InAADR

Drug Information

Drug Name: Troglitazone (97322-87-7)
PubChem ID: 5591
SMILES: CC1=C(C(=C2CCC(OC2=C1C)(C)COC3=CC=C(C=C3)CC4C(=O)NC(=O)S4)C)O
InchiKey: GXPHKUHSUJUWKP-UHFFFAOYSA-N
Therapeutic Category: Cytochrome P-450 CYP3A Inducers, Hypoglycemic Agents

Computed Drug Properties

Molecular Weight (dalton): 441.549
LogP: 4.37426
Ring Count: 2
Hydrogen Bond Acceptor Count: 6
Hydrogen Bond Donor Count: 2
Total Polar Surface Area: 84.86

This panel provides information on interacting drugs and their ADRs along with references

Interacting drug Toxicity Interaction Type Mechanism Reference

This panel provides drug-protein interaction and their ADRs along with references

Toxicity Interacting Protein Mechanism Reference
Beneficial For The Diabetic Heart Glucose transporter I (P11166) Troglitazone induced a dose-dependent increase in 2-deoxyglucose uptake reaching a 40-fold stimulation at 5 mumol/l@This was paralleled by a dose-dependent increase of Glucose transporter-1 (GLUT1) and GLUT4 protein expression;troglitazone exerts multiple effects on cardiomyocytes involving inhibition of PKC and regulation of Glucose transporter expression and distribution which may be beneficial for the diabetic heart and that modulation of PKC-activity could be relevant for improving insulin action in muscle tissue. [ ADR Type 1 ] Acute and chronic effects of troglitazone (CS-045) on isolated rat ventricular cardiomyocytes
Beneficial For The Diabetic Heart Glucose transporter-4 (P14672) Troglitazone induced a dose-dependent increase in 2-deoxyglucose uptake reaching a 40-fold stimulation at 5 mumol/l@This was paralleled by a dose-dependent increase of Glucose transporter-1 (GLUT1) and GLUT4 protein expression;troglitazone exerts multiple effects on cardiomyocytes involving inhibition of PKC and regulation of Glucose transporter expression and distribution which may be beneficial for the diabetic heart and that modulation of PKC-activity could be relevant for improving insulin action in muscle tissue [ ADR Type 1 ] Acute and chronic effects of troglitazone (CS-045) on isolated rat ventricular cardiomyocytes
Beneficial For The Diabetic Heart protein kinase-C (P00047) Troglitazone induced a dose-dependent increase in 2-deoxyglucose uptake reaching a 40-fold stimulation at 5 mumol/l,This was paralleled by a dose-dependent increase of Glucose transporter-1 (GLUT1) and GLUT4 protein expression;troglitazone exerts multiple effects on cardiomyocytes involving inhibition of PKC and regulation of Glucose transporter expression and distribution which may be beneficial for the diabetic heart and that modulation of PKC-activity could be relevant for improving insulin action in muscle tissue [ ADR Type 1 ] Acute and chronic effects of troglitazone (CS-045) on isolated rat ventricular cardiomyocytes
Hepatotoxicity Cytochrome P450 3A4 (P08684) The cytochrome P450 (CYP) inhibitors furafylline (CYP1A1/2)@ omeprazole (CYP2C19)@ ketoconazole (CYP3A4)@ and sulfaphenazole (CYP2C9) had no inhibitory effect on the TGZ metabolism suggesting that several P450s may play a role in the TGZ metabolic pathway [ ADR Type 2 ] Studies on the metabolism of troglitazone to reactive intermediates in vitro and in vivo Evidence for novel biotransformation pathways involving quinone
Obesity lipogenic transcription factor (P00029) mRNA of lipogenic enzymes ranged from 2 4- to 4 6-fold higher than lean controls,which may play a role in the ectopic lipogenesis and lipotoxicity complicating obesity in Zucker diabetic fatty rats [ ADR Type 1 ] Leptin, troglitazone, and the expression of sterol regulatory element binding proteins in liver and pancreatic islets
Obesity Sterol regulatory element-binding protein 1 (P36956) Hepatic SREBP-1 mRNA was 2.4 times higher than in lean +/+ controls@ primarily because of increased SREBP-1c expression@which may play a role in the ectopic lipogenesis and lipotoxicity complicating obesity in Zucker diabetic fatty rats. [ ADR Type 1 ] Leptin, troglitazone, and the expression of sterol regulatory element binding proteins in liver and pancreatic islets

