Your search keyword '"Procainamide toxicity"' showing total 40 results

1. Intravenous Amiodarone and Sotalol Impair Contractility and Cardiac Output, but Procainamide Does Not: A Langendorff Study.

Author

Mackin C, DeWitt ES, Black KJ, Tang X, Polizzotti BD, van den Bosch SJ, Alexander ME, and Kheir JN

Subjects

Amiodarone toxicity, Animals, Anti-Arrhythmia Agents toxicity, Dose-Response Relationship, Drug, Infusions, Intravenous, Isolated Heart Preparation, Procainamide toxicity, Rats, Sprague-Dawley, Risk Assessment, Sotalol toxicity, Amiodarone administration & dosage, Anti-Arrhythmia Agents administration & dosage, Cardiac Output drug effects, Myocardial Contraction drug effects, Procainamide administration & dosage, Sotalol administration & dosage, Ventricular Function, Left drug effects

Abstract

Introduction: Direct comparison of the effects of antiarrhythmic agents on myocardial performance may be useful in choosing between medications in critically ill patients. Studies directly comparing multiple antiarrhythmic medications are lacking. The use of an experimental heart preparation permits examination of myocardial performance under constant loading conditions., Methods: Hearts of Sprague Dawley rats (n = 35, 402-507 g) were explanted and cannulated in working heart model with fixed preload and afterload. Each heart was then exposed to a 3-hour infusion of procainamide (20 µg/kg/min), esmolol (100 or 200 µg/kg/min), amiodarone (10 or 20 mg/kg/d), sotalol (80 mg/m 2 /d), or placebo infusions (n = 5 per dose). Cardiac output, contractility (dP/dT max ), diastolic performance (dP/dT min ), and heart rate were compared between groups over time by linear mixed modeling., Results: Compared with placebo, sotalol decreased contractility by an average of 24% ( P < .001) over the infusion period, as did amiodarone (low dose by 13%, P = .029; high dose by 14%, P = .013). Compared with placebo, mean cardiac output was significantly lower in animals treated with sotalol (by 22%, P = .016) and esmolol 200 μg/kg/min (by 23%, P = .012). Over time, amiodarone decreased cardiac output (20 mg/kg/d, β = -89 [-144, -33] μL/min 2 decrease, P = .002) and also worsened diastolic function, decreasing dP/dT min by ∼18% and 22% ( P = .032 and P = .011, low and high doses, respectively). Procainamide did not have a significant effect on any measures of systolic or diastolic performance., Conclusions: In isolated hearts, amiodarone and sotalol depressed myocardial contractility, cardiac output, and diastolic function. However, procainamide did not negatively affect myocardial performance and represents a favorable agent in settings of therapeutic equivalence.

Published

2019

2. Procainamide-induced autoimmunity: Relationship to T-helper 2-type T-cell activation.

Author

Huang Y, Lin Z, Huo Y, Geng X, Li M, Yang Y, and Li B

Subjects

Animals, Anti-Arrhythmia Agents toxicity, Antibodies, Antinuclear blood, Autoimmunity immunology, B-Lymphocytes drug effects, B-Lymphocytes immunology, Cytokines blood, Male, Rats, Inbred BN, Rats, Inbred Lew, Rats, Sprague-Dawley, Spleen drug effects, Spleen pathology, T-Lymphocytes immunology, Autoimmunity drug effects, Procainamide toxicity, T-Lymphocytes drug effects

Abstract

Drug-induced autoimmunity (DIA) refers to a group of adverse drug reactions, and they remain unpredictable largely due to the limited understanding of the mechanisms involved. There is evidence that procainamide can cause autoimmune reactions in humans but the mechanisms involved remain unclear. To examine the cellular and genetic factors involved in the procainamide-induced autoimmune response, we compared rats that are genetically T-helper (Th)2-predisposed (Brown Norway (BN)), Th1-predisposed (Lewis (LEW)) or not genetically predisposed (Sprague Dawley (SD)). We revealed significant differences in response to autoimmunity induced by procainamide among three strains rats, BN was the most sensitive one, SD exhibited less sensitive, while LEW resistance to procainamide. Much more pronounced of Th2-type responses and more complex differentially expressed genes involved in immune regulation and response in BN might contribute to its susceptibleness to DIA. Moreover, similar immune mechanisms were found between BN and SD, which suggesting that these changes would serve as the potential bridge biomarkers to predict DIA among species. This study may also benefit to further understand the toxicological mechanism of drug-induced autoimmune reactions.

Published

2018

3. Influence of microplastics on the toxicity of the pharmaceuticals procainamide and doxycycline on the marine microalgae Tetraselmis chuii.

Author

Prata JC, Lavorante BRBO, B S M Montenegro MDC, and Guilhermino L

Subjects

Anti-Bacterial Agents toxicity, Aquatic Organisms drug effects, Chlorophyta drug effects, Microalgae drug effects, Microalgae growth & development, Pharmaceutical Preparations, Water Pollutants, Chemical toxicity, Aquatic Organisms metabolism, Chlorophyta metabolism, Doxycycline toxicity, Microalgae metabolism, Plastics toxicity, Procainamide toxicity

Abstract

Microplastics and pharmaceuticals are considered ubiquitous and emergent pollutants of high concern but the knowledge on their effects on primary producers is still limited, especially those caused by mixtures. Thus, the goal of the present study was to investigate if the presence of microplastics (1-5 μm diameter) influences the toxicity of the pharmaceuticals procainamide and doxycycline to the marine microalga Tetraselmis chuii. Bioassays (96 h) to investigate the toxicity of those substances individually and in mixtures (i.e. microplastics-procainamide mixtures and microplastics-doxycycline mixtures) were carried out. Effect criteria were the average specific growth rate (growth rate) and chlorophyll a concentration (chlorophyll). EC 10 , EC 20 and EC 50 were determined. Microplastics alone had no significant effects on growth rate up to 41.5 mg/l, whereas chlorophyll was significantly reduced at 0.9 and 2.1 mg/l of microplastics, but not at higher concentrations. The 96 h EC 50 (growth rate and chlorophyll, respectively) determined for the other bioassays were: 104 and 143 mg/l for procainamide alone; 125 and 31 mg/l for procainamide in the presence of microplastics; 22 and 14 mg/l for doxycycline alone; 11 and 7 mg/l for doxycycline in the presence of microplastics. Significant differences (p < 0.001) between the toxicity curves of each pharmaceutical alone and in mixture with microplastics were found for procainamide (chlorophyll), and doxycycline (both parameters). Thus, both pharmaceuticals were toxic to T. chuii in the low ppm range, and microplastics-pharmaceutical mixtures were more toxic than the pharmaceuticals alone. Very high decreases of doxycycline concentrations in test media were found, indicating degradation of the antibiotic. Thus, although the biological results are expressed in relation to doxycycline concentration, the effects were likely caused by a mixture of the parental compound and its degradation products. The concentrations of microplastics and pharmaceuticals tested (low ppm range) are higher than those expected to be found in waters of the most part of marine ecosystems (ppt or ppb ranges). However, considering the widespread contamination by microplastics and pharmaceuticals, the concentrations already found in waters, sediments and/or organism of heavily polluted areas, the long-term exposure (over generations) of wild populations to such substances in polluted ecosystems and the possibilities of bioaccumulation and toxicological interactions, these findings are of concern and further research on microplastics-pharmaceuticals toxicological interactions is needed., (Copyright © 2018 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2018

4. Procainamide and lidocaine produce dissimilar changes in ventricular repolarization and arrhythmogenicity in guinea-pig.

