucose was infused into the portal vein for 180 min. The mean net hepatic glucose uptake (NHGU) values in the portal insulin infusion group (PI group) were significantly greater than those in the peripheral venous insulin infusion group (VI group); the changes from the baseline values at 180 min were 3.54 +/- 0.66 and 2.45 +/- 0.82 mg kg(-1) min(-1) in the PI and VI groups, respectively, P < 0.05. Furthermore, dogs under pancreatic clamp conditions were controlled after a 2-g/kg oral glucose load by applying the closed-loop intraportal (PO) or intravenous (IV) insulin infusion algorithm. There were no significant differences in glycemic control and insulin requirements between these algorithms. However, the maximum peripheral venous and arterial plasma insulin concentrations with the PO algorithm were significantly lower than those with the IV algorithm [305.1 +/- 68.9 and 468.1 +/- 66.9 pmol/l (peripheral vein) and 305.3 +/- 62.9 and 469.6 +/- 85.1 pmol/l (artery) with the PO and IV algorithms, respectively, P < 0.05]. On the other hand, the maximum portal plasma insulin concentration with the PO algorithm was significantly higher than that with the IV algorithm (619.9 +/- 101.7 and 414.3 +/- 79.9 pmol/l with the PO and IV algorithms, respectively, P < 0.05). The mean NHGU values with the PO algorithm were significantly greater than those with the IV algorithm. Our results confirmed that closed-loop portal insulin delivery is feasible with regard to both insulin profiles and hepatic glucose handling in vivo, and indicated that the portal vein is the most suitable insulin delivery route for the artificial endocrine pancreas.

Published

2004

19. Insulin down-regulates insulin receptor substrate-2 expression through the phosphatidylinositol 3-kinase/Akt pathway.

Author

Hirashima Y, Tsuruzoe K, Kodama S, Igata M, Toyonaga T, Ueki K, Kahn CR, and Araki E

Subjects

Animals, Carcinoma, Hepatocellular, Cell Line, Chromones pharmacology, Cycloheximide pharmacology, Depression, Chemical, Enzyme Inhibitors pharmacology, Flavonoids pharmacology, Humans, Insulin Receptor Substrate Proteins, Intracellular Signaling Peptides and Proteins, Mice, Morpholines pharmacology, Phosphoinositide-3 Kinase Inhibitors, Phosphoproteins genetics, Promoter Regions, Genetic, Protein Synthesis Inhibitors pharmacology, Proto-Oncogene Proteins c-akt, RNA, Messenger analysis, Rats, Sequence Alignment, Insulin pharmacology, Liver metabolism, Phosphatidylinositol 3-Kinases metabolism, Phosphoproteins metabolism, Protein Serine-Threonine Kinases, Proto-Oncogene Proteins metabolism, Signal Transduction

Abstract

Insulin receptor substrate (IRS)-1 and IRS-2 are the major substrates that mediate insulin action. Insulin itself regulates the expression of the IRS protein in the liver, but the underlying mechanisms of IRS-1 and IRS-2 regulation are not fully understood. Here we report that insulin suppressed the expression of both IRS-1 and IRS-2 proteins in Fao hepatoma cells. The decrease in IRS-1 protein occurred via proteasomal degradation without any change in IRS-1 mRNA, whereas the insulin-induced suppression of IRS-2 protein was associated with a parallel decrease in IRS-2 mRNA without changing IRS-2 mRNA half-life. The insulin-induced suppression of IRS-2 mRNA and protein was blocked by the phosphatidylinositol (PI) 3-kinase inhibitor, LY294002, but not by the MAP kinase-ERK kinase (MEK) inhibitor, PD098059. Inhibition of Akt by overexpression of dominant-negative Akt also caused complete attenuation of the insulin-induced decrease in IRS-2 protein and partial attenuation of its mRNA down-regulation. Some nuclear proteins bound to the insulin response element (IRE) sequence on the IRS-2 gene in an insulin-dependent manner in vitro, and the binding was also blocked by the PI 3-kinase inhibitor. Reporter gene assay showed that insulin suppressed the activity of both human and rat IRS-2 gene promoters through the IRE in a PI 3-kinase-dependent manner. Our results indicate that insulin regulates IRS-1 and IRS-2 through different mechanisms and that insulin represses IRS-2 gene expression via a PI 3-kinase/Akt pathway.

Published

2003

20. New aspects of neurotransmitter release and exocytosis: involvement of Ca2+/calmodulin-dependent phosphorylation of synapsin I in insulin exocytosis.

Author

Yamamoto H, Matsumoto K, Araki E, and Miyamoto E

Subjects

Animals, Calcium-Calmodulin-Dependent Protein Kinase Type 2, Calcium-Calmodulin-Dependent Protein Kinases metabolism, Humans, Insulin physiology, Insulin Secretion, Phosphorylation, Calcium-Calmodulin-Dependent Protein Kinases physiology, Exocytosis physiology, Insulin metabolism, Neurotransmitter Agents metabolism, Synapsins metabolism

Abstract

The exocytosis of insulin from pancreatic beta-cells is closely related to intracellular elevation of Ca(2+). The effects of Ca(2+) may be mediated by Ca(2+)/calmodulin-dependent protein kinase II (CaMKII). Four subunits of CaMKII, termed alpha, beta, gamma, and delta, are encoded by distinct genes, and various isoforms of these subunits exist as different splicing variants. In the brain, phosphorylation of synapsin I by the alpha isoform induces neurotransmitter release. In order to clarify whether phosphorylation of synapsin I by CaMKII was involved in insulin exocytosis, we cloned the isoforms of CaMKII and synapsin I from mouse insulinoma MIN6 cells. We found that beta'e and delta2 are the major isoforms of CaMKII and that synapsin Ib is a major isoform of synapsin I in MIN6 cells. It was interesting that delta2 and synapsin Ib were co-localized with insulin secretory granules in the cells. Treatment of MIN6 cells with glucose and tolbutamide rapidly activated CaMKII. Immunoblot analysis with two antibodies against synapsin I phosphorylated by CaMKII demonstrated the increase in phosphorylation of synapsin I by the secretagogues. Furthermore, the secretagogue-induced phosphorylation of synapsin I and insulin secretion were potentiated by transient overexpression of the beta'e or delta2 isoform. These results suggest that activation of CaMKII and the concomitant phosphorylation of synapsin I induce insulin exocytosis from pancreatic beta-cells.

Published

2003

21. Insulin down-regulates resistin mRNA through the synthesis of protein(s) that could accelerate the degradation of resistin mRNA in 3T3-L1 adipocytes.

