Your search keyword '"Pentanoic Acids adverse effects"' showing total 41 results

1. Emricasan to prevent new decompensation in patients with NASH-related decompensated cirrhosis.

Author

Frenette C, Kayali Z, Mena E, Mantry PS, Lucas KJ, Neff G, Rodriguez M, Thuluvath PJ, Weinberg E, Bhandari BR, Robinson J, Wedick N, Chan JL, Hagerty DT, and Kowdley KV

Subjects

Caspase Inhibitors administration & dosage, Caspase Inhibitors adverse effects, Disease Progression, Drug Monitoring methods, End Stage Liver Disease etiology, End Stage Liver Disease prevention & control, Esophageal and Gastric Varices etiology, Esophageal and Gastric Varices physiopathology, Female, Humans, Male, Middle Aged, Treatment Outcome, Ascites etiology, Ascites prevention & control, Gastrointestinal Hemorrhage etiology, Gastrointestinal Hemorrhage prevention & control, Hepatic Encephalopathy etiology, Hepatic Encephalopathy prevention & control, Liver Cirrhosis blood, Liver Cirrhosis drug therapy, Liver Cirrhosis etiology, Liver Cirrhosis mortality, Liver Function Tests methods, Non-alcoholic Fatty Liver Disease complications, Non-alcoholic Fatty Liver Disease diagnosis, Pentanoic Acids administration & dosage, Pentanoic Acids adverse effects, Peritonitis etiology, Peritonitis prevention & control

Abstract

Background & Aims: Non-alcoholic steatohepatitis is a leading cause of end-stage liver disease. Hepatic steatosis and lipotoxicity cause chronic necroinflammation and direct hepatocellular injury resulting in cirrhosis, end-stage liver disease and hepatocellular carcinoma. Emricasan is a pan-caspase inhibitor that inhibits excessive apoptosis and inflammation; it has also been shown to decrease portal pressure and improve synthetic function in mice with carbon tetrachloride-induced cirrhosis., Methods: This double-blind, placebo-controlled study randomized 217 individuals with decompensated NASH cirrhosis 1:1:1 to emricasan (5 mg or 25 mg) or placebo. Patients were stratified by decompensation status and baseline model for end-stage liver disease-sodium (MELD-Na) score. The primary endpoint comprised all-cause mortality, a new decompensation event (new or recurrent variceal hemorrhage, new ascites requiring diuretics, new unprecipitated hepatic encephalopathy ≥grade 2, hepatorenal syndrome, spontaneous bacterial peritonitis), or an increase in MELD-Na score ≥4 points., Results: There was no difference in event rates between either of the emricasan treatment groups and placebo, with hazard ratios of 1.02 (95% CI 0.59-1.77; p = 0.94) and 1.28 (95% CI 0.75-2.21; p = 0.37) for 5 mg and 25 mg of emricasan, respectively. MELD-Na score progression was the most common outcome. There was no significant effect of emricasan treatment on MELD-Na score, international normalized ratio, total serum bilirubin, albumin level or Child-Pugh score. Emricasan was generally safe and well-tolerated., Conclusions: Emricasan was safe but ineffective for the treatment of decompensated NASH cirrhosis. However, this study may guide the design and conduct of future clinical trials in decompensated NASH cirrhosis., Lay Summary: Patients with decompensated cirrhosis related to non-alcoholic steatohepatitis are at high risk of additional decompensation events and death. Post hoc analyses in previous pilot studies suggested that emricasan might improve portal hypertension and liver function. In this larger randomized study, emricasan did not decrease the number of decompensation events or improve liver function in patients with a history of decompensated cirrhosis related to non-alcoholic steatohepatitis. CLINICALTRIALS., Gov Identifier: NCT03205345., Competing Interests: Conflict of interest James Robinson, Jean L. Chan and David Hagerty were employees of Conatus Pharmaceuticals, Inc., during the conduct of the study. Nicole Wedick was a consultant employed by Conatus Pharmaceuticals, Inc., and reports personal fees from SimulStat, Inc., during the conduct of the study. Catherine Frenette reports research funding from Conatus Pharmaceuticals, Inc., during the conduct of this study and personal fees from Conatus Pharmaceuticals, Inc., outside of the submitted work. Kris Kowdley reports grants from Conatus Pharmaceuticals, Inc., during the conduct of the study; personal fees from Abbvie, Gilead and Intercept, outside of the submitted work; grants from Enanta, Genfit, Gilead, CymaBay, HighTide, Intercept, Allergan and LaJolla, outside of the submitted work; royalties from UpToDate, outside of the submitted work. Kris Kowdley was on the Advisory Board of Assembly Biosciences, Blade, Enanta, Genefit, Gillead, CymaBay and Merck and was a consultant for HighTide and Intercept, outside of the submitted work. Guy Neff reports grants from Echosens and personal fees from Intercept, outside the submitted work. Parvez Mantry reports personal fees from Gilead, Intercept, Salix, Eisai, Abbvie and grants from Allergan, Genfit, Bristol-Myers, Galmed, Viking, Pfizer, Merck, outside the submitted work. Ethan Weinberg reports personal fees from Mallinckrodt Pharmaceuticals and from Sequana, outside the submitted work. Please refer to the accompanying ICMJE disclosure forms for further details., (Copyright © 2020 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.)

Published

2021

2. Randomized placebo-controlled trial of emricasan for non-alcoholic steatohepatitis-related cirrhosis with severe portal hypertension.

Author

Garcia-Tsao G, Bosch J, Kayali Z, Harrison SA, Abdelmalek MF, Lawitz E, Satapathy SK, Ghabril M, Shiffman ML, Younes ZH, Thuluvath PJ, Berzigotti A, Albillos A, Robinson JM, Hagerty DT, Chan JL, and Sanyal AJ

Subjects

Administration, Oral, Aged, Biomarkers blood, Caspase Inhibitors adverse effects, Double-Blind Method, Female, Follow-Up Studies, Humans, Hypertension, Portal blood, Liver Cirrhosis blood, Male, Middle Aged, Non-alcoholic Fatty Liver Disease blood, Pentanoic Acids adverse effects, Portal Pressure drug effects, Prospective Studies, Treatment Outcome, Caspase Inhibitors administration & dosage, Hypertension, Portal complications, Hypertension, Portal drug therapy, Liver Cirrhosis complications, Non-alcoholic Fatty Liver Disease complications, Pentanoic Acids administration & dosage, Severity of Illness Index

Abstract

Background & Aims: Emricasan, an oral pan-caspase inhibitor, decreased portal pressure in experimental cirrhosis and in an open-label study in patients with cirrhosis and severe portal hypertension, defined as a hepatic venous pressure gradient (HVPG) ≥12 mmHg. We aimed to confirm these results in a placebo-controlled study in patients with non-alcoholic steatohepatitis (NASH)-related cirrhosis., Methods: We performed a multicenter double-blinded study, randomizing 263 patients with NASH-related cirrhosis and baseline HVPG ≥12 mmHg to twice daily oral emricasan 5 mg, 25 mg, 50 mg or placebo in a 1:1:1:1 ratio for up to 48 weeks. The primary endpoint was change in HVPG (ΔHVPG) at week 24. Secondary endpoints were changes in biomarkers (aminotransferases, caspases, cytokeratins) and development of liver-related outcomes., Results: There were no significant differences in ΔHVPG for any emricasan dose vs. placebo (-0.21, -0.45, -0.58 mmHg, respectively) adjusted for baseline HVPG, compensation status, and non-selective beta-blocker use. Compensated patients (n = 201 [76%]) tended to have a greater decrease in HVPG (emricasan all vs. placebo, p = 0.06), the decrease being greater in those with higher baseline HVPG (p = 0.018), with a significant interaction between baseline HVPG (continuous, p = 0.024; dichotomous at 16 mmHg [median], p = 0.013) and treatment. Biomarkers decreased significantly with emricasan at week 24 but returned to baseline levels by week 48. New or worsening decompensating events (∼10% over median exposure of 337 days), progression in model for end-stage liver disease and Child-Pugh scores, and treatment-emergent adverse events were similar among treatment groups., Conclusions: Despite a reduction in biomarkers indicating target engagement, emricasan was not associated with improvement in HVPG or clinical outcomes in patients with NASH-related cirrhosis and severe portal hypertension. Compensated patients with higher baseline HVPG had evidence of a small treatment effect. Emricasan treatment appeared safe and well-tolerated., Lay Summary: Cirrhosis (scarring of the liver) is the main consequence of non-alcoholic steatohepatitis (NASH). Cirrhosis leads to high pressure in the portal vein which accounts for most of the complications of cirrhosis. Reducing portal pressure is beneficial in patients with cirrhosis. We studied the possibility that emricasan, a drug that improves inflammation and scarring in the liver, would reduce portal pressure in patients with NASH-related cirrhosis and severe portal hypertension. Our results in a large, prospective, double-blind study could not demonstrate a beneficial effect of emricasan in these patients., Clinical Trial Number: Clinical Trials.gov #NCT02960204., Competing Interests: Conflict of interest Jean L. Chan, James Robinson, and David T. Hagerty are employees of Conatus Pharmaceuticals. Please refer to the accompanying ICMJE disclosure forms for further details., (Copyright © 2019 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.)