Author

Osadchii OE

Subjects

Action Potentials drug effects, Animals, Anti-Arrhythmia Agents pharmacology, Arrhythmias, Cardiac physiopathology, Electrocardiography, Female, Guinea Pigs, Lidocaine pharmacology, Long QT Syndrome chemically induced, Long QT Syndrome physiopathology, Procainamide pharmacology, Tachycardia, Ventricular chemically induced, Tachycardia, Ventricular physiopathology, Voltage-Gated Sodium Channel Blockers pharmacology, Voltage-Gated Sodium Channel Blockers toxicity, Anti-Arrhythmia Agents toxicity, Arrhythmias, Cardiac chemically induced, Lidocaine toxicity, Procainamide toxicity

Abstract

Procainamide is class Ia Na(+) channel blocker that may prolong ventricular repolarization secondary to inhibition of IK r , the rapid component of the delayed rectifier K(+) current. In contrast to selective IN a blockers such as lidocaine, procainamide was shown to produce arrhythmogenic effects in the clinical setting. This study examined whether pro-arrhythmic responses to procainamide may be accounted for by drug-induced repolarization abnormalities including impaired electrical restitution kinetics, spatial gradients in action potential duration (APD), and activation-to-repolarization coupling. In perfused guinea-pig hearts, procainamide was found to prolong the QT interval on ECG and left ventricular (LV) epicardial monophasic APD, increased the maximum slope of electrical restitution, enhanced transepicardial APD variability, and eliminated the inverse correlation between the local APD and activation time values determined at distinct epicardial recording sites prior to drug infusion. In contrast, lidocaine had no effect on electrical restitution, the degree of transepicardial repolarization heterogeneities, and activation-to-repolarization coupling. Spontaneous episodes of monomorphic ventricular tachycardia were observed in 57% of procainamide-treated heart preparations. No arrhythmia was induced by lidocaine. In summary, this study suggests that abnormal changes in repolarization may contribute to pro-arrhythmic effects of procainamide., (© 2013 Société Française de Pharmacologie et de Thérapeutique. Published by John Wiley & Sons Ltd.)

Published

2014

5. Molecular organization of the non-bilayer phospholipid arrangements that induce an autoimmune disease resembling human lupus in mice.

Author

Wong-Baeza C, Hernández-Pando R, Reséndiz A, Tescucano A, Bustos I, Ibáñez M, Wong C, and Baeza I

Subjects

Animals, Antibodies blood, Antibodies metabolism, Antibodies, Monoclonal metabolism, Cardiolipins chemistry, Cardiolipins immunology, Cattle, Chlorpromazine toxicity, Kidney Glomerulus pathology, Lupus Erythematosus, Systemic chemically induced, Lupus Erythematosus, Systemic immunology, Lupus Erythematosus, Systemic pathology, Manganese toxicity, Mice, Models, Molecular, Nuclear Magnetic Resonance, Biomolecular, Phosphatidic Acids chemistry, Phosphatidic Acids immunology, Phosphatidylcholines chemistry, Phosphatidylcholines immunology, Phosphatidylserines chemistry, Phosphatidylserines immunology, Procainamide toxicity, Skin pathology, Unilamellar Liposomes chemistry, Unilamellar Liposomes immunology, Lupus Erythematosus, Systemic metabolism, Unilamellar Liposomes metabolism

Abstract

Non-bilayer phospholipid arrangements are three-dimensional structures that can form when anionic phospholipids with an intermediate form of the tubular hexagonal phase II (H(II)), such as phosphatidic acid, phosphatidylserine or cardiolipin, are present in a bilayer of lipids. The drugs chlorpromazine and procainamide, which trigger a lupus-like disease in humans, can induce the formation of non-bilayer phospholipid arrangements, and we have previously shown that liposomes with non-bilayer arrangements induced by these drugs cause an autoimmune disease resembling human lupus in mice. Here we show that liposomes with non-bilayer phospholipid arrangements induced by Mn²⁺ cause a similar disease in mice. We extensively characterize the physical properties and immunological reactivity of liposomes made of the zwitterionic lipid phosphatidylcholine and a H(II)-preferring lipid, in the absence or presence of Mn²⁺, chlorpromazine or procainamide. We use an hapten inhibition assay to define the epitope recognized by sera of mice with the disease, and by a monoclonal antibody that binds specifically to non-bilayer phospholipid arrangements, and we report that phosphorylcholine and glycerolphosphorylcholine, which form part of the polar region of phosphatidylcholine, are the only haptens that block the binding of the tested antibodies to non-bilayer arrangements. We propose a model in which the negatively charged H(II)-preferring lipids form an inverted micelle by electrostatic interactions with the positive charge of Mn²⁺, chlorpromazine or procainamide; the inverted micelle is inserted into the bilayer of phosphatidylcholine, whose polar regions are exposed and become targets for antibody production. This model may be relevant in the pathogenesis of human lupus.

Published

2012

6. DNA methylation and autoimmune disease.

Author

Richardson B

Subjects

Animals, Autoimmune Diseases etiology, Autoimmune Diseases immunology, Autoimmunity drug effects, Azacitidine toxicity, Cell Communication drug effects, Cell Communication immunology, Humans, Hydralazine toxicity, In Vitro Techniques, Lupus Erythematosus, Systemic etiology, Models, Immunological, Procainamide toxicity, T-Lymphocytes drug effects, T-Lymphocytes immunology, T-Lymphocytes metabolism, Autoimmune Diseases metabolism, DNA Methylation drug effects

Abstract

DNA methylation plays an essential role in maintaining T-cell function. A growing body of literature indicates that failure to maintain DNA methylation levels and patterns in mature T cells can result in T-cell autoreactivity in vitro and autoimmunity in vivo. Defective maintenance of DNA methylation may be caused by drugs such as procainamide or hydralazine, or failure to activate the genes encoding maintenance DNA methyltransferases during mitosis, resulting in the development of a lupus-like disease or perhaps other autoimmune disorders. This paper reviews the evidence supporting a role for abnormal T-cell DNA methylation in causing autoimmunity in an animal model of drug-induced lupus, and discusses some of the mechanisms involved. T cells from patients with active lupus have evidence for most if not all of the same methylation abnormalities, suggesting that abnormal DNA methylation plays a role in idiopathic human lupus as well.

Published

2003

7. Pharmacokinetics and central nervous system toxicity of declopramide (3-chloroprocainamide) in rats and mice.

Author

Hua J, Pero RW, and Kane R

Subjects

Administration, Oral, Animals, Antiemetics pharmacokinetics, Antiemetics toxicity, Biological Availability, Dopamine Antagonists pharmacokinetics, Dopamine Antagonists toxicity, Dose-Response Relationship, Drug, Female, Metoclopramide pharmacokinetics, Metoclopramide toxicity, Mice, Mice, SCID, Procainamide metabolism, Procainamide pharmacokinetics, Procainamide toxicity, Rats, Rats, Wistar, Receptors, Dopamine D2 metabolism, Receptors, Serotonin metabolism, Receptors, Serotonin, 5-HT3, Sleep Stages drug effects, Tissue Distribution, Central Nervous System drug effects, Procainamide analogs & derivatives

Abstract

Declopramide (3-chloroprocainamide) has been identified in previous studies as a representative of a new class of chemosensitizers. In this study, the toxicity and pharmacokinetics of declopramide have been investigated and compared with a structural analog, metoclopramide (MCA). Declopramide has not induced central nervous system (CNS)-related side effects in rats at doses up to 200 mg/kg, whereas MCA does at 12.5 mg/kg. In addition, declopramide did not bind to dopamine D2 receptors in subcellular preparations at doses up to 100 microM, whereas MCA showed affinity at 1 microM. Declopramide bound with affinity to 5-hydroxytryptamine3 receptors which are important in controlling vomiting. In contrast to MCA, declopramide has a rapid clearance from serum, a lower tissue concentration (about 15-fold lower than MCA) and a lower oral bioavailability (about 6-fold lower than MCA). However, declopramide was shown in vitro to possess a higher tumor cell absorption rate. One of the main metabolites of declopramide was identified as N-acetyl declopramide. Taken together, these data suggest that the clinical development of declopramide as a sensitizer of radio- and chemotherapies is an improvement over MCA, because it can be administered in a high dose and is devoid of CNS side effects.