Author

Kawashima J, Tsuruzoe K, Motoshima H, Shirakami A, Sakai K, Hirashima Y, Toyonaga T, and Araki E

Subjects

3T3 Cells, Adipocytes drug effects, Animals, Dose-Response Relationship, Drug, Down-Regulation, Insulin administration & dosage, Insulin metabolism, Intercellular Signaling Peptides and Proteins, Mice, Mitogen-Activated Protein Kinases metabolism, Nerve Growth Factor, Phosphatidylinositol 3-Kinases metabolism, Resistin, Signal Transduction, Time Factors, p38 Mitogen-Activated Protein Kinases, Adipocytes metabolism, Hormones, Ectopic genetics, Insulin pharmacology, Proteins, RNA, Messenger metabolism

Abstract

Aims/hypothesis: Resistin is a peptide secreted by adipocytes and recognized as a hormone that could link obesity to insulin resistance. This study was designed to examine the effect and mechanism(s) of insulin on resistin expression in 3T3-L1 adipocytes., Methods: Differentiated 3T3-L1 adipocytes were stimulated with insulin and resistin mRNA expression was examined by Northern blot analysis. In some experiments, the insulin signal was blocked by several chemical inhibitors or overexpression of a dominant negative form (Deltap85) of the p85 subunit of phosphatidylinositol 3-kinase (PI 3-kinase)., Results: Insulin treatment caused a reduction of resistin mRNA in time-dependent and dose-dependent manners in 3T3-L1 adipocytes. Pre-treatment with PD98059, an inhibitor of extracellular signal-regulated kinase 1/2 (ERK1/2) pathway, or SB203580, an inhibitor of p38 mitogen-activated protein-kinase (p38 MAP-kinase) pathway, did not influence insulin-induced reduction of resistin mRNA. Inhibition of PI 3-kinase by LY294002 or Deltap85 also failed to block insulin-induced reduction of resistin mRNA. Cycloheximide, a protein synthesis inhibitor, completely blocked insulin-induced reduction of resistin mRNA. Actinomycin D, a RNA synthesis inhibitor, also blocked insulin-induced reduction of resistin mRNA, and the decreasing rate of resistin mRNA in cells treated with insulin alone was faster than that with actinomycin D., Conclusion/interpretation: Insulin downregulates resistin mRNA via PI 3-kinase, ERK or p38 MAP-kinase independent pathways in 3T3-L1 adipocytes. The downregulation mechanism of resistin mRNA by insulin would be an indirect event through the synthesis of novel protein(s) that could accelerate the degradation of resistin mRNA.

Published

2003

22. Mitochondrial reactive oxygen species reduce insulin secretion by pancreatic beta-cells.

Author

Sakai K, Matsumoto K, Nishikawa T, Suefuji M, Nakamaru K, Hirashima Y, Kawashima J, Shirotani T, Ichinose K, Brownlee M, and Araki E

Subjects

Animals, Cell Line, Electron Transport drug effects, Glucose pharmacology, Glyceraldehyde-3-Phosphate Dehydrogenases antagonists & inhibitors, Glyceraldehyde-3-Phosphate Dehydrogenases metabolism, Humans, In Vitro Techniques, Insulin Secretion, Iodoacetates pharmacology, Islets of Langerhans drug effects, Mice, Mice, Inbred ICR, Mitochondria drug effects, Superoxides metabolism, Insulin metabolism, Islets of Langerhans metabolism, Mitochondria metabolism, Reactive Oxygen Species metabolism

Abstract

Pancreatic beta-cells exposed to hyperglycemia produce reactive oxygen species (ROS). Because beta-cells are sensitive to oxidative stress, excessive ROS may cause dysfunction of beta-cells. Here we demonstrate that mitochondrial ROS suppress glucose-induced insulin secretion (GIIS) from beta-cells. Intracellular ROS increased 15min after exposure to high glucose and this effect was blunted by inhibitors of the mitochondrial function. GIIS was also suppressed by H(2)O(2), a chemical substitute for ROS. Interestingly, the first-phase of GIIS could be suppressed by 50 microM H(2)O(2). H(2)O(2) or high glucose suppressed the activity of glyceraldehyde 3-phosphate dehydrogenase (GAPDH), a glycolytic enzyme, and inhibitors of the mitochondrial function abolished the latter effects. Our data suggested that high glucose induced mitochondrial ROS, which suppressed first-phase of GIIS, at least in part, through the suppression of GAPDH activity. We propose that mitochondrial overwork is a potential mechanism causing impaired first-phase of GIIS in the early stages of diabetes mellitus.

Published

2003

23. Strict glycemic control in diabetic dogs with closed-loop intraperitoneal insulin infusion algorithm designed for an artificial endocrine pancreas.

Author

Matsuo Y, Shimoda S, Sakakida M, Nishida K, Sekigami T, Ichimori S, Ichinose K, Shichiri M, and Araki E

Subjects

Algorithms, Animals, Blood Glucose analysis, Dogs, Eating, Feasibility Studies, Glucose metabolism, Glucose pharmacology, Infusions, Parenteral, Models, Theoretical, Blood Glucose metabolism, Diabetes Mellitus drug therapy, Hypoglycemic Agents administration & dosage, Insulin administration & dosage, Insulin Infusion Systems

Abstract

The ultimate goal of the development of an artificial endocrine pancreas is to achieve long-term strict glycemic regulation. To establish the physiological insulin delivery route of the artificial endocrine pancreas, intraperitoneal insulin infusion may be important. For this purpose, we tried to develop a closed-loop intraperitoneal insulin infusion algorithm by analyzing the pharmacokinetics of intraperitoneal regular insulin absorption using a mathematical model. The parameters for this algorithm were calculated to simulate the plasma insulin profile after intraperitoneal insulin injection as closely as possible. To evaluate the appropriateness of this algorithm, we tried glycemic control after an oral glucose load of 2 g/kg or a meal load of 80 kcal/kg in diabetic dogs by applying the algorithm. With the use of the subcutaneous insulin lispro infusion algorithm, which we have previously reported, alloxan-induced diabetic dogs exhibited postprandial hyperglycemia and delayed hyperinsulinemia, followed by hypoglycemia after an oral glucose load of 2 g/kg. However, by using the intraperitoneal insulin infusion algorithm, excellent glycemic control (postprandial blood glucose levels of 9.1 +/- 0.8 mmol/l at 70 min and 3.8 +/- 0.3 mmol/l at 240 min, respectively) could be achieved without any associated delayed hyperinsulinemia or hypoglycemia. Glycemic excursion after a meal load of 80 kcal/kg was also controlled from 3.9 to 10.1 mmol/l. Our results confirm that the intraperitoneal insulin infusion algorithm in vivo is feasible and that this algorithm can be superior to the subcutaneous insulin lispro infusion algorithm in the regulation of blood glucose.

Published

2003

24. [Exercise, foods and bathing during insulin therapy].

Author

Kishikawa H, Soejima H, Tamama Y, Taguchi T, Araki E, and Shichiri M

Subjects

Blood Glucose metabolism, Blood Glucose Self-Monitoring, Drug Administration Schedule, Humans, Insulin pharmacokinetics, Ketone Bodies blood, Baths, Diabetes Mellitus, Type 1 blood, Diabetes Mellitus, Type 2 blood, Eating physiology, Exercise physiology, Insulin administration & dosage, Self Care

Published

2002

25. [Implantable artificial endocrine pancreas].