Published

2020

3. Hypocarnitinemia Observed in an Infant Treated with Short-Term Administration of Antibiotic Containing Pivalic Acid.

Author

Nakazaki K, Ogawa E, Ishige M, Ishige N, Fuchigami T, and Takahashi S

Subjects

Carbon chemistry, Carnitine analogs & derivatives, Humans, Hypoglycemia diagnosis, Infant, Male, Oxygen chemistry, Tandem Mass Spectrometry, Anti-Bacterial Agents adverse effects, Carnitine blood, Carnitine urine, Metabolic Diseases chemically induced, Metabolic Diseases diagnosis, Pentanoic Acids adverse effects

Abstract

Carnitine is a water-soluble amino acid derivative required for β-oxidation of long-chain fatty acids. In carnitine cycle abnormalities and low carnitine states, fatty acid β-oxidation is inhibited during fasting, resulting in hypoglycemia. Pivalic acid is a substance used in prodrugs to increase absorption of parent drugs, and antibiotics containing pivalic acid are frequently used as wide spectrum antibiotics for pediatric patients in Japan. Pivalic acid released after absorption is conjugated with free carnitine to form pivaloylcarnitine, which is then excreted in urine. As a consequence, long-term administration of pivalic acid containing antibiotics has been associated with depletion of free carnitine, inhibition of energy production and subsequent hypoglycemia. Here we report a case of a 23-month-old boy treated with an antibiotic containing pivalic acid for 3 days for upper respiratory tract infection. Laboratory data at referral indicated hypoglycemia, decreased free carnitine and elevated five-carbon acylcarnitine. Isomer separation confirmed the major component of increased five-carbon acylcarnitine to be pivaloylcarnitine, thereby excluding the possibility of a genetic metabolic disorder detected with similar acylcarnitine profile. The level of carnitine was normal when the antibiotic was not administered. Our case shows that the use of antibiotics containing pivalic acid in young children requires consideration of hypocarnitinemia, even with short-term administration.

Published

2018

4. Newborn hypocarnitinemia due to long-term transplacental pivalic acid passage.

Author

Nasu T, Suzuki M, Uetake K, and Kubota M

Subjects

Carnitine blood, Female, Humans, Infant, Newborn, Male, Pregnancy, Time Factors, Carnitine deficiency, Maternal-Fetal Exchange, Metabolism, Inborn Errors chemically induced, Pentanoic Acids adverse effects

Abstract

Infants often develop hypocarnitinemia and resultant hypoglycemia during long-term treatment with antibiotics that contain pivalic acid, but it is unknown whether maternal treatment with such agents during pregnancy induces hypocarnitinemia in fetuses or neonates. A woman at week 28 of pregnancy was prescribed cefcapene pivoxil for 84 consecutive days for treatment and prophylaxis of pyelonephritis. Using tandem mass spectrometry, both the mother and newborn were found to have hypocarnitinemia soon after delivery. It was concluded that the baby suffered from secondary hypocarnitinemia due to long-term prenatal treatment with antibiotics containing pivalic acid. Long-term treatment with antibiotics containing pivalic acid in pregnant women can induce hypocarnitinemia in both the mother and neonate; reported herein is the first case observed in humans., (© 2014 Japan Pediatric Society.)

Published

2014

5. Efficacy, safety and tolerability of GSK2190915, a 5-lipoxygenase activating protein inhibitor, in adults and adolescents with persistent asthma: a randomised dose-ranging study.

Author

Follows RM, Snowise NG, Ho SY, Ambery CL, Smart K, and McQuade BA

Subjects

5-Lipoxygenase-Activating Protein Inhibitors administration & dosage, 5-Lipoxygenase-Activating Protein Inhibitors adverse effects, Adolescent, Adrenergic beta-2 Receptor Agonists therapeutic use, Adult, Aged, Anti-Asthmatic Agents administration & dosage, Anti-Asthmatic Agents adverse effects, Child, Dose-Response Relationship, Drug, Double-Blind Method, Female, Forced Expiratory Volume, Humans, Indoles administration & dosage, Indoles adverse effects, Male, Middle Aged, Pentanoic Acids administration & dosage, Pentanoic Acids adverse effects, Smoking adverse effects, Treatment Outcome, Young Adult, 5-Lipoxygenase-Activating Protein Inhibitors therapeutic use, Anti-Asthmatic Agents therapeutic use, Asthma drug therapy, Indoles therapeutic use, Pentanoic Acids therapeutic use

Abstract

Background: GSK2190915 is a high affinity 5-lipoxygenase-activating protein inhibitor being developed for the treatment of asthma. The objective of this study was to evaluate GSK2190915 efficacy, dose-response and safety in subjects with persistent asthma treated with short-acting beta2-agonists (SABAs) only., Methods: Eight-week multicentre, randomised, double-blind, double-dummy, stratified (by age and smoking status), parallel-group, placebo-controlled study in subjects aged ≥12 years with a forced expiratory volume in 1 second (FEV1) of 50-85% predicted. Subjects (n = 700) were randomised to receive once-daily (QD) oral GSK2190915 (10-300 mg), twice-daily inhaled fluticasone propionate 100 μg, oral montelukast 10 mg QD or placebo. The primary endpoint was mean change from baseline (randomisation) in trough (morning pre-dose and pre-rescue bronchodilator) FEV1 at the end of the 8-week treatment period. Secondary endpoints included morning and evening peak expiratory flow, symptom-free days and nights, rescue-free days and nights, day and night-time symptom scores, day and night-time rescue medication use, withdrawals due to lack of efficacy, Asthma Control Questionnaire and Asthma Quality of Life Questionnaire scores., Results: For the primary endpoint, there was no statistically significant difference between any dose of GSK2190915 QD and placebo. However, repeated measures sensitivity analysis demonstrated nominal statistical significance for GSK2190915 30 mg QD compared with placebo (mean difference: 0.115 L [95% confidence interval: 0.00, 0.23], p = 0.044); no nominally statistically significant differences were observed with any of the other doses. For the secondary endpoints, decreases were observed in day-time symptom scores and day-time SABA use for GSK2190915 30 mg QD versus placebo (p ≤ 0.05). No dose-response relationship was observed for the primary and secondary endpoints across the GSK2190915 dose range studied; the 10 mg dose appeared to be sub-optimal. GSK2190915 was associated with a dose-dependent reduction in urinary leukotriene E4. The profile and incidence of adverse events were similar between treatment groups., Conclusion: Efficacy was demonstrated for GSK2190915 30 mg compared with placebo in day-time symptom scores and day-time SABA use. No additional improvement on efficacy endpoints was gained by administration of GSK2190915 doses greater than 30 mg. GSK2190915 was well-tolerated. These results may support further studies with GSK2190915 30 mg., Trial Registration: Clinicaltrials.gov: NCT01147744.

Published

2013

6. Pharmacodynamics, pharmacokinetics and safety of GSK2190915, a novel oral anti-inflammatory 5-lipoxygenase-activating protein inhibitor.

Author

Bain G, King CD, Schaab K, Rewolinski M, Norris V, Ambery C, Bentley J, Yamada M, Santini AM, van de Wetering de Rooij J, Stock N, Zunic J, Hutchinson JH, and Evans JF

Subjects

Administration, Oral, Adolescent, Adult, Aged, Area Under Curve, Asian People, Biomarkers blood, Biomarkers urine, Cross-Over Studies, Dose-Response Relationship, Drug, Double-Blind Method, Female, Humans, Leukotriene B4 blood, Leukotriene B4 urine, Leukotriene E4 urine, Male, Middle Aged, White People, Young Adult, 5-Lipoxygenase-Activating Protein Inhibitors adverse effects, 5-Lipoxygenase-Activating Protein Inhibitors pharmacokinetics, 5-Lipoxygenase-Activating Protein Inhibitors pharmacology, Indoles adverse effects, Indoles pharmacokinetics, Indoles pharmacology, Leukotriene E4 blood, Pentanoic Acids adverse effects, Pentanoic Acids pharmacokinetics, Pentanoic Acids pharmacology

Abstract

Aim: To assess the pharmacokinetics, pharmacodynamics, safety and tolerability of the 5-lipoxygenase-activating protein inhibitor, GSK2190915, after oral dosing in two independent phase I studies, one in Western European and one in Japanese subjects, utilizing different formulations., Method: Western European subjects received single (50-1000 mg) or multiple (10-450 mg) oral doses of GSK2190915 or placebo in a dose-escalating manner. Japanese subjects received three of four GSK2190915 doses (10-200 mg) plus placebo once in a four period crossover design. Blood samples were collected for GSK2190915 concentrations and blood and urine were collected to measure leukotriene B₄ and leukotriene E₄, respectively, as pharmacodynamic markers of drug activity., Results: There was no clear difference in adverse events between placebo and active drug-treated subjects in either study. Maximum plasma concentrations of GSK2190915 and area under the curve increased in a dose-related manner and mean half-life values ranged from 16-34 h. Dose-dependent inhibition of blood leukotriene B₄ production was observed and near complete inhibition of urinary leukotriene E₄ excretion was shown at all doses except the lowest dose. The EC₅₀ values for inhibition of LTB₄ were 85 nM and 89 nM in the Western European and Japanese studies, respectively., Conclusion: GSK2190915 is well-tolerated with pharmacokinetics and pharmacodynamics in Western European and Japanese subjects that support once daily dosing for 24 h inhibition of leukotrienes. Doses of ≥50 mg show near complete inhibition of urinary leukotriene E₄ at 24 h post-dose, whereas doses of ≥150 mg are required for 24 h inhibition of blood LTB₄., (© 2012 GlaxoSmithKline. British Journal of Clinical Pharmacology © 2012 The British Pharmacological Society.)