Published

1999

8. [Correction of the cardiotoxic effect of the anti-arrhythmia agents with befol, sufan, and their combination].

Author

Galenko-Iaroshevskiĭ PA, Khankoeva AI, Uvarov AV, Bartashevich VV, Popov PB, Sirotenko DV, and Boldin VB

Subjects

Amiodarone toxicity, Animals, Anti-Arrhythmia Agents pharmacology, Benzimidazoles toxicity, Dibenzazepines toxicity, Drug Antagonism, Electrocardiography, Lidocaine toxicity, Male, Procainamide toxicity, Propranolol toxicity, Rats, Rats, Wistar, Tryptophan pharmacology, Verapamil toxicity, Anti-Arrhythmia Agents toxicity, Benzamides pharmacology, Cardiotonic Agents pharmacology, Morpholines pharmacology, Succinates pharmacology, Tryptophan analogs & derivatives

Published

1998

9. Autoimmunity caused by disruption of central T cell tolerance. A murine model of drug-induced lupus.

Author

Kretz-Rommel A, Duncan SR, and Rubin RL

Subjects

Adoptive Transfer, Animals, Antibodies, Antinuclear biosynthesis, Disease Models, Animal, Female, Humans, Immunity, Cellular drug effects, In Vitro Techniques, Lymphocyte Activation, Male, Mice, Mice, Inbred C57BL, Mice, Inbred DBA, Mice, Inbred MRL lpr, Mice, Inbred NZB, Procainamide toxicity, Thymus Gland drug effects, Thymus Gland immunology, Autoimmunity, Immune Tolerance drug effects, Lupus Erythematosus, Systemic chemically induced, Lupus Erythematosus, Systemic immunology, Procainamide analogs & derivatives, T-Lymphocytes drug effects, T-Lymphocytes metabolism

Abstract

A side effect of therapy with procainamide and numerous other medications is a lupus-like syndrome characterized by autoantibodies directed against denatured DNA and the (H2A-H2B)-DNA subunit of chromatin. We tested the possibility that an effect of lupus-inducing drugs on central T cell tolerance underlies these phenomena. Two intrathymic injections of procainamide-hydroxylamine (PAHA), a reactive metabolite of procainamide, resulted in prompt production of IgM antidenatured DNA antibodies in C57BL/6xDBA/2 F1 mice. Subsequently, IgG antichromatin antibodies began to appear in the serum 3 wk after the second injection and were sustained for several months. Specificity, inhibition and blocking studies demonstrated that the PAHA-induced antibodies showed remarkable specificity to the (H2A-H2B)-DNA complex. No evidence for polyclonal B cell activation could be detected based on enumeration of Ig-secreting B cells and serum Ig levels, suggesting that a clonally restricted autoimmune response was induced by intrathymic PAHA. The IgG isotype of the antichromatin antibodies indicated involvement of T cell help, and proliferative responses of splenocytes to oligonucleosomes increased up to 100-fold. As little as 5 microM PAHA led to a 10-fold T cell proliferative response to chromatin in short term organ culture of neonatal thymi. We suggest that PAHA interferes with self-tolerance mechanisms accompanying T cell maturation in the thymus, resulting in the emergence of chromatin-reactive T cells followed by humoral autoimmunity.

Published

1997

10. Toxicity, antitumor and chemosensitizing effects of 3-chloroprocainamide.

Author

Hua J and Pero RW

Subjects

Animals, Antineoplastic Agents pharmacology, Cisplatin pharmacology, Dose-Response Relationship, Drug, Drug Interactions, Drug Screening Assays, Antitumor, Female, Humans, Male, Metoclopramide pharmacology, Metoclopramide toxicity, Mice, Mice, SCID, Neoplasm Transplantation, Procainamide pharmacology, Procainamide toxicity, Transplantation, Heterologous, Astrocytoma drug therapy, Brain Neoplasms drug therapy, Procainamide analogs & derivatives

Abstract

3-Chloroprocainamide (3-CPA), an analog of metoclopramide (MCA), dose-dependently inhibited tumor growth in scid mice xenografted with a human brain astrocytoma (T24) when given intramuscularly to mice every third day for 14-20 days. 3-CPA was shown to have the same efficacy on tumor growth inhibition as neutral metoclopramide (neutral MCA) at the doses of 10-40 mg/kg when evaluated by tumor doubling time, tumor growth time for tumor volumes to reach 1000 mm3 and area under growth curve. 3-CPA at the dose of 3 x 40 mg/kg was also shown to enhance the cytotoxicity induced by a single dose of cisplatin at 7.5 mg/kg. A dose of < or = 160 mg/kg of 3-CPA did not show any notable extrapyramidal symptoms which was observed for neutral MCA treated mice at the dose of 20 mg/kg. The lethal response dose of 3-CPA for scid mice was 320 mg/kg which is 4 times higher than that determined for neutral MCA (80 mg/kg). These results support 3-CPA as a good candidate drug representing a new generation of benzamides for further clinical development as a cancer therapy drug.

Published

1997

11. Characterization of tumour necrosis factor alpha release by human granulocytes in response to procainamide challenge.

Author

Hill CM, Lunec J, Griffiths HR, and Herbert KE

Subjects

Cell Line, Cell Survival drug effects, Granulocytes metabolism, Humans, Granulocytes drug effects, Procainamide toxicity, Tumor Necrosis Factor-alpha metabolism

Abstract

The role of human granulocytes in the promotion of procainamide (PA) toxicity in vitro has been studied and one of the agents responsible for DNA strand scission and cell death in human target cells has been characterized. Crude peripheral blood mononuclear cells (cPBMNs) isolated by density centrifugation, and the lymphocyte cell lines--CCRF-HSB2 and WIL-2NS--were exposed to PA, and DNA strand breaks were quantified by fluorescent analysis of DNA unwinding. Therapeutic plasma concentrations of PA (0-50 microM) caused dose-dependent cytotoxicity, determined by dye exclusion, and strand breaks in cPBMNs incubated for 3 and 1.5 hr at 37 degrees, respectively. Using 50 microM PA a five-fold increase in DNA strand breaks was observed after 1.5 hr, with significant induction of strand breaks also being observed for 10 and 25 microM concentrations. Toxicity was much reduced in lymphocyte cell lines (maximal killing = 3.0% at 50 microM PA compared with 13.2% in cPBMNs). A similar decrease in toxicity was observed where N-acetyl procainamide (NAPA) was substituted for PA (less than 50% of strand breaks at all concentrations). Further investigations showed that the presence of a contaminating granulocyte population in the cPBMN fraction was responsible for the induction of PA toxicity. Incubation of a highly enriched granulocyte population with PA for 1 hr prior to exposure to purified peripheral blood mononuclear cells (pPBMNs) led to the complete restoration of the toxic effects. The resulting cyto- and genotoxicity were not significantly different to levels observed in cPBMNs. Significantly, incubation of granulocytes with NAPA did not induce toxicity in target pPBMNs. Ultrafiltration of granulocyte supernatants led to the identification of two toxic fractions of < 3000 and > 30,000 Da. Temporal studies showed that the toxicity associated with the < 3000 Da fraction appeared during the first 10-15 min incubation with PA whereas the > 30,000 Da fraction did not display significant toxicity until the 40-60 min period. Further assessment of the nature of these agents indicated that the 30,000 Da fraction was a protein. SDS-PAGE analysis showed an inducible 17,800 Da species appearing in granulocyte supernatants after 40 min incubation with PA. Dot blot analysis indicated that tumour necrosis factor alpha (TNF alpha) was present in the > 30,000 Da fraction. Evidence that TNF alpha was the high-molecular weight species responsible for PA-induced toxicity was obtained from neutralization assays employing an anti-TNF alpha antibody.(ABSTRACT TRUNCATED AT 400 WORDS)