This panel provides drug-food interactions and their ADRs along with references

Food Toxicity Reference

This panel provides information on metabolites and their ADRs along with references

Metabolite Toxicity Place of Metabolism Mechanism Reference

This panel provides information on drug category

Toxicity Source
Abdominal Discomfort MetaADEDB
Abdominal Pain ADReCS
Abdominal Pain MetaADEDB
Abnormal Ecg MetaADEDB
Abscess MetaADEDB
Accident MetaADEDB
Accidental Overdose MetaADEDB
Acute Kidney Failure MetaADEDB
Adenocarcinoma MetaADEDB
Adverse Drug Effect MetaADEDB
Afib MetaADEDB
Alanine Aminotransferase Increased SIDER
Allergic Dermatitis MetaADEDB
Anaemia ADReCS
Anaesthesia MetaADEDB
Angina MetaADEDB
Angina Unstable MetaADEDB
Angiopathy MetaADEDB
Angioplasty MetaADEDB
Anorexia ADReCS
Apathy MetaADEDB
Apoplexy MetaADEDB
Apparent Death MetaADEDB
Arrhythmia MetaADEDB
Arteriosclerosis MetaADEDB
Arteriosclerosis Coronary Artery MetaADEDB
Arteriosclerotic Heart Disease MetaADEDB
Asthenia ADReCS
Atrioventricular Block MetaADEDB
Atrioventricular Block Complete MetaADEDB
Autoimmune Hepatitis MetaADEDB
Azotaemia MetaADEDB
Bacterial Toxaemia MetaADEDB
Basedow Disease MetaADEDB
Blood Cholesterol MetaADEDB
Blood Creatine Phosphokinase Increased ADReCS
Blood Glucose Decreased MetaADEDB
Body Height Decreased MetaADEDB
Body Temperature Increased ADReCS
Bradycardia MetaADEDB
Brain Concussion MetaADEDB
Brain Damage MetaADEDB
Breast Lump MetaADEDB
Breast Microcalcification MetaADEDB
Bundle Branch Block Left MetaADEDB
Cardiac Decompensation MetaADEDB
Cardiac Disease MetaADEDB
Cardiac Enlargement MetaADEDB
Cardiac Failure ADReCS
Cardiac Failure Congestive ADReCS
Cardiac Ischemia MetaADEDB
Cardiomyopathy MetaADEDB
Cardiovascular Disorder MetaADEDB
Carpal Tunnel MetaADEDB
Cataract MetaADEDB
Cellulitis MetaADEDB
Chest Pain MetaADEDB
Choking Sensation MetaADEDB
Cholangiolitis MetaADEDB
Chronic Kidney Disease MetaADEDB
Circumstance Or Information Capable Of Leading To Medication Error MetaADEDB
Clotting MetaADEDB
Cold Sweat MetaADEDB
Confabulation MetaADEDB
Constipated MetaADEDB
Creatine Phosphokinase Increased SIDER
Deafness Congenital MetaADEDB
Decreased Appetite ADReCS
Deep Vein Thromboses MetaADEDB
Dehydration MetaADEDB
Demyelination MetaADEDB
Diabetes MetaADEDB
Diabetes Mellitus Inadequate Control MetaADEDB
Diabetes Mellitus Insulin-Dependent MetaADEDB
Diabetic Foot MetaADEDB
Diabetic Foot Infection MetaADEDB
Diabetic Gangrene MetaADEDB
Diabetic Gastroparesis MetaADEDB
Diabetic Hyperosmolar Coma MetaADEDB
Diabetic Neuropathy MetaADEDB
Diabetic Ulcer MetaADEDB
Diabetic Vascular Disorder MetaADEDB
Diarrhea MetaADEDB
Difficulty In Walking MetaADEDB
Discomfort ADReCS
Disorder Peripheral Vascular MetaADEDB
Diverticulitis MetaADEDB
Diverticulum MetaADEDB
Dizziness ADReCS
Drug Dispensing Error MetaADEDB