Published

2013

7. Primary carnitine deficiency and pivalic acid exposure causing encephalopathy and fatal cardiac events.

Author

Rasmussen J, Nielsen OW, Lund AM, Køber L, and Djurhuus H

Subjects

Adult, Anti-Bacterial Agents adverse effects, Carnitine metabolism, Child, Preschool, Female, Humans, Infant, Retrospective Studies, Arrhythmias, Cardiac etiology, Cardiomyopathies complications, Carnitine deficiency, Death, Sudden, Cardiac etiology, Hyperammonemia complications, Muscular Diseases complications, Pentanoic Acids adverse effects

Abstract

Background: Several episodes of sudden death among young Faroese individuals have been associated with primary carnitine deficiency (PCD). Patients suffering from PCD have low carnitine levels and can present with metabolic and/or cardiac complications. Pivalic acid exposure decreases carnitine levels. The purpose of this study was to investigate and describe the association and pathophysiology of exposure to antibiotics containing pivalic acid and severe neurological and cardiac complications in six identified subjects suffering from PCD., Methods and Materials: Six cases of PCD were identified and studied through medical records and family interview. Stored biomaterial was analyzed for mutations causing PCD., Results: Five patients (two children, three adults) died suddenly while one adult patient survived sudden cardiac arrest. Lethal cardiac arrhythmia was documented in five patients, while one patient was not monitored at time of death, but had signs of cardiac arrhythmia a few days earlier. All patients suffered encephalopathy before cardiac arrhythmia. Autopsy showed severe hepatic steatosis and signs of cerebral edema in four out of five. One subject had a dilated heart. All patients were homozygous for the c.95A>G (p.N32S) mutation in SLC22A5 causing PCD. All patients had been treated with antibiotics containing pivalic acid prior to the episode., Conclusion: Exposure to antibiotics containing pivalic acid was associated with encephalopathy and progression to lethal cardiac arrhythmia in patients suffering from PCD.

Published

2013

8. Metabolism of levulinate in perfused rat livers and live rats: conversion to the drug of abuse 4-hydroxypentanoate.

Author

Harris SR, Zhang GF, Sadhukhan S, Murphy AM, Tomcik KA, Vazquez EJ, Anderson VE, Tochtrop GP, and Brunengraber H

Subjects

Animals, Central Nervous System Depressants pharmacology, Cytoplasm enzymology, Enzyme Inhibitors adverse effects, Enzyme Inhibitors pharmacology, Ethanol pharmacology, Levulinic Acids adverse effects, Levulinic Acids pharmacology, Male, Mitochondria, Liver enzymology, Oxidation-Reduction, Pentanoic Acids adverse effects, Perfusion, Rats, Rats, Sprague-Dawley, Calcium pharmacology, Enzyme Inhibitors pharmacokinetics, Levulinic Acids pharmacokinetics, Liver enzymology, Pentanoic Acids metabolism, Substance-Related Disorders

Abstract

Calcium levulinate (4-ketopentanoate) is used as an oral and parenteral source of calcium. We hypothesized that levulinate is converted in the liver to 4-hydroxypentanoate, a new drug of abuse, and that this conversion is accelerated by ethanol oxidation. We confirmed these hypotheses in live rats, perfused rat livers, and liver subcellular preparations. Levulinate is reduced to (R)-4-hydroxypentanoate by a cytosolic and a mitochondrial dehydrogenase, which are NADPH- and NADH-dependent, respectively. A mitochondrial dehydrogenase or racemase system also forms (S)-4-hydroxypentanoate. In livers perfused with [(13)C(5)]levulinate, there was substantial CoA trapping in levulinyl-CoA, 4-hydroxypentanoyl-CoA, and 4-phosphopentanoyl-CoA. This CoA trapping was increased by ethanol, with a 6-fold increase in the concentration of 4-phosphopentanoyl-CoA. Levulinate is catabolized by 3 parallel pathways to propionyl-CoA, acetyl-CoA, and lactate. Most intermediates of the 3 pathways were identified by mass isotopomer analysis and metabolomics. The production of 4-hydroxypentanoate from levulinate and its stimulation by ethanol is a potential public health concern.

Published

2011

9. Clinical trial: the efficacy and safety of oral PF-03491390, a pancaspase inhibitor - a randomized placebo-controlled study in patients with chronic hepatitis C.

Author

Shiffman ML, Pockros P, McHutchison JG, Schiff ER, Morris M, and Burgess G

Subjects

Adult, Aged, Double-Blind Method, Female, Humans, Male, Middle Aged, Pentanoic Acids adverse effects, Treatment Outcome, Alanine Transaminase blood, Aspartate Aminotransferases blood, Caspase Inhibitors, Hepatitis C, Chronic drug therapy, Pentanoic Acids administration & dosage

Abstract

Background: Elevated serum levels of aspartate aminotransferase (AST) and alanine aminotransferase (ALT) reflect hepatocellular injury in patients with chronic hepatitis C virus (HCV). Increased apoptosis and activated caspases are present in these patients. PF-03491390 inhibits multiple caspases and lowers serum AST and ALT levels in patients with chronic liver diseases., Aim: To determine if treatment with an oral pancaspase inhibitor could reduce serum AST and ALT in patients with HCV., Methods: Double-blind, randomized, placebo-controlled, parallel-dose study in 204 patients treated with placebo or PF-03491390 (5, 25 or 50 mg) orally twice daily (b.d.) for up to 12 weeks. Serum AST and ALT were monitored weekly., Results: Significant reductions in serum AST and ALT were observed within 1 week of initiating PF-03491390 in all treatment groups (P < 0.0001). These reductions in AST and ALT were maintained throughout the 12 week treatment period and returned to baseline levels when PF-03491390 was discontinued. Increasing the dose did not further lower AST or ALT. The most frequently reported adverse events were headache and fatigue., Conclusion: PF-03491390 significantly reduced serum AST and ALT levels in patients with chronic HCV, and was well tolerated over 12 weeks.

Published

2010

10. Carnitine-associated encephalopathy caused by long-term treatment with an antibiotic containing pivalic acid.

Author

Makino Y, Sugiura T, Ito T, Sugiyama N, and Koyama N

Subjects

Acidosis chemically induced, Acidosis drug therapy, Anti-Bacterial Agents chemistry, Brain Diseases, Metabolic drug therapy, Carnitine blood, Carnitine therapeutic use, Cephalosporins chemistry, Humans, Hypoglycemia chemically induced, Infant, Infusions, Intravenous, Male, Otitis Media drug therapy, Pentanoic Acids analysis, Seizures chemically induced, Unconsciousness chemically induced, Vitamin B Complex therapeutic use, Anti-Bacterial Agents adverse effects, Brain Diseases, Metabolic chemically induced, Carnitine deficiency, Cephalosporins adverse effects, Pentanoic Acids adverse effects

Abstract

An 18-month-old boy was treated with an antibiotic containing pivalic acid for 6 months for intractable otitis media and then developed repeated convulsions and loss of consciousness. Laboratory data showed hypoglycemia and hypocarnitinemia. Intravenous administration of glucose was ineffective against the seizures and loss of consciousness. However, the patient regained consciousness and recovered soon after intravenous infusion of carnitine. To our knowledge, intravenous carnitine administration that contributed to marked improvements in neurologic deficit caused by administration of an antibiotic containing pivalic acid has not been reported previously. These findings indicate that long-term use of such antibiotics should be avoided.

Published

2007

11. Oral IDN-6556, an antiapoptotic caspase inhibitor, may lower aminotransferase activity in patients with chronic hepatitis C.

Author

Pockros PJ, Schiff ER, Shiffman ML, McHutchison JG, Gish RG, Afdhal NH, Makhviladze M, Huyghe M, Hecht D, Oltersdorf T, and Shapiro DA

Subjects

Administration, Oral, Double-Blind Method, Female, Hepatitis C, Chronic enzymology, Hepatitis C, Chronic virology, Humans, Male, Middle Aged, Pentanoic Acids administration & dosage, Pentanoic Acids adverse effects, RNA, Viral blood, Alanine Transaminase blood, Apoptosis drug effects, Aspartate Aminotransferases blood, Caspase Inhibitors, Enzyme Inhibitors therapeutic use, Hepatitis C, Chronic drug therapy, Pentanoic Acids therapeutic use

Abstract

Unlabelled: Increased rates of apoptosis (programmed cell death) have been demonstrated in many hepatic diseases including chronic hepatitis C. IDN-6556 is a potent inhibitor of caspases, the proteases that execute apoptosis. In a prior phase 1 study, IDN-6556 lowered aminotransferase activity in a small number of patients with liver impairment. The purpose of this study was to further explore the effect of IDN-6556 in patients with liver disease in a multicenter, double-blind, placebo-controlled, dose-ranging study with a 14-day dosing period. A total of 105 patients were enrolled in the study; 79 received active drug; 80 patients had chronic hepatitis C and 25 had other liver diseases including nonalcoholic steatohepatitis (NASH), hepatitis B, primary biliary cirrhosis (PBC), and primary sclerosing cholangitis (PSC). IDN-6556 doses ranged from 5 mg to 400 mg daily, given from 1 to 3 times per day. In the HCV patients, all doses of IDN-6556 significantly lowered ALT and AST (P = 0.0041 to P < 0.0001 for various dosing groups in Wilcoxon tests comparing IDN-6556 to placebo), with the exception of the lowest dose. Declines in aminotransferase activity were also seen in patients with NASH but effects were not apparent in the small number of other liver diseases. Adverse experiences were not different between IDN-6556 and placebo. There were no clinically meaningful changes in other laboratory parameters. In particular, mean HCV RNA levels did not show significant changes., Conclusion: Oral IDN-6556, given for 14 days, significantly lowered aminotransferase activity in HCV patients and appeared to be well tolerated. Longer studies to assess potential effects of IDN-6556 on liver inflammation and fibrosis are merited.

Published

2007

12. The single-dose pharmacokinetics of the novel CCK1 receptor antagonist, dexloxiglumide, are not influenced by age and gender.