Published

1995

12. Neutrophils and drug metabolism.

Author

von Schmiedeberg S, Goebel C, Gleichmann E, and Uetrecht J

Subjects

Animals, Autoimmunity, Gold Sodium Thiomalate metabolism, Gold Sodium Thiomalate toxicity, Mice, Neutrophils physiology, Procainamide metabolism, Procainamide toxicity, Propylthiouracil metabolism, Propylthiouracil toxicity, Autoimmune Diseases chemically induced, T-Lymphocytes, Helper-Inducer immunology

Published

1995

13. Testing of metoclopramide and procainamide for their ability to induce genotoxic effects in cultured mammalian cells.

Author

Martelli A, Campart GB, Canonero R, Mattioli F, and Brambilla G

Subjects

Animals, Autoradiography, Cells, Cultured, Cricetinae, Cricetulus, DNA Repair, DNA, Single-Stranded drug effects, Humans, Liver drug effects, Lung drug effects, Lymphocytes drug effects, Male, Micronuclei, Chromosome-Defective drug effects, Mutagenicity Tests, Rats, Rats, Sprague-Dawley, Metoclopramide toxicity, Mutagens toxicity, Procainamide toxicity

Abstract

Metoclopramide (MCA) and procainamide (PCA), two widely used benzamide drugs developed before the present regulatory climate but recently found to induce DNA breaks in human lymphocytes, were evaluated for their genotoxic effects in cultured rodent and human cells. In subtoxic concentrations neither MCA (from 0.10 to 0.32 mM) nor PCA (from 0.18 to 0.56 mM) induced DNA fragmentation and repair in primary cultures of metabolically competent rat and human hepatocytes. In the absence of metabolic activation a meaningful increase in the frequency of 6-thioguanine-resistant V79 cells was produced by the maximum tolerated concentration of MCA (3.2 mM), whereas PCA resulted nonmutagenic. Any clastogenic effect was absent in human lymphocytes exposed to MCA for 28 hr, but a statistically significant increase in the frequency of micronucleated cells was observed when the exposure was prolonged to 72 hr. In contrast, PCA was never clastogenic under the same experimental conditions. These results suggest that of the two benzamides tested only MCA should be considered potentially capable of producing mutagenic and clastogenic effects; it presumably behaves as an agent which is rapidly transformed by the liver into inactive metabolites, and the clinical relevance of its genotoxic activity remains to be ascertained.

Published

1995

14. Evaluation of DNA-damaging, clastogenic, and promoting activities of metoclopramide and procainamide in rats.

Author

Mereto E, Robbiano L, Ghia M, Allavena A, Martelli A, and Brambilla G

Subjects

Administration, Oral, Animals, Carcinogens toxicity, Liver drug effects, Liver enzymology, Male, Micronucleus Tests, Nitroso Compounds toxicity, Rats, Rats, Sprague-Dawley, DNA drug effects, Metoclopramide toxicity, Mutagens toxicity, Procainamide toxicity

Abstract

The DNA-damaging and clastogenic activities of metoclopramide (MCA) and procainamide (PCA), two substituted benzamides not systematically tested for genotoxicity before clinical use, were investigated in rats given a single high oral dose (500 mg/kg) of these drugs. Neither MCA nor PCA induced DNA fragmentation in liver, kidney, gastric mucosa, spleen, and bone marrow, as detected by the alkaline elution technique. Moreover, neither drug increased the frequency of micronucleated hepatocytes and the frequency of micronucleated polychromatic erythrocytes in the bone marrow of partially hepatectomized rats. However, in rats initiated with N-nitrosodiethylamine and given water containing 0.125% MCA for 14 successive days a clear-cut and statistically significant increase in the number and size of liver gamma-glutamyltranspeptidase-positive foci and basophilic foci, which are consistent with potential promoting activity, was observed. Under the same experimental conditions the effect of PCA was markedly lower, only limited to a modest increase of the number and area of gamma-glutamyltranspeptidase-positive foci.

Published

1995

15. Transformation of lupus-inducing drugs to cytotoxic products by activated neutrophils.

Author

Jiang X, Khursigara G, and Rubin RL

Subjects

Animals, Biological Assay, Biotransformation, Chlorpromazine analogs & derivatives, Chlorpromazine metabolism, Chlorpromazine toxicity, Humans, Hydralazine analogs & derivatives, Hydralazine metabolism, Hydralazine toxicity, Hydrogen Peroxide metabolism, Isoniazid analogs & derivatives, Isoniazid metabolism, Isoniazid toxicity, Mice, Neutrophils enzymology, Procainamide analogs & derivatives, Procainamide metabolism, Procainamide toxicity, Propylthiouracil analogs & derivatives, Propylthiouracil metabolism, Propylthiouracil toxicity, Quinidine analogs & derivatives, Quinidine metabolism, Quinidine toxicity, Tumor Cells, Cultured, Cell Death drug effects, Lupus Erythematosus, Systemic chemically induced, Neutrophil Activation, Neutrophils metabolism, Peroxidase metabolism

Abstract

Drug-induced lupus is a serious side effect of certain medications, but the chemical features that confer this property and the underlying pathogenesis are puzzling. Prototypes of all six therapeutic classes of lupus-inducing drugs were highly cytotoxic only in the presence of activated neutrophils. Removal of extracellular hydrogen peroxide before, but not after, exposure of the drug to activated neutrophils prevented cytotoxicity. Neutrophil-dependent cytotoxicity required the enzymatic action of myeloperoxidase, resulting in the chemical transformation of the drug to a reactive product. The capacity of drugs to serve as myeloperoxidase substrates in vitro was associated with the ability to induce lupus in vivo.

Published

1994

16. Comparison of popliteal lymph node responses in various strains of rats.

Author

Patriarca C, Verdier F, Brouland JP, Vial T, and Descotes J

Subjects

Animals, Barbital toxicity, Female, Hindlimb, Isoniazid toxicity, Male, Phenytoin toxicity, Procainamide toxicity, Rats, Rats, Inbred Strains, Rats, Sprague-Dawley, Rats, Wistar, Species Specificity, Streptozocin toxicity, Lymph Nodes drug effects

Abstract

Outbred (namely Wistar and Sprague-Dawley) and inbred (Wistar-Furth, Lewis, Fisher 344 and Brown-Norway) strains of rats were screened for their responses to reference compounds in the popliteal lymph node (PLN) assay. Streptozotocin and diphenylhydantoin gave positive responses as evidenced by increased weight and cellularity indices in all strains used whereas procainamide, isoniazid and barbital consistently gave negative responses. Although these findings overall are in agreement with previous investigations involving these compounds, the lack of marked interstrain differences in PLN responses argues against a strong immunogenetically controlled mechanism as could be assumed in presumably auto-immune reactions. The question is raised whether drug-induced side-effects predicted by the PLN assay are basically non-autoimmune as suggested by clinical and immunological findings in man.