Drug Hypersensitivity MetaADEDB
Drug Toxicity MetaADEDB
Dyslipidaemia MetaADEDB
Dysstasia MetaADEDB
Dysthymic Disorder MetaADEDB
Economic Problem MetaADEDB
Electrocardiogram T Wave Abnormal MetaADEDB
Electromechanical Dissociation MetaADEDB
Embolism Pulmonary MetaADEDB
Encephalitis Allergic MetaADEDB
Encephalopathy MetaADEDB
Enlarged Liver MetaADEDB
Escherichia Urinary Tract Infection MetaADEDB
Esophageal Stenosis MetaADEDB
Excess Potassium MetaADEDB
Face Injury MetaADEDB
Facial Bones Fracture MetaADEDB
Fatigue ADReCS
Feeling Abnormal ADReCS
Fluid Intake Reduced MetaADEDB
Gastric Disorder MetaADEDB
Gastrointestinal Disorder MetaADEDB
Gastrointestinal Pain ADReCS
General Physical Health Deterioration MetaADEDB
Glomerulosclerosis MetaADEDB
Glycosylated Haemoglobin Increased MetaADEDB
Haemodialysis MetaADEDB
Heart Attack MetaADEDB
Heart Injury MetaADEDB
Heart Rate Increased MetaADEDB
Hepatic Failure MetaADEDB
Hepatic Fibrosis MetaADEDB
Hepatic Function Abnormal ADReCS
Hepatitis ADReCS
Hepatocellular Damage MetaADEDB
Hepatotoxicity MetaADEDB
Hesitancy MetaADEDB
Hyperglycaemia ADReCS
Hypophagia MetaADEDB
Hypovolaemia MetaADEDB
Ill-Defined Disorder ADReCS
Impaired Gastric Emptying MetaADEDB
Incontinence MetaADEDB
Infection Urinary Tract MetaADEDB
Intention Tremor MetaADEDB
International Normalised Ratio Increased MetaADEDB
Ischaemic Cardiomyopathy MetaADEDB
Jaundice ADReCS
Kidney Failure MetaADEDB
Kidney Fibrosis MetaADEDB
Laboratory Test Abnormal ADReCS
Leg Amputation MetaADEDB
Liver Function Test Abnormal ADReCS
Liver Transplant MetaADEDB
Loss Of Consciousness ADReCS
Lumbar Vertebral Fracture MetaADEDB
Lung Edema MetaADEDB
Lung Neoplasm Malignant MetaADEDB
Malaise ADReCS
Multiple Injuries MetaADEDB
Muscle Necrosis MetaADEDB
Muscle Weakness MetaADEDB
Nausea ADReCS
Neuropathy Peripheral MetaADEDB
Oedema ADReCS
Pain ADReCS
Palpitation MetaADEDB
Paranasal Sinus Hypersecretion MetaADEDB
Pedal Pulse Absent MetaADEDB
Pericardial Effusion MetaADEDB
Pericarditis MetaADEDB
Pharmaceutical Product Complaint MetaADEDB
Pleural Effusion MetaADEDB
Postoperative Infection MetaADEDB
Prescribed Overdose MetaADEDB
Prothrombin Time Prolonged MetaADEDB
Rash Generalised MetaADEDB
Reflux Esophagitis MetaADEDB
Renal Atrophy MetaADEDB
Renal Cyst MetaADEDB
Renal Tubular Atrophy MetaADEDB
Renal Tubular Necrosis MetaADEDB
Shock ADReCS
Small Intestinal Obstruction MetaADEDB
Social Avoidant Behaviour ADReCS
Spinal Compression Fracture MetaADEDB
Stevens-Johnson Syndrome MetaADEDB
Swollen Tongue MetaADEDB
Syncope ADReCS
Throat Tightness MetaADEDB
Unevaluable Event MetaADEDB
Upper Limb Fracture MetaADEDB
Volume Blood Increased ADReCS
Volume Plasma Increased SIDER
Vomiting ADReCS
Weight Gain MetaADEDB
Weight Increased ADReCS
Withdrawn SIDER
Wound Abscess MetaADEDB

InAADR: Drug-Protein-ADRs database