Author

Shichiri M, Nishida K, Sakakida M, and Araki E

Subjects

Biosensing Techniques, Blood Glucose analysis, Diabetes Mellitus blood, Diabetes Mellitus drug therapy, Humans, Monitoring, Physiologic instrumentation, Monitoring, Physiologic methods, Telemetry, Hypoglycemic Agents administration & dosage, Infusion Pumps, Implantable, Insulin administration & dosage, Insulin Infusion Systems

Published

2002

26. [Intensive insulin therapy to prevent the progression of chronic vascular complications in type 2 diabetes mellitus].

Author

Kishikawa H, Araki E, Wake N, and Shichiri M

Subjects

Blood Glucose, Chronic Disease, Clinical Trials as Topic, Diabetes Mellitus, Type 2 blood, Diabetes Mellitus, Type 2 complications, Disease Progression, Humans, Insulin adverse effects, Quality of Life, Risk Reduction Behavior, Diabetes Mellitus, Type 2 drug therapy, Diabetic Angiopathies prevention & control, Hypoglycemic Agents administration & dosage, Insulin administration & dosage

Published

2002

27. [The study of development and progression of long-term complications in type I diabetes].

Author

Araki E and Matsumura T

Subjects

Blood Glucose, Diabetes Mellitus, Type 1 blood, Diabetes Mellitus, Type 1 complications, Diabetic Angiopathies etiology, Diabetic Nephropathies etiology, Diabetic Neuropathies etiology, Disease Progression, Glycated Hemoglobin metabolism, Humans, Quality of Life, Time Factors, Clinical Trials as Topic, Diabetes Mellitus, Type 1 drug therapy, Diabetic Angiopathies prevention & control, Diabetic Nephropathies prevention & control, Diabetic Neuropathies prevention & control, Hypoglycemic Agents administration & dosage, Insulin administration & dosage

Published

2002

28. [Application and practice of intensive insulin therapy].

Author

Kishikawa H, Soejima H, Tamama Y, Araki E, and Shichiri M

Subjects

Blood Glucose Self-Monitoring, Diabetic Angiopathies prevention & control, Drug Administration Schedule, Humans, Hypoglycemia etiology, Hypoglycemia prevention & control, Hypoglycemic Agents adverse effects, Injections, Subcutaneous, Insulin adverse effects, Insulin Infusion Systems, Obesity etiology, Obesity prevention & control, Diabetes Mellitus, Type 1 drug therapy, Diabetes Mellitus, Type 2 drug therapy, Hypoglycemic Agents administration & dosage, Insulin administration & dosage

Published

2002

29. Regulation of the insulin gene transcription by glucose.

Author

Furukawa N, Shirotani T, Nakamaru K, Matsumoto K, Shichiri M, and Araki E

Subjects

Animals, Humans, Insulin genetics, Islets of Langerhans physiopathology, Promoter Regions, Genetic physiology, Rats, Transcription, Genetic physiology, Gene Expression Regulation physiology, Glucose physiology, Insulin biosynthesis

Published

2002

30. The gene for hepatocyte nuclear factor (HNF)-4alpha is activated by glucocorticoids and glucagon, and repressed by insulin in rat liver.

Author

Oyadomari S, Matsuno F, Chowdhury S, Kimura T, Iwase K, Araki E, Shichiri M, Mori M, and Takiguchi M

Subjects

Animals, Blotting, Western, Cells, Cultured, Dexamethasone antagonists & inhibitors, Diabetes Mellitus, Experimental chemically induced, Diabetes Mellitus, Experimental genetics, Diabetes Mellitus, Experimental metabolism, Glucagon antagonists & inhibitors, Glucose metabolism, Hepatocyte Nuclear Factor 4, Insulin Antagonists pharmacology, Liver cytology, Liver metabolism, Liver pathology, Male, Phosphoproteins metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, Rats, Rats, Wistar, Transcription Factors metabolism, Transcriptional Activation drug effects, DNA-Binding Proteins, Dexamethasone pharmacology, Gene Expression Regulation drug effects, Glucagon pharmacology, Insulin pharmacology, Liver drug effects, Phosphoproteins genetics, Transcription Factors genetics

Abstract

The gene for a transcription factor hepatocyte nuclear factor-4alpha (HNF-4alpha) is responsible for maturity-onset diabetes of the young, type 1. We examined hormonal regulation of the HNF-4alpha gene in the liver. Stimulation of primary-cultured rat hepatocytes with dexamethasone or glucagon led to induction of HNF-4alpha mRNA, being antagonized by insulin. In the liver of streptozotocin-induced diabetic rat, mRNA and protein levels for HNF-4alpha were elevated, and were normalized by insulin treatment. Therefore, HNF-4alpha in the liver is likely to be involved in the regulation of glucose metabolism in response to these hormones.

Published

2000

31. Bradykinin enhances insulin receptor tyrosine kinase in 32D cells reconstituted with bradykinin and insulin signaling pathways.

Author

Motoshima H, Araki E, Nishiyama T, Taguchi T, Kaneko K, Hirashima Y, Yoshizato K, Shirakami A, Sakai K, Kawashima J, Shirotani T, Kishikawa H, and Shichiri M

Subjects

Animals, Cell Line, Insulin pharmacology, Insulin Receptor Substrate Proteins, Isoenzymes metabolism, Mice, Phosphatidylinositol 3-Kinases metabolism, Phosphoproteins metabolism, Phosphorylation drug effects, Receptor, Bradykinin B2, Receptor, Insulin metabolism, Receptors, Bradykinin metabolism, Subcellular Fractions metabolism, Time Factors, Transfection, Tyrosine metabolism, Bradykinin pharmacology, Insulin physiology, Protein-Tyrosine Kinases metabolism, Signal Transduction physiology

Abstract

We have previously shown that bradykinin potentiated insulin-induced glucose uptake through GLUT4 translocation in canine adipocytes and skeletal muscles. The aim of this study was to determine the molecular mechanism of bradykinin enhancement of the insulin signal. For this purpose, 32D cells, which express a limited number of insulin receptors and lack endogenous bradykinin B2 receptor (BK2R) or insulin receptor substrate (IRS)-1 were transfected with BK2R cDNA and/or insulin receptor cDNA and/or IRS-1 cDNA, and analyzed. In 32D cells that expressed BK2R and insulin receptor (32D-BKR/IR), bradykinin alone had no effect on the phosphorylation of the insulin receptor, but it enhanced insulin-stimulated tyrosine phosphorylation of the insulin receptor. In 32D cells that expressed BK2R, insulin receptor and IRS-1 (32D-BKR/IR/IRS1), bradykinin also enhanced insulin-stimulated tyrosine phosphorylation of the insulin receptor and IRS-1. An increase in insulin-stimulated phosphorylation of IRS-1 by treatment with bradykinin in 32D-BKR/IR/IRS1 cell was associated with increased binding of 85 kD subunit of phosphatidylinositol 3 (PI 3)-kinase and increased IRS-1 associated PI 3-kinase activity. These effects of bradykinin were not observed in 32D cells which lack the expression of BK2R (32D-IR/IRS1) or insulin receptor (32D-BKR/IRS1). Furthermore, tyrosine phosphatase activity against insulin receptor beta-subunit in plasma membrane fraction of 32D-BKR/IR cells was significantly reduced by bradykinin, suggesting that the effect of bradykinin was in part mediated by inhibition of protein tyrosine phosphatase(s). Our results clearly demonstrated that bradykinin enhanced insulin-stimulated tyrosine kinase activity of the insulin receptor and downstream insulin signal cascade through the BK2R mediated signal pathway.