Published

1994

17. T lymphocytes ignore procainamide, but respond to its reactive metabolites in peritoneal cells: demonstration by the adoptive transfer popliteal lymph node assay.

Author

Kubicka-Muranyi M, Goebels R, Goebel C, Uetrecht J, and Gleichmann E

Subjects

Acecainide immunology, Acetylation, Animals, Female, Humans, Hydroxylation, Immunologic Memory, Lymph Nodes immunology, Mice, Mice, Inbred A, Mice, Inbred C57BL, Peritoneal Cavity cytology, Phagocytes metabolism, Procainamide immunology, Procainamide metabolism, Spleen cytology, T-Lymphocytes drug effects, Acecainide toxicity, Lymph Nodes drug effects, Procainamide analogs & derivatives, Procainamide toxicity, T-Lymphocytes immunology

Abstract

The drug procainamide (PA) is notorious for causing drug-induced systemic lupus erythematosus (SLE) in humans. Indirect evidence suggests that metabolism of PA to a reactive intermediate metabolite is involved in the pathogenesis of drug-induced SLE in that N-hydroxylation of the arylamine group of PA favors this condition, whereas N-acetylation prevents it. If this is correct, one would expect hydroxylamine-PA (HAPA) to be immunogenic, whereas N-acetyl-PA (N-ac-PA) should be nonimmunogenic. This hypothesis was confirmed by means of the popliteal lymph node assay (PLNA) in mice: injection of PA and N-ac-PA failed to induce a reaction in the direct PLNA, whereas HAPA induced a vigorous reaction. Using the adoptive transfer PLNA, splenic T cells of mice that had received three injections of HAPA were shown to be specifically sensitized to this metabolite, but not to PA or N-ac-PA. In this system, an anamnestic T cell response could also be elicited when homogenized peritoneal cells of mice that had been treated with PA for 4 months were used as the challenging antigen, indicating that the peritoneal cells of PA-treated animals contained or had been exposed to the reactive intermediate metabolite HAPA. Whereas in slow acetylator mice this 4-month PA treatment sufficed to generate HAPA in peritoneal cells, fast acetylators required additional stimulation of their oxidative metabolism in order to produce enough HAPA detectable by sensitized T cells. These findings clearly support the concept that reactive intermediate metabolites, such as HAPA, are generated by the oxidative metabolism of phagocytic cells and are immunogenic for T cells.

Published

1993

18. The use of a three compartment in vitro model to investigate the role of hepatic drug metabolism in drug-induced blood dyscrasias.

Author

Tingle MD and Park BK

Subjects

Animals, Dapsone metabolism, Dapsone toxicity, Erythrocyte Count drug effects, Humans, Hydralazine metabolism, Hydralazine toxicity, In Vitro Techniques, Male, Methemoglobin metabolism, Microsomes, Liver metabolism, Models, Biological, Neutrophils drug effects, Primaquine metabolism, Primaquine toxicity, Procainamide metabolism, Procainamide toxicity, Rats, Rats, Wistar, Drug-Related Side Effects and Adverse Reactions, Hematologic Diseases chemically induced, Liver metabolism, Pharmaceutical Preparations metabolism

Abstract

1. N-hydroxylation is thought to be an essential step in the haemotoxicity of dapsone (DDS). To investigate both metabolism-dependent and cell-selective drug toxicity in vitro we have developed a three-compartment system in which an hepatic drug metabolizing system is contained within a central compartment separated by semipermeable membranes from compartments containing mononuclear leucocytes (MNL) and red blood cells (RBC). 2. Metabolism of dapsone (100 microM) by rat liver microsomes resulted in toxicity to RBC cells (47.3 +/- 2.1% methaemoglobin), but there was no significant toxicity toward MNL (3.7 +/- 1.3% cell death) compared with control values (1.6 +/- 0.9%). However, when RBC were replaced with buffer in the third compartment there was significantly greater (P < 0.001) white cell toxicity (17.6 +/- 0.6% cell death), demonstrating the protection of MNL by RBC. Metabolism of dapsone by human liver microsomes again resulted in RBC toxicity (12.5 +/- 3.3% methaemoglobin) but no significant MNL toxicity (2.9 +/- 0.8% cell death). Replacement of RBC resulted in a significant (P < 0.001) increase in MNL toxicity (6.5 +/- 0.7% cell death). Addition of synthetic dapsone hydroxylamine (30 microM) in the absence of a metabolizing system and with no RBC in the third compartment resulted in significant (P < 0.001) toxicity toward MNL (43.36 +/- 5.82% cell death) compared with control (1.8 +/- 1.1%). The presence of RBC in the third compartment resulted in a significant (P < 0.001) decrease in MNL toxicity (17.6 +/- 2.2% cell death), with 40.1 +/- 3.7% methaemoglobin in the RBC.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1993

19. Modulation of procainamide toxicity by selenium-enriched yeast in rats.

Author

Toborek M, Magner-Wróbel K, Drózdz M, Danch A, and Kopieczna-Grzebieniak E

Subjects

Animals, Antioxidants analysis, Female, Free Radicals, Lipid Peroxidation, Rats, Rats, Wistar, Yeasts, Procainamide toxicity, Selenium pharmacology

Abstract

Free radical processes are proposed to play a crucial role in the development of procainamide adverse effects. Therefore, selenium, as a potent antioxidant, may modified procainamide toxicity. To test this hypothesis plasma and liver thiobarbituric acid-reacting substances (TBARS), plasma antioxidant activity (AOA), erythrocyte and liver superoxide dismutase (SOD), catalase, as well as selenium-dependent glutathione peroxidase (Se-GPX) were determined in the following four groups of rats: selenium-treated (Se), procainamide-treated (P), procainamide and selenium-treated (P + Se), and control (C). Morphological studies of leukocytes [tested for lupus erythematosus (LE) cells] and liver were also made. Atypical, i.e. enlarged and swollen, leukocytes resulting from procainamide and selenium treatment were observed. These changes were found in four out of five rats in the Se group, eight out of ten in the P group, and in seven out of ten in the P + Se group. LE-like cells were observed in two rats in the P + Se group. A statistically significant decrease in plasma and liver TBARS by 20% and 36%, respectively, increased activity of SOD by 20%, catalase by 48% and Se-GPX by 15% in erythrocytes, and decreased activity of liver SOD by 17% and catalase by 22% were found in the P + Se group as compared to the P group. These results indicated that selenium exerted antioxidant effects on the procainamide-treated rats. However, selenium did not prevent the development of disturbances in leukocyte morphology, on the contrary, it possibly promoted the conversion of leukocytes to LE cells.

Published

1993

20. Popliteal lymph node response to procainamide and isoniazid. Role of beta-naphthoflavone, phenobarbitone and S9-mix pretreatment.