Author

Roy P, Wangsa J, Patel A, Nolting A, Persiani S, Abramowitz W, and Kapil R

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Area Under Curve, Female, Half-Life, Humans, Male, Pentanoic Acids adverse effects, Pentanoic Acids blood, Pentanoic Acids pharmacokinetics, Receptor, Cholecystokinin A antagonists & inhibitors

Abstract

Objective: The effects of age and gender on the single-dose pharmacokinetics of dexloxiglumide, a selective cholecystokinin (CCK1-subtype) receptor antagonist, were assessed in healthy young and elderly male and female subjects., Methods: In total, 24 males and 24 females (12 young and 12 elderly subjects per gender group) received a single oral dose of 200 mg dexloxiglumide under fasted conditions. Mean (range) ages were 23.8 (18 - 32) and 71.3 (66 - 88) years for young and elderly subjects, respectively. Analysis of covariance (ANCOVA) with age group and gender as factors and body weight as a covariate was performed on the dexloxiglumide pharmacokinetic parameters of peak plasma concentration (C(max)) and the area under the plasma concentration-time curve (AUC). The p values obtained from ANCOVA were considered for the assessment of age and gender effects., Results: A small (approximately 18%) but statistically significant (p < or = 0.036) increase in the area under the plasma concentration-time curve from 0 to time of last quantifiable concentration (AUC(0-t) and the area under the plasma concentration-time curve from 0 to infinity (AUC(0-infinity)) in elderly compared to young subjects was noted. Given the lack of age effects on the other pharmacokinetic parameters of dexloxiglumide, this limited difference is unlikely to be clinically relevant. Without the adjustment for body weights, female subjects exhibited mean C(max) and AUC values approximately 26% and 36% higher than male subjects; however, these exposure differences did not reach statistical significance (p > 0.05) following ANCOVA analysis with body weight as a covariate. Likewise, there were no statistically significant differences (p > 0.05) observed for any other pharmacokinetic parameters between young and elderly and between male and female groups., Conclusions: Dose adjustments based on age and gender are not necessary. Dexloxiglumide administration was safe and well tolerated in these subjects.

Published

2005

13. Carnitine deficiency disorders in children.

Author

Stanley CA

Subjects

Anti-Bacterial Agents adverse effects, Carnitine metabolism, Child, Preschool, Fatty Acids metabolism, Humans, Mutation, Organic Cation Transport Proteins deficiency, Organic Cation Transport Proteins genetics, Oxidation-Reduction, Pentanoic Acids adverse effects, Solute Carrier Family 22 Member 5, Carnitine deficiency

Abstract

Mitochondrial oxidation of long-chain fatty acids provides an important source of energy for the heart as well as for skeletal muscle during prolonged aerobic work and for hepatic ketogenesis during long-term fasting. The carnitine shuttle is responsible for transferring long-chain fatty acids across the barrier of the inner mitochondrial membrane to gain access to the enzymes of beta-oxidation. The shuttle consists of three enzymes (carnitine palmitoyltransferase 1, carnitine acylcarnitine translocase, carnitine palmitoyl-transferase 2) and a small, soluble molecule, carnitine, to transport fatty acids as their long-chain fatty acylcarnitine esters. Carnitine is provided in the diet (animal protein) and also synthesized at low rates from trimethyl-lysine residues generated during protein catabolism. Carnitine turnover rates (300-500 micromol/day) are <1% of body stores; 98% of carnitine stores are intracellular (total carnitine levels are 40-50 microM in plasma vs. 2-3 mM in tissue). Carnitine is removed by urinary excretion after reabsorption of 98% of the filtered load; the renal carnitine threshold determines plasma concentrations and total body carnitine stores. Because of its key role in fatty acid oxidation, there has long been interest in the possibility that carnitine might be of benefit in genetic or acquired disorders of energy production to improve fatty acid oxidation, to remove accumulated toxic fatty acyl-CoA metabolites, or to restore the balance between free and acyl-CoA. Two disorders have been described in children where the supply of carnitine becomes limiting for fatty acid oxidation: (1) A recessive defect of the muscle/kidney sodium-dependent, plasma membrane carnitine symporter, which presents in infancy with cardiomyopathy or hypoketotic hypoglycemia; treatment with oral carnitine is required for survival. (2) Chronic administration of pivalate-conjugated antibiotics in which excretion of pivaloyl-carnitine can lead to carnitine depletion; tissue levels may become low enough to limit fatty acid oxidation, although no cases of illness due to carnitine deficiency have been described. There is speculation that carnitine supplements might be beneficial in other settings (such as genetic acyl-CoA oxidation defects--"secondary carnitine deficiency", chronic ischemia, hyperalimentation, nutritional carnitine deficiency), but efficacy has not been documented. The formation of abnormal acylcarnitines has been helpful in expanded newborn screening programs using tandem mass-spectrometry of blood spot acylcarnitine profiles to detect genetic fatty acid oxidation defects in neonates. Carnitine-deficient diets (vegetarian) do not have much effect on carnitine pools in adults. A modest 50% reduction in carnitine levels is associated with hyperalimentation in newborn infants, but is of doubtful significance. The above considerations indicate that carnitine does not become rate-limiting unless extremely low; testing the benefits of nutritional supplements may require invasive endurance studies of fasting ketogenesis or muscle and cardiovascular work.

Published

2004

14. Effects of hydrochloric, valeric, and other volatile fatty acids on pathogenesis of ulcers in the nonglandular portion of the stomach of horses.

Author

Nadeau JA, Andrews FM, Patton CS, Argenzio RA, Mathew AG, and Saxton AM

Subjects

Animals, Culture Techniques, Electric Conductivity, Female, Horse Diseases physiopathology, Horses, Hydrogen-Ion Concentration, Male, Membrane Potentials drug effects, Sodium metabolism, Stomach pathology, Stomach Ulcer pathology, Time Factors, Fatty Acids, Volatile adverse effects, Hydrochloric Acid adverse effects, Pentanoic Acids adverse effects, Stomach drug effects, Stomach Ulcer chemically induced, Stomach Ulcer veterinary

Abstract

Objective: To identify in vitro effects of hydrochloric acid, valeric acid, and other volatile fatty acids (VFAs) on the pathogenesis of ulcers in the nonglandular portion of the equine stomach., Sample Population: Gastric tissues from 13 adult horses., Procedure: Nonglandular gastric mucosa was studied by use of Ussing chambers. Short-circuit current (Isc) and potential difference were measured and electrical resistance and conductance calculated after tissues were bathed in normal Ringer's solution (NRS) or NRS and hydrochloric, valeric, acetic, propionic, and butyric acids. Treated tissues were examined histologically., Results: Incubation in 60mM valeric acid at pH < or = 7.0 abruptly and irreversibly abolished Isc, which was followed by a slower decrease in resistance and an increase in conductance. Incubation in 60mM acetic, propionic, and butyric acids and, to a lesser extent, hydrochloric acid at pH < or = 7.0 significantly decreased Isc, which was followed by an increase in resistance and a decrease in conductance., Conclusions and Clinical Relevance: Incubation in valeric acid at pH < or = 7.0 caused a dramatic decrease in mucosal barrier function in the nonglandular portion of the stomach. Changes in barrier function attributable to exposure to valeric acid were associated with histopathologic evidence of cellular swelling in all layers of the nonglandular mucosa. Because of its high lipid solubility, valeric acid penetrates the nonglandular gastric mucosa, resulting in inhibition of sodium transport and cellular swelling. Valeric acid and other VFAs in gastric contents may contribute to the pathogenesis of ulcers in the nonglandular portion of the stomach of horses.

Published

2003

15. Pharmacokinetics of dexloxiglumide after administration of single and repeat oral escalating doses in healthy young males.

Author

Persiani S, D'Amato M, Makovec F, Tavares IA, Bishai PM, and Rovati LC

Subjects

Administration, Oral, Adult, Analysis of Variance, Area Under Curve, Chromatography, High Pressure Liquid, Double-Blind Method, Half-Life, Humans, Male, Pentanoic Acids administration & dosage, Pentanoic Acids adverse effects, Receptor, Cholecystokinin A, Time Factors, Pentanoic Acids pharmacokinetics, Receptors, Cholecystokinin antagonists & inhibitors