Published

2000

32. Cost-effectiveness of intensive insulin therapy for type 2 diabetes: a 10-year follow-up of the Kumamoto study.

Author

Wake N, Hisashige A, Katayama T, Kishikawa H, Ohkubo Y, Sakai M, Araki E, and Shichiri M

Subjects

Adult, Cohort Studies, Cost-Benefit Analysis, Diabetic Nephropathies prevention & control, Diabetic Neuropathies prevention & control, Diabetic Retinopathy prevention & control, Drug Administration Schedule, Female, Follow-Up Studies, Health Care Costs, Humans, Hypoglycemic Agents adverse effects, Hypoglycemic Agents therapeutic use, Injections, Insulin adverse effects, Insulin therapeutic use, Male, Middle Aged, Time Factors, Treatment Outcome, Diabetes Mellitus, Type 2 drug therapy, Hypoglycemic Agents administration & dosage, Hypoglycemic Agents economics, Insulin administration & dosage, Insulin economics

Abstract

To evaluate the cost and effectiveness of intensive insulin therapy for type 2 diabetes on the prevention of diabetes complications in Japan, we performed economic evaluation based on a randomized controlled trial. A total of 110 patients with type 2 diabetes were randomly assigned into two groups, a multiple insulin injection therapy (MIT) group or a conventional insulin injection therapy (CIT) group, and were followed-up for 10 years. Economic evaluation (cost-consequences analysis) was applied to evaluate both health and economic outcomes. As outcome measures for effectiveness of intensive insulin therapy, the frequency of complications, such as retinopathy, nephropathy, neuropathy, macrovascular event, and diabetes-related death, was used. For estimating costs, a viewpoint of the payer (the National Health Insurance) was adopted. Direct medical costs associated with diabetes care during 10 years were calculated and evaluated. In a base case analysis, all costs were discounted to the present value at an annual rate of 3%. Sensitivity analyses were carried out to assess the robustness of the results to changes in the values of important variables. MIT reduced the relative risk in the progression of retinopathy by 67%, photocoagulation by 77%, progression of nephropathy by 66%, albuminuria by 100% and clinical neuropathy by 64%, relative to CIT. Moreover, MIT prolonged the period in which patients were free of complications, including 2.0 years for progression of retinopathy (P<0.0001), 0.3 years for photocoagulation (P<0.05), 1.5 years for progression of nephropathy (P<0.01) and 2.2 years for clinical neuropathy (P<0.0001). The total cost (discounted at 3%) per patient during the 10-year period for each group was $30310 and 31525, respectively. The reduction of total costs in MIT over CIT was mainly due to reduced costs for management of diabetic complications. Our results show that MIT is more beneficial than CIT in both cost and effectiveness. Therefore, MIT is recommended for the treatment of type 2 diabetic patients who require insulin therapy as early as possible from the perspective of both patients and health policy.

Published

2000

33. Insulin inhibits glucagon secretion by the activation of PI3-kinase in In-R1-G9 cells.

Author

Kaneko K, Shirotani T, Araki E, Matsumoto K, Taguchi T, Motoshima H, Yoshizato K, Kishikawa H, and Shichiri M

Subjects

Animals, Cell Line, Enzyme Activation drug effects, Enzyme Inhibitors pharmacology, Gene Expression Regulation drug effects, Insulin Receptor Substrate Proteins, Islets of Langerhans drug effects, Islets of Langerhans metabolism, Kinetics, Phosphoinositide-3 Kinase Inhibitors, Phosphoproteins metabolism, Phosphorylation, Time Factors, Wortmannin, Androstadienes pharmacology, Glucagon genetics, Glucagon metabolism, Insulin pharmacology, Islets of Langerhans physiology, Phosphatidylinositol 3-Kinases metabolism

Abstract

Intracellular mechanisms through which insulin inhibits glucagon secretion remain to be elucidated in glucagon secreting cells. In this study, we confirmed that, in In-R1-G9 cells, a pancreatic alpha cell line, insulin stimulated phosphorylation of insulin receptor substrate-1 (IRS-1) and activated phosphatidylinositol 3-kinase (PI3-kinase). We further studied, using wortmannin, an inhibitor of PI3-kinase, whether the inhibitory effect of insulin on glucagon secretion was mediated through PI3-kinase pathway in these cells. In static incubation studies, insulin significantly inhibited glucagon secretion at 2, 6 and 12 h, which was completely abolished by pretreatment with wortmannin. In perifusion studies, insulin significantly suppressed glucagon secretion after 10 min, which was also blocked by wortmannin. Insulin also reduced glucagon mRNA at 6 and 12 h but not at 2 h. Wortmannin also abolished insulin-induced reduction of glucagon mRNA. Insulin increased the amount of 85 kDa subunit of PI3-kinase in plasma membrane fraction (PM), with a reciprocal decrease of the kinase in cytosol fraction (CY). Insulin also increased PI3-kinase activity in PM, but not in CY. Our results suggest that insulin suppressed glucagon secretion by inhibiting glucagon release and gene expression. Both actions were mediated by activation of PI3-kinase. Recruitment and activation of PI3-kinase in plasma membrane might be relevant at least in part to insulin-induced inhibition of glucagon release.

Published

1999

34. Cellular characterization of pituitary adenoma cell line (AtT20 cell) transfected with insulin, glucose transporter type 2 (GLUT2) and glucokinase genes: insulin secretion in response to physiological concentrations of glucose.