Author

Patriarca C, Verdier F, Brouland JP, and Descotes J

Subjects

Animals, Autoimmune Diseases chemically induced, Biotransformation, Drug Evaluation, Preclinical, Enzyme Induction, Female, Isoniazid pharmacokinetics, Knee, Male, Models, Biological, Procainamide pharmacokinetics, Rats, Rats, Inbred BN, Rats, Sprague-Dawley, Time Factors, beta-Naphthoflavone, Benzoflavones pharmacology, Isoniazid toxicity, Liver Extracts pharmacology, Lymph Nodes drug effects, Phenobarbital pharmacology, Procainamide toxicity

Abstract

The popliteal lymph node assay (PLNA) was proposed for the preclinical prediction of xenobiotics-induced autoimmune reactions in humans. Among the substances so far tested in this model, procainamide and isoniazid gave negative PLNA responses despite reports of lupus syndromes in man. To confirm the hypothesis that a metabolite instead of the parent molecule is involved, rats were pretreated with phenobarbital or beta-naphthoflavone, then injected with procainamide or isoniazid. In additional groups of animals, procainamide or isoniazid were injected together with S9-mix following various incubation times. Pretreated rats had a positive PLNA response when injected with procainamide, whereas preincubation with S9-mix resulted in a positive response to isoniazid. These results further support the validity of the PLNA.

Published

1993

21. Proarrhythmic effects of procainamide and tocainide in a canine infarction model.

Author

Steinberg JS, Sahar DI, Rosenbaum M, Cook JR, and Bigger JT Jr

Subjects

Animals, Blood Pressure drug effects, Dogs, Electric Stimulation, Electrocardiography, Electrophysiology, Heart drug effects, Heart physiology, Heart Rate drug effects, Heart Ventricles drug effects, Ventricular Fibrillation physiopathology, Ventricular Function, Arrhythmias, Cardiac chemically induced, Myocardial Infarction physiopathology, Procainamide toxicity, Tocainide toxicity

Abstract

A canine model of myocardial infarction (MI) was used to study the type and frequency of ventricular antiarrhythmic and proarrhythmic effects due to procainamide and tocainide and the risk factors associated with development of proarrhythmia. An anterior MI was created by a 2-h occlusion of the left anterior descending artery (LAD) with complete reperfusion. Programmed ventricular stimulation was performed on two occasions after MI, on days 4-6 and on days 8-10, before drug and during antiarrhythmic drug infusion at three dose levels. The antiarrhythmic drugs were given in a randomized cross-over design. Only procainamide caused a dose-dependent increase in QRS, JTc, and right ventricular effective refractory period (ERP). Neither procainamide nor tocainide made sustained ventricular tachycardia (VT) noninducible, but procainamide slowed the tachycardia rate. Both drugs successfully made ventricular fibrillation (VF) noninducible: procainamide in 78% of trials and tocainide in 50% of trials. Proarrhythmia (development of inducible VT during drug when not present before drug or inability to terminate VT during drug administration) developed in 29% of dogs that received procainamide and 25% of dogs that received tocainide. There was no apparent correlation of QRS, JTc, and right ventricular ERP after drugs and proarrhythmia due to procainamide or tocainide. There was no significant difference in the size of MI between dogs with one or more proarrhythmic response to either drug and dogs that had no proarrhythmia. In this model, procainamide and tocainide had no antiarrhythmic efficacy for VT, but had moderate proarrhythmia potential that was unpredictable.

Published

1992

22. Exacerbated muscle dysfunction by procainamide in rats with experimental myasthenia gravis.

Author

Yeh TM, Tami JA, and Krolick KA

Subjects

Animals, Antibodies immunology, Disease Models, Animal, Dose-Response Relationship, Drug, Female, Rats, Rats, Inbred Lew, Receptors, Cholinergic immunology, Receptors, Cholinergic metabolism, Autoimmune Diseases physiopathology, Muscle Contraction drug effects, Myasthenia Gravis physiopathology, Procainamide toxicity

Abstract

The induction of experimental autoimmune myasthenia gravis (EAMG) has long been shown to result in inefficient function of the acetylcholine receptor (AChR) and concomitant impairment of AChR-dependent neuromuscular communication. As an animal model of human myasthenia gravis, AChR-immunized rats demonstrate symptoms of MG very similar to those observed in human patients resulting from the presence of circulating anti-AChR antibodies which interfere with the normal function of the receptor. In addition to antibody antagonists of neuromuscular function, a variety of drugs have been observed to be associated with possible exacerbations of impaired neuromuscular function leading to myasthenic crisis in some MG patients. One drug, the cardiac anti-arrhythmic agent, procainamide, has been reported to cause both pre-synaptic and post-synaptic electrophysiologic effects at the neuromuscular junction. The study described below extends these observations to include the demonstration of perturbed AChR-dependent contractile muscle function in a rat model of MG.

Published

1992

23. A new series of antiarrhythmic procainamide derivatives: toxicity and activity-simulated passive absorption relation.

Author

Brazier M, Lefebvre C, Robert H, Reynaud P, Nguyen-Tri-Xuong E, Arnould-Guérin ML, and Pieri F

Subjects

Absorption, Animals, Anti-Arrhythmia Agents pharmacokinetics, Anti-Arrhythmia Agents toxicity, Biological Availability, Diffusion, Lethal Dose 50, Membranes, Artificial, Mice, Procainamide pharmacokinetics, Procainamide toxicity, Anti-Arrhythmia Agents chemical synthesis, Procainamide analogs & derivatives, Procainamide pharmacology

Abstract

Several compounds derived from benzamidines and nicotinic pyridinic amidines with a structure similar to that of procainamide, exhibit notable antiarrhythmic properties after injection into animals. The diffusion rate of these different compounds through a solid lipidic artificial membrane was studied with Dibbern's apparatus. A statistical relation was established between the diffusion rate and the principal pharmacological parameters obtained after intraperitoneal injection (toxicity and anthiarrhythmic activity). Essential structural elements seem to determine a better bioavailability than procainamide: character of the substitution (in para) of the benzenic cycle; length of the lateral chain.

Published

1990

24. [The effect of metabolic agents on the antiarrhythmic activity of novocainamide and acetylnovocainamide].

Author

Beregovaia EG, Gorchakova NA, Samarskaia TG, Dunaev VV, and Chekman IS

Subjects

Animals, Anti-Arrhythmia Agents toxicity, Arrhythmias, Cardiac chemically induced, Arrhythmias, Cardiac drug therapy, Calcium Chloride, Drug Evaluation, Preclinical, Drug Synergism, Drug Therapy, Combination, Isoproterenol, Lethal Dose 50, Myocardial Infarction chemically induced, Myocardial Infarction drug therapy, Pituitary Hormones, Posterior, Potassium therapeutic use, Procainamide toxicity, Rats, Rats, Inbred Strains, Succinic Acid, Anti-Arrhythmia Agents therapeutic use, Malates therapeutic use, Procainamide analogs & derivatives, Procainamide therapeutic use, Succinates therapeutic use

Abstract

The effects of potassium malate and sodium succinate on the antiarrhythmic activity of novocainamide and acetylnovocainamide during modelling of chlor-calcium-induced arrhythmia as well as in disorders of cardiac rhythm during modelling of pituitrin-isadrine-induced myocardial infarction were studied. The metabolic agents were found to increase the effectiveness of acetylnovocainamide and the toxicity of novocainamide. To interpret the specific features of the mechanism of the anti-arrhythmic action of the compounds there was studied their ability to form complexes with components of biomembranes and ions of biometals.