Abstract

Objective: To assess the pharmacokinetics, safety and tolerability of dexloxiglumide, a new CCK1 receptor antagonist currently under development for the treatment of the constipation-predominant irritable bowel syndrome., Subjects and Methods: Twelve volunteers were enrolled in the present study and received orally 100, 200 and 400 mg of dexloxiglumide as tablets as a single dose followed by repeated t.i.d. doses for 7 days according to a randomized, double-blind, double-dummy complete crossover design. Plasma and urine were collected before drug administration and up to 72 h after dosing. Dexloxiglumide plasma and urinary concentration, determined using validated HPLC methods with UV detection, were used for the pharmacokinetic analysis by standard noncompartmental methods. In addition, dexloxiglumide safety and tolerability were evaluated throughout the study period by performing standard laboratory tests, by recording vital signs and ECGs and by monitoring the occurrence and severity of adverse events., Results: After a single oral administration, dexloxiglumide was rapidly bioavailable with mean t(max) ranging from 0.9 - 1.6 h at all doses. The mean peak plasma concentrations (Cmax) were 1.7+/-0.6, 5.4+/-1.7, and 11.9+/-4.7 microg/ml, and the mean area under the plasma concentration-time curves (AUC) were 4.4+/-3.3, 8.6+/-3.6, and 18.3+/-5.9 microg x h/ml at the 3 doses, respectively. Apparent plasma clearance (CL/F) was 30.8+/-13.9, 27.2+/-10.6, and 21.1+/-8.6 l/h at the 3 doses, respectively. The apparent elimination half-life from plasma (t1/2) ranged from 2.6 - 3.3 h at the 3 doses. The excretion of unchanged dexloxiglumide in 0 - 72 h urine accounted for approximately 1% of the administered dose and this was true for all doses. Dexloxiglumide renal clearance (CLR) averaged 0.4+/-0.4, 0.4+/-0.2, and 0.3+/-0.3 l/h for the 3 doses, respectively. After the last dose of the repeated dosing period dexloxiglumide Cmax occurred at 1.1 - 1.6 h after drug administration and averaged 2.4+/-1.3, 7.1+/-2.9, and 15.3+/-2.7 microg/ml for the 3 doses, respectively. The AUC values averaged 5.9+/-3.0, 16.0+/-8.8, and 50.8+/-38.1 microg x h/ml, respectively. The area under the plasma concentration-time curve calculated at steady state within a dosing interval (AUCss) averaged 4.6+/-1.6, 11.3+/-3.6, and 28.4+/-8.2 microg x h/ml, whereas CL/F averaged 20.3+/-8.3, 16.3+/-9.0, and 10.3+/-5.0 l/h at the 3 doses, respectively. Dexloxiglumide t1/2 could not be accurately calculated due to the high inter-subject variability and to sustained dexloxiglumide plasma concentrations that precluded the identification ofthe terminal phase of the plasma concentration-time profiles. However, it appeared that dexloxiglumide t1/2 was considerably prolonged at the dose of 400 mg. CLR averaged 0.4+/-0.4, 0.3+/-0.3, and 0.3+/-0.1 l/h for the 3 doses, respectively. After a single dose, the plasma pharmacokinetics of dexloxiglumide were dose-independent in the dose range 100 - 400 mg. After repeated dose the pharmacokinetics of dexloxiglumide were virtually dose-independent in the dose range 100 - 200 mg. A slight deviation from linear pharmacokinetics was found with a dose of 400 mg. Dexloxiglumide plasma pharmacokinetics were also time-independent in the dose range 100 - 200 mg with a deviation from expectation based on the superimposition principle with a dose of 400 mg. Dexloxiglumide urinary excretion and renal clearance were both dose- and time-independent in the dose range 100 - 400 mg. The safety and tolerability of dexloxiglumide administered to healthy young males was good up to the maximum investigated dose of 400 mg both after single and after repeated doses., Conclusions: The safety and pharmacokinetic profile of dexloxiglumide when the drug is administered as single and repeated doses in the dose range 100 - 400 mg provides the rationale for the choice of the treatment schedule (200 mg t.i.d.) for the efficacy trials in patients with (constipation-predominant) irritable bowel syndrome.

Published

2002

16. Dexloxiglumide Rotta Research Lab.

Author

Varga G

Subjects

Animals, Clinical Trials as Topic, Colonic Diseases, Functional drug therapy, Digestive System Physiological Phenomena, Dyspepsia drug therapy, Gallbladder Emptying drug effects, Humans, Pentanoic Acids adverse effects, Pentanoic Acids metabolism, Pentanoic Acids pharmacology, Receptors, Cholecystokinin antagonists & inhibitors

Abstract

Dexloxiglumide, the (R)-isomer of loxiglumide, is a selective and highly potent CCK1 receptor antagonist. It is twice as potent as the racemic compound. because the anti-CCK activity is specific to the (R)-form, whereas the (S)-isomer is almost ineffective. It has been developed by Rotta Research Lab SpA for the treatment of diseases in which CCK1 receptor activity is potentially involved, including gastrointestinal motility, food intake and pancreatic disorders [218696]. Its receptor-mediated actions have been described in multiple in vitro and in vivo pharmacological systems. Results from both preclinical and clinical studies indicate that it is an effective inhibitor of gallbladder contraction, improves lower esophegal sphincter (LES) function, accelerates gastric emptying, accelerates colonic transit and significantly decreases symptoms in IBS and functional dyspepsia patients, and therefore has potential as an effective treatment for constipation-predominant IBS. functional dyspesia, constipation, LES function, gastric emptying disorders and biliary colics. Forest Laboratories has entered into an agreement with Rotta for the development and marketing of dexloxiglumide for the treatment of constipation-predominant IBS and phase III studies are currently ongoing in the US. In August 2000, Merrill Lynch expected that dexloxiglumide would not be launched until 2004 [379892], and in June 2001, predicted a US filing date in 2003 [413928].

Published

2002

17. Efficacy and safety of oral ridogrel in the treatment of ulcerative colitis: two multicentre, randomized, double-blind studies.

Author

Tytgat GN, Van Nueten L, Van De Velde I, Joslyn A, and Hanauer SB

Subjects

Administration, Oral, Adult, Aged, Aged, 80 and over, Anti-Inflammatory Agents, Non-Steroidal adverse effects, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Dose-Response Relationship, Drug, Double-Blind Method, Female, Humans, Male, Mesalamine adverse effects, Mesalamine pharmacology, Middle Aged, Placebos, Treatment Outcome, Colitis, Ulcerative drug therapy, Gastrointestinal Agents adverse effects, Gastrointestinal Agents pharmacology, Pentanoic Acids adverse effects, Pentanoic Acids pharmacology, Pyridines adverse effects, Pyridines pharmacology

Abstract

Background: Ridogrel at low doses inhibits thromboxane synthase. Oral ridogrel, from 5 mg once daily to 150 mg twice daily, improves the endoscopic appearance of colonic mucosa and clinical manifestations in mild to moderate ulcerative colitis., Aim: One US trial and one international trial were conducted to determine the effect of ridogrel on mild to severe active ulcerative colitis., Methods: Two 12-week, double-blind, randomized, parallel-group trials were conducted. A US trial compared 0.5 mg, 2.5 mg and 5 mg of ridogrel once daily with placebo. An international trial compared 0.5 mg of ridogrel once daily with 2.5 mg and 5.0 mg of ridogrel once daily and 800 mg of mesalazine (known as mesalamine in the USA) three times daily. The primary efficacy outcome measure was the rate of complete remission., Results: In the US trial, complete remission was achieved in 20.8% of patients in the 0.5 mg ridogrel group, 17.9% in the 2.5 mg ridogrel group, 20.6% in the 5.0 mg ridogrel group and 13.6% in the placebo group. In the international trial, 14.4% of patients in the 0.5 mg ridogrel group, 19.6% in the 2.5 mg ridogrel group, 19.4% in the 5.0 mg ridogrel group and 16.4% in the mesalazine group experienced complete remission. In the international trial, rates of complete remission at the end-point were greater in the 2.5 mg and 5.0 mg ridogrel groups than in the 0.5 mg ridogrel group, but the differences were not statistically significant. In the US trial, rates of complete remission at the end-point were greater in the 2.5 mg and 5.0 mg ridogrel groups than in the placebo group, but the differences were not statistically significant. Approximately 30% of the patients in each group discontinued treatment before the 12-week end-point owing to a lack of therapeutic response. All doses of ridogrel were well tolerated and comparable with placebo or mesalazine in terms of safety., Conclusions: No significant differences in the primary efficacy outcome measure were found between either the 2.5 mg or the 5.0 mg dose of ridogrel and placebo in the US trial and between either the 2.5 mg or the 5.0 mg dose of ridogrel and the 0.5 mg dose of ridogrel, a surrogate dose for placebo, in the international trial. There was no clear indication in either trial of an effective dose of ridogrel in the treatment of ulcerative colitis.

Published

2002

18. Carnitine protects mitochondria and removes toxic acyls from xenobiotics.

Author

Arrigoni-Martelli E and Caso V

Subjects

Acyl Coenzyme A metabolism, Ammonia adverse effects, Animals, Anti-Bacterial Agents adverse effects, Anti-HIV Agents adverse effects, Antineoplastic Agents adverse effects, Bacterial Toxins adverse effects, Carnitine metabolism, Carnitine pharmacology, Humans, Mitochondria physiology, Pentanoic Acids adverse effects, Peroxisome Proliferators adverse effects, Valproic Acid adverse effects, Carnitine therapeutic use, Mitochondria drug effects, Xenobiotics adverse effects

Abstract

The carnitine system is altered by several xenobiotics (drugs and chemicals). These alterations are responsible for most toxic effects, which can be reverted or minimized by L-carnitine administration. Formation of nonmetabolizable acyl coenzyme A (CoA) is a typical step in the biotransformation of pivaloyl antibiotics, valproate and ifosfamide. The elevated levels of acylcarnitine occurring in human urine due to impaired metabolism of specific acyl CoA support the role of L-carnitine as an acceptor of specific, nonmetabolizable acyl CoA. The consequence of this process is a secondary carnitine deficiency. The formation of stable complexes with an essential component of mitochondrial membrane, cardiolipin, and the inhibition of myocardial specific isoform of carnitine-palmitoyl transferase are presumably the basis of adriamycin cardiotoxicity. L-carnitine interacts with cardiolipin, modifying membrane permeability and protecting the functions of the mitochondria. This mechanism can be proposed to explain the protective effects of L-carnitine against adriamycin cardiotoxicity, ammonium acetate and zidovudine-induced mitochondrial ultrastructural and functional alterations. Cisplatin, cephalosporin and carbapenem antibiotics inhibit carnitine reabsorption in renal tubules and cause proximal tubular damage. The study of peroxisomal producing agents belonging to largely different chemical classes showed that these agents caused carnitine system perturbations which may have the potential to be highly relevant biomarkers of exposure to the nongenotoxic peroxisomal proliferating agent class of hepatic tumorigens.