Author

Motoyoshi S, Shirotani T, Araki E, Sakai K, Kaneko K, Motoshima H, Yoshizato K, Shirakami A, Kishikawa H, and Shichiri M

Subjects

Calcium Channel Blockers pharmacology, Corticotropin-Releasing Hormone pharmacology, Diazoxide pharmacology, Gene Expression, Glucose pharmacology, Glucose Transporter Type 2, Glyburide pharmacology, Humans, Hypoglycemic Agents, Insulin Secretion, Nifedipine pharmacology, Potassium Chloride pharmacology, Transfection, Tumor Cells, Cultured, Adenoma metabolism, Glucokinase genetics, Insulin genetics, Insulin metabolism, Monosaccharide Transport Proteins genetics, Pituitary Neoplasms metabolism

Abstract

We investigated the mechanisms of insulin secretion by transfecting into a pituitary adenoma cell line (AtT20) a combination of genes encoding human insulin (HI), glucose transporter type 2 (GLUT2) and glucokinase (GK), followed by studying the characteristics of these cells. In static incubation, a cell line transfected with insulin gene alone (AtT20HI) secreted mature human insulin but this was not in a glucose-dependent manner. Other cell lines transfected with insulin and GLUT2 genes (AtT20HI-GLUT2-3) or with insulin and GK genes (AtT20HI-GK-1) secreted insulin in response to glucose concentrations of only less than 1 mmol/l. In contrast, cell lines transfected with insulin, GLUT2 and GK genes (AtT20HI-GLUT2-GK-6, AtT20HI-GLUT2-GK-7 and AtT20HI-GLUT2-GK-10) showed a glucose-dependent insulin secretion up to 25 mmol/l glucose. Glucose utilization and oxidation were increased in AtT20HI-GLUT2-GK cell lines but not in AtT20HI, AtT20HI-GLUT2-3 and AtT20HI-GK-1 cells at physiological glucose concentrations, compared with AtT20 cells. Diazoxide, nifedipine and 2-deoxy glucose suppressed (p < 0.05) glucose stimulated insulin secretion in AtT20HI-GLUT2-GK-6 cells. Glibenclamide, KCl or corticotropin releasing factor (CRF) stimulated (p < 0.05) insulin secretion both in AtT20HI and AtT20HI-GLUT2-GK-6 cells. Insulin secretion stimulated by glibenclamide, KCl or CRF was further enhanced by the addition of 25 mmol/l glucose in AtT20HI-GLUT2-GK-6 cells but not in AtT20HI cells. In perifusion experiments, a stepwise increase in glucose concentration from 5 to 25 mmol/l stimulated insulin secretion in AtT20HI-GLUT2-GK cell lines but the response lacked a clear first phase of insulin secretion. Our results suggest that both GLUT2 and glucokinase are necessary for the glucose stimulated insulin secretion in at least rodent cell lines, and that other element(s) are necessary for a biphasic insulin secretion typically observed in beta cells.

Published

1998

35. Creation and characterization of a mitochondrial DNA-depleted pancreatic beta-cell line: impaired insulin secretion induced by glucose, leucine, and sulfonylureas.

Author

Tsuruzoe K, Araki E, Furukawa N, Shirotani T, Matsumoto K, Kaneko K, Motoshima H, Yoshizato K, Shirakami A, Kishikawa H, Miyazaki J, and Shichiri M

Subjects

Adenosine Triphosphate biosynthesis, Calcium metabolism, Cell Respiration, Ethidium pharmacology, Glucose metabolism, Histocytochemistry, Humans, Insulin biosynthesis, Insulin genetics, Insulin Secretion, Intracellular Fluid metabolism, Islets of Langerhans cytology, Mitochondria enzymology, Oxidation-Reduction, Phosphorylation, RNA, Messenger biosynthesis, Tumor Cells, Cultured, DNA, Mitochondrial biosynthesis, Glucose pharmacology, Insulin metabolism, Islets of Langerhans metabolism, Leucine pharmacology, Sulfonylurea Compounds pharmacology

Abstract

It has been proposed that mitochondrial oxidative phosphorylation in pancreatic beta-cells plays an important role in insulin secretion. To examine the impact of mitochondrial dysfunction on insulin secretion, we created a MIN6 cell line that depleted mitochondrial DNA (mtDNA) by treatment with ethidium bromide (EtBr), and studied the response of the cell line to various secretagogues. MIN6 cells cultured with 0.5 microg/ml EtBr for over 2 months (termed MIN6 deltamt cells) revealed a marked (>90%) decrease in mtDNA content and a lack of mRNAs encoded by mtDNA. MIN6 deltamt cells showed the defects of cytochrome c oxidase activity, glucose- and leucine-induced increase in cellular ATP content, and respiratory chain-driven ATP synthesis, suggesting that MIN6 deltamt cells lost oxidative phosphorylation activity due to the selective disruption of the subunits of respiratory chain enzymes encoded by mtDNA. MIN6 deltamt cells also showed a decrease in glucose utilization, suggesting the impairment of the glycolytic pathway as well. After stimulation with glucose and leucine, MIN6 deltamt cells showed no response in insulin secretion or intracellular free Ca2+ concentration ([Ca2+]i). On the other hand, arginine stimulated insulin secretion and an increase in [Ca2+]i in MIN6 deltamt cells as in MIN6 cells. Glibenclamide also stimulated insulin secretion and an increase in [Ca2+]i in both types of cells, but the responses of MIN6 deltamt cells were significantly lower than those of MIN6 cells. These results suggest the importance of ATP production in insulin secretion and an increase in [Ca2+]i, both induced by glucose and leucine. Moreover, mitochondrial function turns out to be not essential but important for the activation of sulfonylurea-induced insulin secretion.

Published

1998

36. Bradykinin potentiates insulin-stimulated glucose uptake and enhances insulin signal through the bradykinin B2 receptor in dog skeletal muscle and rat L6 myoblasts.

Author

Miyata T, Taguchi T, Uehara M, Isami S, Kishikawa H, Kaneko K, Araki E, and Shichiri M

Subjects

Animals, Base Sequence, Binding Sites, Binding, Competitive, Bradykinin analysis, Bradykinin pharmacology, Cell Line, DNA Primers chemistry, Dogs, Dose-Response Relationship, Drug, Insulin pharmacology, Insulin Receptor Substrate Proteins, Male, Muscle, Skeletal cytology, Muscle, Skeletal drug effects, Phosphoproteins drug effects, Phosphoproteins metabolism, Phosphorylation drug effects, Polymerase Chain Reaction, RNA, Messenger analysis, RNA, Messenger genetics, Rats, Receptor, Insulin drug effects, Receptors, Bradykinin drug effects, Signal Transduction drug effects, Tritium, Bradykinin metabolism, Glucose metabolism, Insulin metabolism, Muscle, Skeletal metabolism, Receptor, Insulin metabolism, Receptors, Bradykinin metabolism, Signal Transduction physiology

Abstract

Previously we demonstrated that bradykinin infusion could increase glucose uptake into dog peripheral tissues, and that bradykinin could potentiate insulin-induced glucose uptake through glucose transporter 4 (GLUT4) translocation in dog adipocytes. However, skeletal muscle is the predominant tissue for insulin-mediated glucose disposal. The aim of this study was to determine how bradykinin affected insulin-stimulated glucose uptake in dog skeletal muscle and myotubes transformed from rat L6 myoblasts. The bradykinin receptor binding studies revealed that dog skeletal muscle and rat L6 myoblasts possessed significant numbers of bradykinin receptors (Kd = 88 and 76 pmol/l, Bmax = 82.5 and 20 fmol/mg protein respectively). An RT-PCR (reverse transcriptase-polymerase chain reaction) amplification showed mRNA specific for bradykinin B2 receptor in both cells. Bradykinin significantly increased 2-deoxyglucose uptake in isolated muscle and L6 myoblasts in the presence of insulin (10(-7) mol/l) in a dose-dependent manner, but not in the absence of insulin. Bradykinin also enhanced insulin-stimulated GLUT4 translocation, and insulin-induced phosphorylation of insulin receptor beta subunit and insulin receptor substrate-1 (IRS-1) without affecting the binding affinities or numbers of cell surface insulin receptors in both cells. It is concluded that bradykinin could potentiate the insulin-induced glucose uptake through GLUT4 translocation in dog skeletal muscle and rat L6 myoblasts. This effect could be explained by the potency of bradykinin to upregulate the insulin receptor tyrosine kinase activity which stimulates phosphorylation of IRS-1, followed by an increase in GLUT4 translocation.