Published

1990

25. Applicability of the popliteal lymph node assay in the Brown-Norway rat.

Author

Verdier F, Virat M, and Descotes J

Subjects

Animals, Drug Evaluation, Preclinical, Female, Isoniazid toxicity, Lymph Nodes immunology, Lymph Nodes pathology, Male, Organ Size drug effects, Procainamide toxicity, Rats, Rats, Inbred BN, Streptozocin toxicity, Autoimmune Diseases chemically induced, Lymph Nodes drug effects

Abstract

A number of drugs and chemicals can induce autoimmune disorders. Previous studies suggested the popliteal lymph node (PLN) assay might be a suitable and reliable model to detect such compounds in the mouse. The applicability of this assay has been examined in the Brown-Norway rat using a panel of positive as well as negative reference compounds. Popliteal lymph nodes were excised and weighed seven days after subcutaneous injection of 5 mg of each compound into one footpad. Interestingly, all negative reference compounds produced no significant increase in PLN weight index whereas four positive reference compounds were associated with PLN-weight indices greater than 2.3. However, no increase in PLN weight was noted in procainamide- and isoniazide-treated rats as previously reported in the mouse. This first set of experiments indicates that the PLN assay is applicable to Brown-Norway rats and warrants further investigation.

Published

1990

26. Epicardial mapping of polymorphous ventricular tachycardias induced in the canine heart with procainamide.

Author

Murakawa Y, Inoue H, Toda I, Nozaki A, Kawakubo K, and Sugimoto T

Subjects

Animals, Arrhythmias, Cardiac physiopathology, Cardiac Pacing, Artificial, Dogs, Electrocardiography, Electrophysiology, Heart Conduction System physiopathology, Pericardium physiopathology, Procainamide toxicity, Arrhythmias, Cardiac chemically induced, Heart Conduction System drug effects, Procainamide pharmacology, Ventricular Fibrillation prevention & control

Abstract

To elucidate the mechanisms of the arrhythmogenic and antifibrillatory action of procainamide, 24 episodes of polymorphous ventricular tachycardia were analyzed. They were induced electrically in 12 canine hearts before and after the administration of 40 mg/kg of procainamide. The isochronal maps of the epicardial activation sequence were successfully constructed by 40 simultaneously recorded bipolar electrograms in 14 of 17 episodes after procainamide. The isochronal maps showed a possible macroreentrant circuit in 12 episodes, and in four of them the functional block was noticed to have disappeared before the termination of tachycardia. This study suggests that procainamide predisposes the ventricle to reentrant tachyarrhythmias and that the dimension of the reentrant circuit induced is too large to be fragmented into multiple reentries, which results in the prevention of the development of ventricular fibrillation.

Published

1988

27. Metabolism of procainamide to the cytotoxic hydroxylamine by neutrophils activated in vitro.

Author

Rubin RL and Curnutte JT

Subjects

Adult, B-Lymphocytes metabolism, Biotransformation, Cell Line, Chromatography, High Pressure Liquid, Female, Humans, Hydrogen Peroxide, Hypochlorous Acid, Male, Neutrophils drug effects, Neutrophils physiology, Oxygen Consumption drug effects, Procainamide toxicity, Neutrophils metabolism, Phagocytosis drug effects, Procainamide analogs & derivatives, Procainamide metabolism

Abstract

An almost universal side effect of long-term therapy with procainamide is the appearance of serum autoantibodies and less frequently a syndrome resembling lupus erythematosus. Previous studies demonstrated that procainamide-hydroxylamine (PAHA), a metabolite generated by hepatic mixed function oxidases, was highly toxic to dividing cells, but evidence that PAHA could be formed in the circulation was lacking. This study examines the capacity of neutrophils to metabolize procainamide to reactive forms. Neutrophils activated with opsonized zymosan were cytotoxic only if procainamide was present, whereas N-acetyl procainamide, which does not induce autoimmunity, was inert in this bioassay. PAHA was detected by HPLC in the extracellular medium if ascorbic acid was present. Generation of PAHA and cytotoxic procainamide metabolites was inhibited by NaN3 and catalase but not by superoxide dismutase, indicating that H2O2 and myeloperoxidase were involved. Nonactivated neutrophils and neutrophils from patients with chronic granulomatous disease did not generate cytotoxic PAHA, demonstrating that H2O2 was derived from the respiratory burst accompanying neutrophil activation. These conclusions were supported by results of a cell-free system in which neutrophils were replaced by myeloperoxidase and H2O2 or an H2O2 generating system. These studies demonstrate the capacity of neutrophils to mediate metabolism of procainamide and establish the role of myeloperoxidase released during degranulation and H2O2 derived from the respiratory burst in the direct cooxidation of procainamide to PAHA. The profound biologic activity of this metabolite and its possible generation within lymphoid compartments implicate this process in the induction of autoimmunity by procainamide.

Published

1989

28. Diaphragmatic paralysis.

Author

Javaheri S, Logemann TN, Corser BC, Guerra LF, and Means E

Subjects

Aged, Humans, Male, Respiratory Insufficiency chemically induced, Procainamide toxicity, Respiratory Paralysis chemically induced

Published

1989

29. Procainamide induces a transitory impairment of B cell mitogenesis in beagle dogs.

Author

Mulhern SA, Daguillard F, Robinson CJ, and Balazs T

Subjects

Animals, Cell Division drug effects, DNA biosynthesis, Dogs, Female, Flow Cytometry, Fluorescent Antibody Technique, Male, Membrane Potentials drug effects, Mitogens pharmacology, Thymidine analogs & derivatives, Thymidine metabolism, Time Factors, B-Lymphocytes drug effects, Mitosis drug effects, Procainamide toxicity

Abstract

Beagle dogs (3 to 6 years old) were treated with 100-150 mg procainamide HC1/kg/day. After 2, 5, and 9 months of treatment, peripheral blood lymphocytes were isolated and stimulated with pokeweed mitogen. The data demonstrated a suppression of mitogenesis only at 2 and 5 months after procainamide treatment. The lymphocytes from dogs treated for 9 months had a normal response to pokeweed mitogen. At no time during this experiment were any significant levels of serum antinuclear antibodies detected nor was any change in the number of cycling lymphocytes apparent in the experimental versus control groups. The resting membrane potential of both control and experimental groups was similar and pokeweed mitogen depolarized the cells from both groups.

Published

1988

30. Prolongation of procaine's and procainamide's actions by binding to acryloyl polymers.

Author

Erker EF, Baker T, Okamoto M, Udenfriend S, and Riker WF Jr

Subjects

Acrylic Resins toxicity, Animals, Arrhythmias, Cardiac chemically induced, Arrhythmias, Cardiac drug therapy, Cats, Dose-Response Relationship, Drug, Female, Kinetics, Lethal Dose 50, Male, Mice, Procainamide toxicity, Procaine toxicity, Acrylic Resins pharmacology, Procainamide analogs & derivatives, Procainamide pharmacology, Procaine analogs & derivatives, Procaine pharmacology

Abstract

Procaine and procainamide were covalently bound to acryloyl monomers and polymers. The dose-response and time-action parameters of the cardiac antiarrhythmic protection afforded by the prototype drugs and their acryloyl derivatives against chloroform-hypoxia-induced cardiac arrhythmias in unanesthetized mice and epinephrine-induced arrhythmias in alpha-chloralose anesthetized cats were determined. Similarly, the pharmacological parameters which characterized their acute toxic responses in unanesthetized male albino mice were also determined. The similar pharmacological spectra of their activity and the parallelism of their lethal dose-response curves indicate that the active constituents of the polymer derivatives are the local anesthetic moieties. Compared to the prototype drugs, the polymer derivatives were more potent on a molar basis and their pharmacological effects were prolonged. The increased potency and duration of action reinforce the idea that the local anesthetic moieties are pharmacologically active while still bound to the polymer backbones.