Published

2001

19. Ridogrel. R 68070.

Subjects

Animals, Colitis, Ulcerative drug therapy, Dogs, Drugs, Investigational adverse effects, Drugs, Investigational pharmacokinetics, Drugs, Investigational pharmacology, Enzyme Inhibitors adverse effects, Enzyme Inhibitors pharmacokinetics, Enzyme Inhibitors pharmacology, Gastrointestinal Agents adverse effects, Gastrointestinal Agents pharmacokinetics, Humans, Male, Pentanoic Acids adverse effects, Pentanoic Acids pharmacokinetics, Pentanoic Acids pharmacology, Pyridines adverse effects, Pyridines pharmacokinetics, Pyridines pharmacology, Thromboxane-A Synthase antagonists & inhibitors, Drugs, Investigational therapeutic use, Enzyme Inhibitors therapeutic use, Gastrointestinal Agents therapeutic use, Inflammatory Bowel Diseases drug therapy, Pentanoic Acids therapeutic use, Pyridines therapeutic use

Published

1999

20. Pivalic acid-induced carnitine deficiency and physical exercise in humans.

Author

Abrahamsson K, Eriksson BO, Holme E, Jodal U, Jönsson A, and Lindstedt S

Subjects

Adolescent, Adult, Amdinocillin Pivoxil chemistry, Blood Glucose metabolism, Fatty Acids, Nonesterified blood, Female, Glycogen blood, Humans, Male, Middle Aged, Pentanoic Acids adverse effects, Pivampicillin chemistry, Triglycerides blood, Amdinocillin Pivoxil adverse effects, Carnitine deficiency, Exercise, Pivampicillin adverse effects

Abstract

To study the effect of carnitine depletion on physical working capacity, healthy subjects were administered pivaloyl-conjugated antibiotics for 54 days. The mean carnitine concentration in serum decreased from 35.0 to 3.5 mmicromol/L, and in muscle from 10 to 4.3 micromol/g noncollagen protein (NCP). Exercise tests were performed before and after 54 days' administration of the drug. At submaximal exercise, there was a slight increase in the concentration of 3-hydroxybutyrate in serum, presumably caused by decreased fatty acid oxidation in the liver. There was also a decreased consumption of muscle glycogen, indicating decreased glycolysis in the skeletal muscle. The muscle presumably had enough energy available, since there was no significant decrease in the concentration of adenosine triphosphate (ATP) and creatine phosphate during exercise. The work at maximal oxygen uptake (VO2max) and the maximal heart rate were reduced. Since VO2max is considered dependent on heart function, carnitine depletion seemed to affect cardiac function.

Published

1996

21. Selective depletion of mitochondrial glutathione content by pivalic acid and valproic acid in rat liver: possibility of a common mechanism.

Author

Zanelli U, Puccini P, Acerbi D, Ventura P, and Gervasi PG

Subjects

Animals, Anticonvulsants adverse effects, Anticonvulsants pharmacokinetics, Injections, Intraperitoneal, Male, Mitochondria, Liver drug effects, Pentanoic Acids adverse effects, Pentanoic Acids pharmacokinetics, Rats, Rats, Sprague-Dawley, Valproic Acid adverse effects, Valproic Acid pharmacokinetics, Anticonvulsants pharmacology, Glutathione metabolism, Mitochondria, Liver metabolism, Pentanoic Acids pharmacology, Valproic Acid pharmacology

Published

1996

22. Transient reduction of human left ventricular mass in carnitine depletion induced by antibiotics containing pivalic acid.

Author

Abrahamsson K, Mellander M, Eriksson BO, Holme E, Jodal U, Jönsson A, and Lindstedt S

Subjects

Adolescent, Adult, Carnitine blood, Carnitine urine, Echocardiography, Female, Humans, Male, Middle Aged, Muscle, Skeletal chemistry, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Myocardium pathology, Time Factors, Amdinocillin Pivoxil adverse effects, Anti-Bacterial Agents adverse effects, Carnitine deficiency, Heart Septum drug effects, Myocardium metabolism, Pentanoic Acids adverse effects

Abstract

Objective: To study the effect of induced carnitine depletion on myocardial structure and function., Subjects and Design: 7 healthy adult volunteers given 1200 mg pivmecillinam per day for 7-8 weeks were studied by echocardiography before and after 7-8 weeks of treatment and a 15 months follow up after the treatment period., Setting: Teaching hospital., Main Outcome Measures: Carnitine concentration in serum, urine, and muscle and echocardiographic measurements., Results: After 7-8 weeks of treatment the median free serum carnitine concentration was reduced to 7% and the median total muscle carnitine concentration to 46% of the pretreatment levels. The median diastolic interventricular septum thickness decreased by 14% (mean 26%, P = 0.028) and the median left ventricular mass by 10% (mean 20%, P = 0.018). Fifteen months later these dimensions had increased but not completely returned to pretreatment values., Conclusions: Extended treatment with pivalic acid containing antibiotics causes carnitine depletion which may lead to changes in cardiac structure.

Published

1995

23. Effect of short-term treatment with pivalic acid containing antibiotics on serum carnitine concentration--a risk irrespective of age.

Author

Abrahamsson K, Holme E, Jodal U, Lindstedt S, and Nordin I

Subjects

Adolescent, Adult, Age Factors, Aged, Amdinocillin Pivoxil administration & dosage, Carnitine deficiency, Female, Humans, Male, Middle Aged, Norfloxacin administration & dosage, Penicillins administration & dosage, Pentanoic Acids administration & dosage, Prodrugs administration & dosage, Prodrugs adverse effects, Risk Factors, Time Factors, Urinary Tract Infections drug therapy, Amdinocillin Pivoxil adverse effects, Carnitine blood, Penicillins adverse effects, Pentanoic Acids adverse effects

Abstract

Treatment with pivalic acid containing prodrugs has been shown to cause carnitine depletion by loss of pivaloyl carnitine in urine. A 7-day standard pivmecillinam treatment of adults lead to a marked decrease of the free serum carnitine concentration (44.6 to 12.9 mumol/liter), whereas no change was seen in those given norfloxacine (40.0 to 40.5 mumol/liter). In some patients irrespective of age the free serum carnitine concentration was decreased to levels (around 10 mumol/liter) at which an impaired ketone-body production may occur. Therefore, there is reason for cautious use of this type of drug irrespective of the age of the patients.

Published

1995

24. Effects of pivalic acid-containing prodrugs on carnitine homeostasis and on response to fasting in children.

Author

Holme E, Jodal U, Linstedt S, and Nordin I

Subjects

Amdinocillin Pivoxil administration & dosage, Carnitine metabolism, Child, Child, Preschool, Female, Homeostasis, Humans, Muscles metabolism, Pivampicillin administration & dosage, Reference Values, Amdinocillin Pivoxil adverse effects, Carnitine deficiency, Fasting physiology, Pentanoic Acids adverse effects, Pivampicillin adverse effects, Prodrugs adverse effects

Abstract

Treatment of 17 children aged 2-9.5 years with a combination of pivmecillinam and pivampicillin (250-500 mumol 24 h-1) for more than 1 year resulted in a reduction of the free carnitine concentration in serum and muscle to less than 10% of the mean reference value. The decline in serum was slow, with an estimated half-life of about 5 months. Spontaneous replenishment occurred at about the same slow rate. Thus, there is no increase in endogenous carnitine synthesis as a response to increased demand of carnitine for detoxification. Supplementation with carnitine during treatment required at least a four-fold molar excess over pivalic acid to achieve and sustain a normal carnitine concentration. The replenishment of carnitine occurred with a half-life of 1.1-3.0 months. From determination of muscle-carnitine concentration in patients treated with pivaloyl-containing antibiotics and in patients with organic aciduris, we conclude that serum carnitine is a good predictor of carnitine stores in the body. Six non-supplemented patients with a serum free-carnitine concentration of 0.7-2.6 mumol l-1 had an inadequate ketone-body increase during a 24-h fast. Vomiting, nausea and tiredness occurred in three cases following the fasting period. After normalization of the serum-carnitine concentration, a normal response to fasting was observed. Thus, in some organic acidurias, for example medium-chain acyl-CoA dehydrogenase deficiency, a low liver concentration of carnitine may be an important contributing factor to hypoglycaemic and Reye-like attacks. We believe that prodrugs which contain pivalic acid should be avoided if acceptable alternatives exist. If used, supplementation with at least four-fold molar excess of carnitine is advisable.

Published

1992

25. Ridogrel inhibits systemic and renal formation of thromboxane A2 and antagonizes platelet thromboxane A2/prostaglandin endoperoxide receptors upon chronic administration to man.