Published

1998

37. Impact of natural IRS-1 mutations on insulin signals: mutations of IRS-1 in the PTB domain and near SH2 protein binding sites result in impaired function at different steps of IRS-1 signaling.

Author

Yoshimura R, Araki E, Ura S, Todaka M, Tsuruzoe K, Furukawa N, Motoshima H, Yoshizato K, Kaneko K, Matsuda K, Kishikawa H, and Shichiri M

Subjects

Animals, Blotting, Western, Calcium-Calmodulin-Dependent Protein Kinases metabolism, Cell Line, DNA biosynthesis, DNA, Complementary genetics, Electrophoresis, Polyacrylamide Gel, Enzyme Activation, Humans, Insulin Receptor Substrate Proteins, Mice, Phosphoproteins biosynthesis, Phosphoproteins metabolism, Phosphorylation, Precipitin Tests, Rats, Thymidine metabolism, Gene Expression Regulation genetics, Insulin pharmacology, Mutation genetics, Phosphoproteins genetics, Phosphotransferases (Alcohol Group Acceptor) metabolism, Receptor, Insulin metabolism, Signal Transduction

Abstract

Insulin receptor substrate-1 (IRS-1) is one of the major substrates of insulin receptor tyrosine kinase and mediates various insulin signals downstream. In this study, we have examined the impact of three natural IRS-1 mutations identified in NIDDM patients (G971R, P170R, and M209T) on insulin signaling. G971R is located near src homology 2 protein binding sites, and P170R and M209T are located in the phosphotyrosine binding domain of IRS-1. 32D-IR cells, stably overexpressing human insulin receptor, were transfected with wild-type human IRS-1 cDNA (WT) or three mutant IRS-1 cDNAs and analyzed. All the cell lines expressing mutant IRS-1 showed a significant reduction in [3H]thymidine incorporation compared with WT. Upon insulin stimulation, cells expressing G971R showed a 39% decrease (P < 0.005) in phosphatidylinositol 3-kinase (PI 3-kinase) activity, a 43% decrease (P < 0.01) in binding of the 85-kDa regulatory subunit of PI 3-kinase, and a 22% decrease (P < 0.05) in mitogen-activated protein kinase activity compared with those expressing WT. Cells expressing P170R and M209T showed slight but significant decreases in PI 3-kinase activity (17 and 14%, respectively; both P < 0.05) and in binding of p85 (22 and 16%, respectively; both P < 0.05) and a greater decrease in mitogen-activated protein kinase activity (41 and 43%, respectively; both P < 0.005) compared with WT. After insulin stimulation, cells expressing P170R and M209T showed significant decreases in IRS-1 phosphorylation (37 and 42%, respectively; both P < 0.05) and in IRS-1 binding to the insulin receptor (48 and 53%, respectively; P < 0.01) compared with WT. G971R showed no changes in IRS-1 phosphorylation and in IRS-1 binding to the insulin receptor compared with WT. These data suggest that the impaired mitogenic response of P170R and M209T was mainly due to reduced binding to the insulin receptor, whereas the impaired response of G971R was mainly due to reduced association with PI 3-kinase p85.

Published

1997

38. Intensive insulin therapy prevents the progression of diabetic microvascular complications in Japanese patients with non-insulin-dependent diabetes mellitus: a randomized prospective 6-year study.

Author

Ohkubo Y, Kishikawa H, Araki E, Miyata T, Isami S, Motoyoshi S, Kojima Y, Furuyoshi N, and Shichiri M

Subjects

Albuminuria, Blood Glucose metabolism, Blood Pressure, C-Peptide urine, Cholesterol blood, Cholesterol, HDL blood, Cohort Studies, Diabetic Angiopathies epidemiology, Diabetic Angiopathies physiopathology, Diabetic Nephropathies epidemiology, Diabetic Nephropathies physiopathology, Diabetic Nephropathies prevention & control, Diabetic Neuropathies epidemiology, Diabetic Neuropathies physiopathology, Diabetic Neuropathies prevention & control, Diabetic Retinopathy epidemiology, Diabetic Retinopathy physiopathology, Diabetic Retinopathy prevention & control, Female, Humans, Japan, Male, Middle Aged, Neural Conduction, Prospective Studies, Statistics, Nonparametric, Time Factors, Triglycerides blood, Diabetes Mellitus, Type 2 drug therapy, Diabetes Mellitus, Type 2 physiopathology, Diabetic Angiopathies prevention & control, Insulin therapeutic use

Abstract

To examine whether intensive glycemic control could decrease the frequency or severity of diabetic microvascular complications, we performed a prospective study of Japanese patients with non-insulin-dependent diabetes mellitus (NIDDM) treated with multiple insulin injection treatment. A total of 110 patients with NIDDM was randomly assigned to multiple insulin injection treatment group (MIT group) or to conventional insulin injection treatment group (CIT group). Fifty-five NIDDM patients who showed no retinopathy and urinary albumin excretions < 30 mg/24 h at the baseline were evaluated in the primary-prevention cohort, and the other 55 NIDDM patients who showed simple retinopathy and urinary albumin excretions < 300 mg/24 h were evaluated in the secondary-intervention cohort. The appearance and the progression of retinopathy, nephropathy and neuropathy were evaluated every 6 months over a 6-year period. The worsening of complications in this study was defined as an increase of 2 or more steps in the 19 stages of the modified ETDRS interim scale for retinopathy and an increase of one or more steps in 3 stages (normoalbuminuria, microalbuminuria and albuminuria) for nephropathy. The cumulative percentages of the development and the progression in retinopathy after 6 years were 7.7% for the MIT group and 32.0% for the CIT group in the primary-prevention cohort (P = 0.039), and 19.2% for MIT group and 44.0% for CIT group in the secondary-intervention cohort (P = 0.049). The cumulative percentages of the development and the progression in nephropathy after 6 years were 7.7% for the MIT group and 28.0% for the CIT group in the primary-prevention cohort (P = 0.032), and 11.5% and 32.0%, respectively, for the MIT and CIT groups in the secondary-intervention cohort (P = 0.044). In neurological tests after 6 years, MIT group showed significant improvement in the nerve conduction velocities, while the CIT group showed significant deterioration in the median nerve conduction velocities and vibration threshold. Although both postural hypotension and the coefficient of variation of R-R interval tended to improve in the MIT group, they deteriorated in the CIT group. In conclusion, intensive glycemic control by multiple insulin injection therapy can delay the onset and the progression of diabetic retinopathy, nephropathy and neuropathy in Japanese patients with NIDDM. From this study, the glycemic threshold to prevent the onset and the progression of diabetic microangiopathy is indicated as follows; HbA1c < 6.5%, FBG < 110 mg/dl, and 2-h post-prandial blood glucose concentration < 180 mg/dl.