Published

1985

31. Procainamide hydroxylamine lymphocyte toxicity--I. Evidence for participation by hemoglobin.

Author

Roberts SM, Adams LE, Donovan-Brand R, Budinsky R, Skoulis NP, Zimmer H, and Hess EV

Subjects

Acecainide toxicity, Animals, Ascorbic Acid pharmacology, Carbon Monoxide pharmacology, Chemical Phenomena, Chemistry, In Vitro Techniques, Liver drug effects, Male, Methemoglobin biosynthesis, Monocytes drug effects, Monocytes metabolism, Procainamide chemical synthesis, Procainamide toxicity, Rats, Rats, Inbred Strains, Spleen cytology, Spleen drug effects, Thymidine metabolism, Hemoglobins physiology, Lymphocytes drug effects, Procainamide analogs & derivatives

Abstract

A number of lines of evidence suggest that the lupus-like symptoms associated with procainamide therapy may be caused by products of metabolic N-oxidation. In the present study, the perfusion of the isolated rat liver with a hemoglobin-free solution containing procainamide (100 microM) resulted in the rapid appearance of the N-oxidation metabolite procainamide hydroxylamine in the perfusate. Addition of procainamide hydroxylamine in vitro to whole rat blood (1-40 microM) resulted in a concentration-dependent loss of proliferative response among mononuclear cells isolated from the treated blood and cultured with mitogens (phytohemagglutinin, PHA-P: concanavalin A, Con A; and pokeweed mitogen, PWM), as well as a loss of viability. Similar effects on lymphocyte mitogen responsiveness were observed when procainamide hydroxylamine (1-40 microM) was added to rat whole splenic cell populations. Carbon monoxide or ascorbic acid pretreatment inhibited the toxicity of procainamide hydroxylamine to lymphocytes in whole blood, but only carbon monoxide pretreatment inhibited procainamide hydroxylamine-induced methemoglobin formation. These observations are consistent with the participation of hemoglobin in a redox cycle with procainamide hydroxylamine, generating products which are primarily responsible for its cytotoxicity in blood.

Published

1989

32. Drug polymer combinations IV. Toxicity screening of procainamide and its methacrylamide derivates on Artemia.

Author

Gyselinck P, Van Severen R, Braeckman P, Van Haecke P, and Schacht E

Subjects

Animals, Artemia drug effects, Procainamide toxicity

Published

1981

33. Pharmacologic therapy of ventricular arrhythmias.

Author

Winkle RA, Glantz SA, and Harrison DC

Subjects

Anti-Arrhythmia Agents pharmacology, Anti-Arrhythmia Agents toxicity, Arrhythmias, Cardiac etiology, Drug Therapy, Combination, Humans, Kinetics, Lidocaine metabolism, Lidocaine pharmacology, Lidocaine toxicity, Models, Biological, Procainamide metabolism, Procainamide pharmacology, Procainamide toxicity, Propranolol metabolism, Propranolol pharmacology, Propranolol toxicity, Quinidine metabolism, Quinidine pharmacology, Quinidine toxicity, Anti-Arrhythmia Agents therapeutic use, Arrhythmias, Cardiac drug therapy

Abstract

To treat patients with ventricular arrhythmias properly, one must characterize the arrhythmia, define the underlying heart disease and look for and treat reversible causes. When arrhythmias are suitable for pharmacologic suppression, it is necessary to predefine therapeutic goals, then carefully document that the drug accomplishes these goals. Knowledge of a drug's metabolism, excretion, active metabolites and plasma protein binding is often required for full understanding of its clinical effect. Pharmacokinetic principles require that antiarrhythmic drugs be given on a rigid schedule and that plasma drug levels be frequently determined. Use of compartment models and the principle of superposition can enable one to achieve and maintain therapeutic drug concentrations while avoiding toxic side effects. The drugs commonly used to treat arrhythmias, lidocaine, propranolol, procainamide, diphenylhydantoin and quinidine, as well as some newer agents, have specific pharmacokinetics and toxic effects that must be understood.

Published

1975

34. Comparative vagolytic effects of procainamide and N-acetylprocainamide in the dog.

Author

Pearle DL, Souza JD, and Gillis RA

Subjects

Animals, Blood Pressure drug effects, Dogs, Female, Heart Rate drug effects, Male, Vagus Nerve physiology, Acecainide toxicity, Procainamide analogs & derivatives, Procainamide toxicity, Vagus Nerve drug effects

Abstract

Procainamide exerts vagolytic effects which are deleterious in clinical therapy for supraventricular arrhythmias. The purpose of the present study was to determine if N-acetylprocainamide (NAPA), an active metabolite of procainamide which has been proposed as an effective and less toxic alternative, would exert an equivalent degree of vagal blockade. In anesthetized dogs, the right cervical vagus nerve was electrically stimulated at supramaximal voltage using frequencies from 0.5 to 20 Hz to slow the sinus rate. The ability of NAPA and procainamide to block this response was tested with infusion of equimolar doses (1.0 and 0.87 mg/kg/min i.v., respectively) continuously over a period of 40-78 min. Both drugs exerted statistically significant vagolytic effects at the higher frequencies of stimulation. Although the vagolytic effect appeared to be more pronounced with procainamide, this could not be demonstrated by statistical analysis of the data.

Published

1983

35. [Untoward effects of novocaine amide].

Author

STEIMATSKII AR and ANDREEVA ST

Subjects

Procainamide toxicity, Procaine

Published

1959

36. Treatment of procaine amide intoxication; an experimental study.

Author

WASSERMAN F, BRODSKY L, KATHE JH, DICK MM, and RODENSKY PL

Subjects

Humans, Lactates pharmacology, Norepinephrine pharmacology, Procainamide toxicity

Published

1959

37. Pharmacokinetic of procainamide in man.

Author

Koch-Weser J

Subjects

Administration, Oral, Arrhythmias, Cardiac drug therapy, Blood Urea Nitrogen, Half-Life, Humans, Injections, Intramuscular, Injections, Intravenous, Intestinal Absorption, Kinetics, Procainamide administration & dosage, Procainamide blood, Procainamide therapeutic use, Procainamide toxicity, Procainamide metabolism

Published

1971

38. Treatment of procaine amide intoxication.

Author

RODENSKY PL and WASSERMAN F

Subjects

Humans, Lactates therapy, Norepinephrine therapy, Procainamide toxicity

Published

1959

39. Antiarrhythmic activity of some isoquinoline derivatives determined by a rapid screening procedure in the mouse.

Author

Lawson JW

Subjects

Animals, Atropine pharmacology, Atropine toxicity, Chloroform, Diphenhydramine pharmacology, Electrocardiography, Female, Methods, Methoxamine pharmacology, Mice, Naphazoline pharmacology, Oxyphenonium pharmacology, Oxyphenonium toxicity, Papaverine pharmacology, Phenylephrine pharmacology, Procainamide pharmacology, Procainamide toxicity, Propranolol pharmacology, Propranolol toxicity, Quinidine pharmacology, Quinidine toxicity, Reserpine pharmacology, Ventricular Fibrillation chemically induced, Anti-Arrhythmia Agents pharmacology, Heart Rate drug effects, Quinolines pharmacology

Published

1968

40. [Change of toxicity of procaine, procaine amide and tetracaine by ingredients of lytic mixtures].

Author

WELLHOENER HH, HARTMANN H, HEIDEL J, and MASCHHOUR M

Subjects

Humans, Anesthetics, Anesthetics, Local toxicity, Procainamide toxicity, Procaine toxicity, Tetracaine

Published

1959