Author

Weber C, Beetens JR, Tegtmeier F, Van Rooy P, Vercammen E, Wouters L, and De Clerck F

Subjects

Adult, Blood Platelets metabolism, Drug Evaluation, Drug Tolerance, Humans, Kidney drug effects, Kidney metabolism, Male, Middle Aged, Pentanoic Acids administration & dosage, Pentanoic Acids adverse effects, Platelet Aggregation drug effects, Platelet Aggregation Inhibitors pharmacology, Prostaglandins blood, Prostaglandins urine, Pyridines administration & dosage, Pyridines adverse effects, Receptors, Prostaglandin antagonists & inhibitors, Receptors, Thromboxane antagonists & inhibitors, Safety, Thromboxane-A Synthase antagonists & inhibitors, Blood Platelets drug effects, Pentanoic Acids pharmacology, Pyridines pharmacology, Thromboxane A2 biosynthesis

Abstract

The effects of ridogrel, a dual thromboxane A2 (TXA2) synthase inhibitor and TXA2/prostaglandin (PG) endoperoxide receptor antagonist, on systemic and renal production of prostaglandins and on platelet TXA2/PG endoperoxide receptors was evaluated upon chronic administration (300 mg b.i.d. orally, for 8 and 29 days) to man. Such a medication with ridogrel inhibits the systemic as well as the renal production of TXA2 as measured by the urinary excretion of 2,3-dinor-TXB2 and TXB2 respectively without inducing significant changes in systemic or renal PGI2 production. Simultaneously with the latter effects, the production of TXB2 by spontaneously coagulated whole blood ex vivo is inhibited (greater than 99%) while that of PGE2 and PGF2 alpha is largely increased. Administration of ridogrel causes a three- to five-fold shift to the right of concentration-response curves for U46619 in eliciting platelet aggregation; no tachyphylaxis is observed after 29 days of treatment in this respect. Apart from a reduction of serum uric acid levels with a concomitant increase in urinary uric acid excretion during the first days of treatment, no clinically significant changes in hematological, biochemical, hemodynamic and coagulation parameters occur during the 8 days or 29 days study. The study demonstrates that ridogrel is a potent inhibitor of the systemic as well as renal TXA2 synthase and an antagonist of platelet TXA2/PG endoperoxide receptor in man, covering full activity during 24 h at steady-state plasma level conditions without tachyphylaxis during 29 days of medication. The compound is well tolerated, at least during 1 month of administration.

Published

1992

26. Ridogrel in the setting of percutaneous transluminal coronary angioplasty.

Author

Timmermans C, Vrolix M, Vanhaecke J, Stammen F, Piessens J, Vercammen E, and De Geest H

Subjects

6-Ketoprostaglandin F1 alpha blood, Administration, Oral, Aged, Coronary Disease blood, Coronary Disease diagnostic imaging, Drug Administration Schedule, Drug Therapy, Combination, Female, Follow-Up Studies, Hemorrhage chemically induced, Humans, Male, Middle Aged, Pentanoic Acids adverse effects, Pentanoic Acids blood, Pilot Projects, Pyridines adverse effects, Pyridines blood, Radiography, Recurrence, Thromboxane B2 blood, Angioplasty, Balloon, Coronary, Coronary Disease therapy, Heparin administration & dosage, Pentanoic Acids administration & dosage, Pyridines administration & dosage, Salicylates therapeutic use, Thromboxane-A Synthase antagonists & inhibitors

Abstract

The safety of the combination of heparin and ridogrel therapy and its antiplatelet efficacy was examined in the setting of percutaneous transluminal coronary angioplasty (PTCA). In 32 patients without known aspirin intake for 10 days before PTCA, therapy with ridogrel (300-mg intravenous bolus) was begun just before PTCA and continued orally at a dose of 300 mg twice daily until discharge. Heparin was administered as a 10,000 IU bolus dose before PTCA and followed by an intravenous infusion at a rate of 1,000 IU/hour for 24 hours. Bleeding problems at the arterial entry site occurred in 13 patients, which required a blood transfusion in only 2 patients. One patient underwent emergency bypass surgery without specific problems of hemostasis. Ridogrel virtually eliminated thromboxane B2 from the serum (29,990 +/- 6,555 pg/0.1 ml before vs 63 +/- 7 pg/0.1 ml at 2 hours after ridogrel), with a concomitant increase in serum 6-keto-prostaglandin F1 alpha (511 +/- 34 pg/0.1 ml before vs 1,190 +/- 146 pg/0.1 ml at 24 hours after ridogrel). There were no acute reocclusions in the ridogrel-treated patients, whereas acute reocclusions occurred in 5.6% of the patients taking the standard aspirin + heparin regimen during the same period. Furthermore, at 6-month clinical follow-up patients treated with ridogrel compared favorably with those receiving standard treatment.

Published

1991

27. Gemfibrozil for hyperlipidemia.

Subjects

Cholesterol blood, Gemfibrozil, Humans, Hypolipidemic Agents adverse effects, Pentanoic Acids adverse effects, Triglycerides blood, Hyperlipidemias drug therapy, Hypolipidemic Agents therapeutic use, Pentanoic Acids therapeutic use, Valerates therapeutic use

Published

1982

28. Treatment of type III hyperlipoproteinemia with gemfibrozil to retard progression of coronary artery disease.

Author

Kuo PT, Wilson AC, Kostis JB, Moreyra AB, and Dodge HT

Subjects

Adult, Combined Modality Therapy, Coronary Disease etiology, Drug Evaluation, Exercise Test, Female, Gemfibrozil, Hand Dermatoses etiology, Hand Dermatoses prevention & control, Humans, Hyperlipoproteinemia Type III complications, Hyperlipoproteinemia Type III diet therapy, Hypolipidemic Agents adverse effects, Lipids blood, Lipoproteins blood, Male, Middle Aged, Pentanoic Acids adverse effects, Xanthomatosis etiology, Xanthomatosis prevention & control, Coronary Disease prevention & control, Hyperlipoproteinemia Type III drug therapy, Hypolipidemic Agents therapeutic use, Pentanoic Acids therapeutic use, Valerates therapeutic use

Abstract

Eight type III hyperlipoproteinemic (type III HLP), homozygous E 2/2 patients were enrolled in two periods of long-term diet-gemfibrozil treatment. The combined therapy resulted in highly significant decreases in their low-density lipoprotein cholesterol, very-low density lipoprotein cholesterol, very-low density lipoprotein triglycerides, and increases in their high-density lipoprotein cholesterol during the first treatment period of 24 to 28 months. Type III HLP reasserted itself following an 8-week interruption of gemfibrozil therapy. Resumption of gemfibrozil therapy again lowered the high lipid-lipoprotein concentrations of these patients toward normal. Tuboeruptive xanthomata, palmar xanthoma, and xanthoma striata palmare subsided with treatment. Follow-up coronary arteriograms performed 2.5 to 3.0 years after initiation of diet-drug treatment showed stabilization of coronary arterial lesions, which was associated with improvement in exercise tolerance.

Published

1988

29. Adverse effects of the treatment for hyperlipidemia.

Author

Malinow MR

Subjects

Anion Exchange Resins adverse effects, Anticholesteremic Agents adverse effects, Bibliographies as Topic, Clofibrate adverse effects, Diet adverse effects, Drug Therapy, Combination adverse effects, Gemfibrozil, Humans, Hyperlipidemias diet therapy, Hyperlipidemias drug therapy, Hypolipidemic Agents adverse effects, Male, Neomycin adverse effects, Niacin adverse effects, Pentanoic Acids adverse effects, Physical Exertion, Probucol adverse effects, Risk, Hyperlipidemias therapy

Abstract

A variety of treatments to lower elevated plasma lipid levels in patients with hyperlipidemia are available. Adverse side effects ranging from mere annoyances to uncommon serious consequences may be associated with dietary modification, recreational physical exercise, and drug intervention. As in other clinical circumstances, risk-to-benefit ratios must be taken into consideration in the management of hyperlipidemia.

Published

1986

30. Exacerbation of psoriasis by the hypolipidemic agent, gemfibrozil.

Author

Fisher DA, Elias PM, and LeBoit PL

Subjects

Female, Gemfibrozil, Humans, Middle Aged, Psoriasis pathology, Hypolipidemic Agents adverse effects, Pentanoic Acids adverse effects, Psoriasis chemically induced, Valerates adverse effects

Published

1988

31. Clinical results with gemfibrozil.

Author

Pickering JE

Subjects

Cholesterol blood, Cholesterol, HDL, Cholesterol, LDL, Clinical Trials as Topic, Gemfibrozil, Humans, Hyperlipoproteinemias blood, Lipoproteins, HDL blood, Lipoproteins, LDL blood, Lipoproteins, VLDL blood, Pentanoic Acids adverse effects, Triglycerides blood, Hyperlipoproteinemias drug therapy, Hypolipidemic Agents therapeutic use, Pentanoic Acids therapeutic use, Valerates therapeutic use

Published

1983

32. A comparison of different formulations and dosage administrations of gemfibrozil.

Author

Kovanen PT, Koskinen P, and Manninen V

Subjects

Administration, Oral, Adult, Apolipoproteins blood, Cholesterol, HDL blood, Cholesterol, LDL blood, Drug Administration Schedule, Female, Gemfibrozil, Humans, Hyperlipoproteinemia Type II blood, Hypolipidemic Agents adverse effects, Male, Middle Aged, Pentanoic Acids adverse effects, Tablets, Time Factors, Hyperlipoproteinemia Type II drug therapy, Hypolipidemic Agents administration & dosage, Pentanoic Acids administration & dosage, Valerates administration & dosage

Abstract

To assess the lipid-regulating effects of 2 new gemfibrozil formulations, a nonblind parallel group comparison was performed using Finnish industrial workers with types IIA and IIB primary hyperlipoproteinemia. In all, 670 subjects were evaluated; 416 had total low density lipoprotein (LDL) cholesterol (serum total cholesterol--high density lipoprotein [HDL] cholesterol) levels greater than or equal to 200 mg/dl and thus qualified for the screening period of the trial. During this 2-month period, the subjects were placed on an optimal diet according to their Fredrickson phenotype. Those whose total LDL levels remained greater than or equal to 200 mg/dl until the end of the 2-month period (n = 321) were admitted to the active drug phase of the trial and randomized to 1 of 3 treatment groups. Group 1 received the standard gemfibrozil dosage of two 300-mg capsules 2 times a day, for a total daily dosage equal to 1,200 mg. Group 2 also received a 1,200-mg daily dose, given as a 600-mg tablet of gemfibrozil 2 times a day. Group 3 received a once-a-day dose of two 450-mg tablets in the evening. Preliminary results show that the alternate gemfibrozil formulations are thus far equal to the standard gemfibrozil dosage in their effects on blood lipids. Substantial decreases have been noted in serum cholesterol, serum triglycerides, LDL cholesterol and serum apolipoprotein B. The 3 formulations also produced similar increases in HDL cholesterol and its subfractions HDL2 and HDL3, as well as in serum apolipoproteins AI and AII.