Published

1995

39. Expression of insulin receptor on clonal pancreatic alpha cells and its possible role for insulin-stimulated negative regulation of glucagon secretion.

Author

Kisanuki K, Kishikawa H, Araki E, Shirotani T, Uehara M, Isami S, Ura S, Jinnouchi H, Miyamura N, and Shichiri M

Subjects

Animals, Base Sequence, Blotting, Northern, Clone Cells, Cricetinae, DNA Primers, Humans, Immunohistochemistry, Insulinoma, Kinetics, Methionine metabolism, Molecular Sequence Data, Pancreatic Neoplasms, Polymerase Chain Reaction, RNA, Messenger analysis, RNA, Messenger biosynthesis, Receptor, Insulin analysis, Receptor, Insulin metabolism, Sulfur Radioisotopes, Tumor Cells, Cultured, Gene Expression, Glucagon metabolism, Insulin pharmacology, Receptor, Insulin biosynthesis

Abstract

In pancreatic alpha cells, the existence and function of the insulin receptor has not yet been fully established. In this study, to confirm the expression of functional insulin receptors in pancreatic alpha cells, we performed: 1) insulin receptor binding assay, 2) Northern blot analysis and RT-PCR (reverse transcription-polymerase chain reaction) amplification of insulin receptor mRNA, 3) immunocytochemical staining, 4) biosynthetic labelling of insulin receptor protein using [35S]methionine, 5) analysis of insulin-stimulated autophosphorylation of the insulin receptor in glucagon secreting cell lines, In-R1-G9 and alpha TC clone 6 cells. Glucagon secretion decreased with the addition of insulin in both cells. The receptor binding studies using [125I-Tyr-A14] insulin revealed that both cells possessed a significant number of insulin receptors (In-R1-G9:K1 = 2.1 x 10(9) mol/l-1, K2 = 6.2 x 10(7) mol/l-1, R1 = 0.27 x 10(4), R2 = 1.86 x 10(4) sites/cell; alpha TC clone 6: K1 = 2.1 x 10(9) mol/l-1, K2 = 7.3 x 10(7) mol/l-1, R1 = 0.27 x 10(4), R2 = 1.95 x 10(4) sites/cell). Northern blot analysis as well as RT-PCR amplification showed the mRNA specific for insulin receptor in both cells. By immunocytochemical staining using anti-insulin receptor alpha-subunit antibody, positive immunostaining for insulin receptor was observed in both cells. [35S]Methionine labelling of both cells followed by immunoprecipitation using anti-insulin receptor antibody showed the correct size of the insulin receptor protein. The insulin receptor expressed in these cells underwent autophosphorylation by insulin stimulation.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1995

40. Alternative pathway of insulin signalling in mice with targeted disruption of the IRS-1 gene.

Author

Araki E, Lipes MA, Patti ME, Brüning JC, Haag B 3rd, Johnson RS, and Kahn CR

Subjects

Animals, Blood Glucose metabolism, Female, Growth physiology, Insulin Receptor Substrate Proteins, Insulin Resistance physiology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Phosphatidylinositol 3-Kinases, Phosphoproteins deficiency, Phosphotransferases (Alcohol Group Acceptor) metabolism, Phosphotyrosine, Tyrosine analogs & derivatives, Tyrosine metabolism, Insulin physiology, Insulin-Like Growth Factor I physiology, Phosphoproteins physiology, Signal Transduction physiology

Abstract

The principal substrate for the insulin and insulin-like growth factor-1 (IGF-1) receptors is the cytoplasmic protein insulin-receptor substrate-1 (IRS-1/pp185). After tyrosine phosphorylation at several sites, IRS-1 binds to and activates phosphatidylinositol-3'-OH kinase (PI(3)K) and several other proteins containing SH2 (Src-homology 2) domains. To elucidate the role of IRS-1 in insulin/IGF-1 action, we created IRS-1-deficient mice by targeted gene mutation. These mice had no IRS-1 and showed no evidence of IRS-1 phosphorylation or IRS-1-associated PI(3)K activity. They also had a 50 per cent reduction in intrauterine growth, impaired glucose tolerance, and a decrease in insulin/IGF-1-stimulated glucose uptake in vivo and in vitro. The residual insulin/IGF-1 action correlated with the appearance of a new tyrosine-phosphorylated protein (IRS-2) which binds to PI(3)K, but is slightly larger than and immunologically distinct from IRS-1. Our results provide evidence for IRS-1-dependent and IRS-1-independent pathways of insulin/IGF-1 signalling and for the existence of an alternative substrate of these receptor kinases.

Published

1994

41. Regulation of insulin receptor, insulin receptor substrate-1 and phosphatidylinositol 3-kinase in 3T3-F442A adipocytes. Effects of differentiation, insulin, and dexamethasone.

Author

Saad MJ, Folli F, Araki E, Hashimoto N, Csermely P, and Kahn CR

Subjects

3T3 Cells, Adipocytes cytology, Adipocytes drug effects, Amino Acid Sequence, Animals, Antibodies, Base Sequence, Cell Differentiation, DNA Primers, Enzyme Activation, Gene Expression, Immunoblotting, Insulin Receptor Substrate Proteins, Kinetics, Mice, Molecular Sequence Data, Oligopeptides chemical synthesis, Oligopeptides immunology, Phosphatidylinositol 3-Kinases, Phosphorylation, Phosphotyrosine, Polymerase Chain Reaction, Protein Tyrosine Phosphatases metabolism, RNA, Messenger biosynthesis, Time Factors, Tyrosine analogs & derivatives, Tyrosine analysis, Adipocytes metabolism, Dexamethasone pharmacology, Insulin pharmacology, Phosphoproteins biosynthesis, Phosphotransferases (Alcohol Group Acceptor) biosynthesis, Receptor, Insulin biosynthesis

Abstract

Insulin rapidly stimulates tyrosine kinase activity of its receptor resulting in phosphorylation of its cytosolic substrate insulin receptor substrate 1 (IRS-1), which in turn associates with and activates the enzyme phosphatidylinositol 3-kinase (PI 3-kinase). In the present study we have examined these three initial steps in insulin action during the differentiation of 3T3-F442A adipocytes and after treatment with dexamethasone or insulin. The differentiation of 3T3-F442A cells was characterized by a 13-fold increase in insulin receptor protein, a 9-fold increase in IRS-1, and a 10- and 4.5-fold increase in their insulin-stimulated phosphorylation, respectively. The mRNA expression of these two proteins showed a similar 8-fold increase during differentiation. In addition there was a 3.5-fold increase in PI 3-kinase protein [85 kilodalton (kDa) subunit] and a 16-fold increase in IRS-1-associated PI 3-kinase activity between day 0 and day 8 of differentiation. Dexamethasone (1 microM) treatment of differentiated cells induced a further 48% (P < 0.05) increase in insulin receptor level, but the autophosphorylation of the receptor was decreased by 31 +/- 1% (P < 0.02). At the same time there was a decrease by 56 +/- 4% (P < 0.005) in IRS-1 protein and by 31 +/- 1% (P < 0.001) in IRS-1 phosphorylation. The expression of insulin receptor mRNA was unchanged, but the expression of IRS-1 mRNA was decreased by approximately 75% after dexamethasone. By contrast, dexamethasone induced a 69% increase in the level of PI 3-kinase as determined by immunoblotting. The combined effect of decreased IRS-1 phosphorylation and increased PI 3-kinase protein was a minimal change (15% decrease) in the association/activation between IRS-1 and PI 3-kinase. Chronic treatment with 100 nM insulin induced a time- and dose-dependent decrease in insulin receptor and IRS-1 protein levels reaching a nadir of 34 +/- 5% (P < 0.005) and 39 +/- 5% (P < 0.01) of control levels after 24 h, respectively. There was an even more marked decrease in the phosphorylation level of these proteins. Chronic insulin treatment also produced a 30% decrease in PI 3-kinase protein levels and a approximately 50% decrease in the association/activation between IRS-1/PI 3-kinase. The expression of insulin receptor and IRS-1 mRNA was unchanged during chronic insulin treatment.(ABSTRACT TRUNCATED AT 400 WORDS)

Published

1994

42. The insulin receptor and its substrate: molecular determinants of early events in insulin action.

Author

Kahn CR, White MF, Shoelson SE, Backer JM, Araki E, Cheatham B, Csermely P, Folli F, Goldstein BJ, and Huertas P

Subjects

Amino Acid Sequence, Animals, Humans, Molecular Sequence Data, Molecular Structure, Mutagenesis, Phosphotyrosine, Receptor, Insulin biosynthesis, Receptor, Insulin chemistry, Receptor, Insulin genetics, Tyrosine analogs & derivatives, Tyrosine metabolism, Insulin physiology, Receptor, Insulin physiology

Published

1993

43. Insulin stimulates tyrosine phosphorylation of multiple high molecular weight substrates in Fao hepatoma cells.

Author

Miralpeix M, Sun XJ, Backer JM, Myers MG Jr, Araki E, and White MF

Subjects

Amino Acid Sequence, Animals, Blotting, Western, In Vitro Techniques, Liver Neoplasms, Experimental, Molecular Sequence Data, Molecular Weight, Phosphatidylinositol 3-Kinases, Phosphoproteins chemistry, Phosphorylation, Phosphotransferases metabolism, Phosphotyrosine, Time Factors, Tumor Cells, Cultured, Tyrosine metabolism, Insulin pharmacology, Phosphoproteins metabolism, Protein-Tyrosine Kinases metabolism, Receptor, Insulin metabolism, Tyrosine analogs & derivatives

Abstract

Insulin rapidly stimulates tyrosine phosphorylation of cellular proteins which migrate between 165 and 190 kDa during SDS-PAGE. These proteins, collectively called pp185, were originally found in anti-phosphotyrosine antibody (alpha PY) immunoprecipitates from insulin-stimulated Fao rat hepatoma cells. Recently, we purified and cloned IRS-1, one of the phosphoproteins that binds to alpha PY and migrates near 180 kDa following insulin stimulation of rat liver [Sun, X. J., et al. (1991) Nature 352, 73-77]. IRS-1 and pp185 undergo tyrosine phosphorylation immediately after insulin stimulation and show an insulin dose response similar to that of insulin receptor autophosphorylation. However, IRS-1 was consistently 10 kDa smaller than the apparent molecular mass of pp185. The pp185 contained some immunoblottable IRS-1; however, cell lysates depleted of IRS-1 with anti-IRS-1 antibody still contained the high molecular weight forms of pp185 (HMW-pp185). Furthermore, the tryptic phosphopeptide map of IRS-1 was distinct from that of HMW-pp185, suggesting that at least two substrates migrate in this region during SDS-PAGE. Moreover, the phosphatidylinositol 3'-kinase and its 85-kDa associated protein (p85) bound to IRS-1 in Fao cells, but weakly or not at all to HMW-pp185. Our results show that Fao cells contain at least two insulin receptor substrates, IRS-1 and HMW-pp185, which may play unique roles in insulin signal transmission.

Published

1992

44. Replacement of lysine residue 1030 in the putative ATP-binding region of the insulin receptor abolishes insulin- and antibody-stimulated glucose uptake and receptor kinase activity.

Author

Ebina Y, Araki E, Taira M, Shimada F, Mori M, Craik CS, Siddle K, Pierce SB, Roth RA, and Rutter WJ

Subjects

Animals, Base Sequence, Binding Sites, Cell Line, Codon, Genetic Vectors, Insulin analogs & derivatives, Insulin metabolism, Kinetics, Protein-Tyrosine Kinases metabolism, Receptor, Insulin drug effects, Receptor, Insulin metabolism, Adenosine Triphosphate metabolism, Glucose metabolism, Insulin pharmacology, Lysine, Mutation, Protein-Tyrosine Kinases genetics, Receptor, Insulin genetics

Abstract

To test whether the tyrosine kinase activity of the insulin receptor is crucial for insulin action, we have constructed mutations of the human insulin receptor at Lys-1030, which is in the presumed ATP-binding region. By using oligonucleotide-directed mutagenesis, this lysine residue was replaced with either methionine, arginine, or alanine. Chinese hamster ovary cells were transfected by mutant cDNAs and the expressed insulin receptors were characterized. We show here that none of these mutants exhibited insulin-activated autophosphorylation and kinase activity in vitro. They also do not mediate insulin- and antibody-stimulated uptake of 2-deoxyglucose. The tyrosine kinase activity is thus required for a key physiological response of insulin.

Published

1987

45. The insulin receptor and its substrate: molecular determinants of early events in insulin action

Author

Cr, Kahn, Mf, White, Se, Shoelson, Jm, Backer, Araki E, Cheatham B, Csermely P, franco folli, Bj, Goldstein, and Huertas P

Subjects

Molecular Structure, Mutagenesis, Molecular Sequence Data, Animals, Humans, Insulin, Tyrosine, Amino Acid Sequence, Phosphotyrosine, Receptor, Insulin

Published

1993