Published

1986

33. Treatment of hyperlipidemia with gemfibrozil.

Author

Hartshorn JC and Deans K

Subjects

Gemfibrozil, Humans, Pentanoic Acids adverse effects, Hyperlipidemias drug therapy, Hypolipidemic Agents therapeutic use, Pentanoic Acids therapeutic use, Valerates therapeutic use

Published

1987

34. Light and electron microscopy of liver in hyperlipoproteinemic patients under long-term gemfibrozil treatment.

Author

De La Iglesia FA, Lewis JE, Buchanan RA, Marcus EL, and McMahon G

Subjects

Gemfibrozil, Humans, Hyperlipoproteinemias drug therapy, Hypolipidemic Agents therapeutic use, Liver ultrastructure, Long-Term Care, Microscopy, Electron, Pentanoic Acids therapeutic use, Hyperlipoproteinemias pathology, Hypolipidemic Agents adverse effects, Liver pathology, Pentanoic Acids adverse effects, Valerates adverse effects

Abstract

The effects of long-term gemfibrozil (Lopid) therapy on human liver structure are not known. Studies of this nature are becoming essential in determining the risk/benefit ratio since gemfibrozil is an effective agent for the control of hyperlipoproteinemia types IIa, IIb, and IV. Particularly, gemfibrozil is effective when dietary management or available therapeutic control fail to reduce serum cholesterol and triglycerides as well as normalizing the lipoprotein pattern. Percutaneous liver biopsies of 9 patients on long-term gemfibrozil therapy were evaluated by light microscopy, interference contrast optics and transmission electron microscopy. The distribution of patients according to lipoprotein phenotype was 3 Type IIa, 3 Type IIb, and 3 Type IV. Their lipoprotein patterns approached normal and the serum lipids were controlled during gemfibrozil therapy. By light microscopy, the lobular architecture and other parameters were within normal limits. Varying degrees of fatty change were found as would be expected. No preferential lobular disposition of the fat globules was evident. Coalescence of fat droplets, nuclear displacement and fatty cysts were noted. Differential interference contrast microscopy revealed several degrees of contrast amplitude in these droplets suggesting a heterogeneous lipid deposition in hepatocytes. The subcellular analysis revealed a moderate degree of glycogen deposition, absence of nuclear abnormalities and unremarkable mitochondria; the rough endoplasmic reticulum was not significantly altered and smooth surfaced membranes appeared proliferated. Detailed analysis of the peroxisome population showed matrix rarefaction, marginal plate formation and spurious densities though no significant proliferation occurred. Distribution of peroxisomes in hepatocytes varied widely from cell to cell and in different lobular areas. This study confirmed the association of hepatic fatty change with hyperlipoproteinemia irrespective of the pattern observed in circulating lipoproteins. Peroxisome proliferation, as seen in rodents when receiving gemfibrozil, did not occur and the structure of these subcellular organelles was not compromised. It was concluded that the long-term administration of this compound did not show adverse effects on the hepatocyte in hyperlipoproteinemia.

Published

1982

35. Gemfibrozil-induced headache.

Author

Arellano F, de Cos MA, Valiente R, and Quirós C

Subjects

Female, Gemfibrozil, Humans, Middle Aged, Headache chemically induced, Hypolipidemic Agents adverse effects, Pentanoic Acids adverse effects, Valerates adverse effects

Published

1988

36. Helsinki Heart Study: primary-prevention trial with gemfibrozil in middle-aged men with dyslipidemia. Safety of treatment, changes in risk factors, and incidence of coronary heart disease.

Author

Frick MH, Elo O, Haapa K, Heinonen OP, Heinsalmi P, Helo P, Huttunen JK, Kaitaniemi P, Koskinen P, and Manninen V

Subjects

Adult, Cholesterol blood, Clinical Trials as Topic, Coronary Disease prevention & control, Double-Blind Method, Finland, Gemfibrozil, Humans, Hypercholesterolemia blood, Hypercholesterolemia drug therapy, Hypolipidemic Agents administration & dosage, Hypolipidemic Agents adverse effects, Male, Middle Aged, Pentanoic Acids administration & dosage, Pentanoic Acids adverse effects, Random Allocation, Risk Factors, Triglycerides blood, Cholesterol, HDL blood, Cholesterol, LDL blood, Coronary Disease epidemiology, Hypolipidemic Agents therapeutic use, Pentanoic Acids therapeutic use, Valerates therapeutic use

Abstract

In a randomized, double-blind five-year trial, we tested the efficacy of simultaneously elevating serum levels of high-density lipoprotein (HDL) cholesterol and lowering levels of non-HDL cholesterol with gemfibrozil in reducing the risk of coronary heart disease in 4081 asymptomatic middle-aged men (40 to 55 years of age) with primary dyslipidemia (non-HDL cholesterol greater than or equal to 200 mg per deciliter [5.2 mmol per liter] in two consecutive pretreatment measurements). One group (2051 men) received 600 mg of gemfibrozil twice daily, and the other (2030 men) received placebo. Gemfibrozil caused a marked increase in HDL cholesterol and persistent reductions in serum levels of total, low-density lipoprotein (LDL), and non-HDL cholesterol and triglycerides. There were minimal changes in serum lipid levels in the placebo group. The cumulative rate of cardiac end points at five years was 27.3 per 1,000 in the gemfibrozil group and 41.4 per 1,000 in the placebo group--a reduction of 34.0 percent in the incidence of coronary heart disease (95 percent confidence interval, 8.2 to 52.6; P less than 0.02; two-tailed test). The decline in incidence in the gemfibrozil group became evident in the second year and continued throughout the study. There was no difference between the groups in the total death rate, nor did the treatment influence the cancer rates. The results are in accord with two previous trials with different pharmacologic agents and indicate that modification of lipoprotein levels with gemfibrozil reduces the incidence of coronary heart disease in men with dyslipidemia.

Published

1987

37. Effects of gemfibrozil on serum lipids.

Author

Samuel P

Subjects

Adult, Aged, Double-Blind Method, Drug Evaluation, Female, Gemfibrozil, Humans, Hypolipidemic Agents adverse effects, Male, Middle Aged, Pentanoic Acids adverse effects, Hyperlipoproteinemias drug therapy, Hypolipidemic Agents therapeutic use, Lipids blood, Pentanoic Acids therapeutic use, Valerates therapeutic use

Abstract

A two-part, multicenter study to assess the clinical efficacy, side effects, and safety of gemfibrozil in 427 patients over treatment durations of up to 13 months showed that this drug markedly reduces the level of serum triglycerides, while moderately lowering total serum cholesterol levels. The high-density lipoprotein cholesterol level was substantially increased, with concomitant decreases in low-density lipoprotein and very low-density lipoprotein cholesterol levels. The drug was generally well tolerated. However, a potential for increasing blood glucose levels was noted and careful monitoring during therapy is recommended.

Published

1983

38. Gemfibrozil and coronary heart disease.

Subjects

Accidents, Adult, Gemfibrozil, Humans, Male, Middle Aged, Violence, Coronary Disease prevention & control, Hypolipidemic Agents adverse effects, Pentanoic Acids adverse effects, Valerates adverse effects

Published

1988

39. Lipid-lowering drugs.

Subjects

Cataract chemically induced, Cholesterol, HDL blood, Coronary Disease prevention & control, Gemfibrozil, Humans, Pentanoic Acids adverse effects, Pentanoic Acids therapeutic use, Hypolipidemic Agents adverse effects, Hypolipidemic Agents therapeutic use

Published

1988

40. Lessons from the Helsinki Heart Study. Fibric acid therapy for dyslipidemia.

Author

Grundy SM

Subjects

Adult, Bile Acids and Salts metabolism, Cholesterol, HDL metabolism, Cholesterol, LDL metabolism, Gemfibrozil, Humans, Male, Middle Aged, Pentanoic Acids adverse effects, Triglycerides metabolism, Coronary Disease prevention & control, Hypercholesterolemia drug therapy, Hypolipidemic Agents therapeutic use, Lipoproteins metabolism, Pentanoic Acids therapeutic use, Valerates therapeutic use

Published

1988

41. The Gemfibrozil Study.

Author

Manninen V

Subjects

Adult, Clinical Trials as Topic, Female, Gemfibrozil, Humans, Lipoproteins, LDL blood, Male, Middle Aged, Pentanoic Acids adverse effects, Pentanoic Acids pharmacology, Coronary Disease prevention & control, Hypolipidemic Agents therapeutic use, Pentanoic Acids therapeutic use, Valerates therapeutic use

Abstract

In clinical studies in dyslipidaemic patients gemfibrozil has produced falls in LDL and VLDL of 10-20% and 30-50%, respectively, but a rise in HDL of 15-25%. Gemfibrozil also produces increases in both Apo AI and AII, and in kininogen and prekallikrein. Side-effects are not a major problem. The Helsinki Heart Study has compared the effects of gemfibrozil with those of placebo in a group of 4080 dyslipidaemic Finnish men aged 40-55. The results are not yet available but there is reason to believe that the probable level of coronary risk reduction will be at least as great as that reported by the Lipid Research Clinics Study Coronary Primary Prevention Trial (LRC-CPPT).

Published

1985