ACUTE SELF-POISONINGS BY VERAPAMIL B.Pavlovski, J.Pavlovska, T. Panovska, C.Bozinovska, N.Popovski, N. Becarovski, L.Meloska, Z. Pereska Clinic of Toxicology and Urgent Internal Medicine and Institute of Cardiology. Clinical Center. Skopje. R. Macedonia
CALCIUM ANTAGONISTS: VERAPAMIL (PROTECTIVE NAME), ISOPTIN. LECOPTIN,VERAPAMILUM, VERANORM), NIFEDIPIN DILTIAZEM AMLODIPIN NICARDIPIN NITRENDIPIN
PHARMACODYNAMIC PROPERTIES VERAPAMIL IS A PHENYLALKYLAMINE DERIVATIVE WHICH ANTAGONISES CALCIUM INFLUX THROUGH THE SLOW CHANNELS OF VASCULAR SMOOTH MUSCLE AND CARDIAC CELL MEMBRANES. BY REDUCING INTRACELLULAR FREE CALCIUM CONCENTRATIONS, VERAPAMIL CAUSES CORONARY AND PERIPHERAL VASODILATATION AND DEPRESS MYOCARDIAL CONTRACTILITY AND ELECTRICAL ACTIVITY IN THE ATRIOVENTRICULAR AND SINOATRIAL NODES
PHARMACOKINETIC PROPERTIES ON CALCIUM ANTAGONISTS Bioavailability p.binding.p T/2 renal elimination VERAPAMIL 10-20 90 3-7hours 60-70% DILTIAZEM 40 80 3-5 NIFEDIPIN 50 96 2 AMLODIPIN 52-88 97 33 EFFECT AFTER 30-60 min. PHARMACOLOGICAL RESPONSE ON DEPURATION TECHNICS
CLINICAL PHARMACOLOGY ON CALCIUM ANTAGONISTS------TOXICOLOGICAL VIEW PHARMACODYNAMIC MECHANISM AND CONSEQUENCES ON MYOCARDIUM, CONDUCTION SYSTEM AND BLOOD VESSELS DECREASE: 1.CONTRACTILITY 2. AV-CONDUCTION 3. TONUS OF BLOOD VESSELS BRADYCARDIA, BLOCKS, HYPOTENSION, HYPOXIA, SHOCK, DYSMETABOLIC CHANGE PHARMACOLOGICAL RESPONSE: INCREASE: 1. CONTRACTILITY
THE AIM OF THIS STUDY WAS TO EVALUATE THE THERAPEUTIC APPROACH BY VERAPAMIL POISONINGS, ALONE AND COMBINED WITH THE OTHER DRUGS
MATERIAL AND METHOD: We have observed thirty eight patients acutely intoxicated by Verapamil of both sexes,(29 women and 9 men). The mean age of this group was 29 +-3 years. Other drugs also were ingested by twenty five patients. (Antibiotics, Benzodiazepines, Vitamins and Beta-Blockers in one case. The dose ingested ranged between 10 t0 40 tablets(800mgr to 3,2gr).All patients have treated in the Inensive Care Unit
THERAPEUTIC PROCEDURES: Drug removal by gastric lavage and administration of charcoal was the mainstay of the therapy in the firsts hours since ingestion.AV-blocks, I- II- grades, have treated with Atropin and Orciprenalin.The treatment of cardiogenic shock included artificial ventilation, several vasopresors, Dopamin, inotropic agents, plazma expanders and temporary pacemacer at one case(intoxicated by Verapamil and Atenolol). Calcium Gluconatum as antidote was given to every patients. Othervise, vigorous fluid resuscitation, cardiac pacing and control of acid-base status and electrolytes measurements provided the basic of the therapy.
CLINICAL PICTURES: GASTRIC SYNDROME CARDIOVASCULARE SYNDROME CEREBRAL SYNDROME DISMETABOLIC SYNDROME CARDIAC DYSRHYTHMIAS: LOW GRADE- SINUS BRADICARDIAS MILD GRADE- HYPOTENSION, AV- BLOCKS I- AND II- GRADES HARD GRADE- BRADYARHYTHMIAS, SHOCK
TIME AFTER ARRIVAL BP HR Ecg 0 1 6 12 36h 120/8o 100/7o 90/60 11o/65 120/7o 75 55 6o 7o 75 NSR AVB AVB AVB AVB I
TIME AFTER ADMISSION(h) 132 134 136 138 3,6 3,3 3,6 3,9 4,o 6,o 12,o 11,0 7,o 6,0 Three hours after a,patients were hypokalemic and hyperglycemic. N K Gly
ALL PATIENTS DEVELOPED CARDIAC CONDUCTION ABNORMALITIES AND BECOME HYPOTENSIVE. BLOOD PRESSURE WAS ON AVERAGE < 90/60 mmHg. HEART RATE ON AVERAGE < 50+-5, PROLONGED PQ INTERVAL HAD 22 PATIENTS, AV- BLOCKS II- GRADES HAD 13 PATIENTS AND TOTAL AV-BLOCKS HAD 3 PATIENTS.
RESULTS AND CONCLUSIONS: IN DESPITE OF INTENSIVE THERAPY , SEVERAL VASOPRESSORS, INOTROPIC AGENTS, NOOTROPIC DRUGS, Calcium Gluconatum, Glucagon, implantations of cardiac pacemacer, one patient died of hypotension and cardiac conduction total AV-block, 24 hours after overdose.The other patients recovered without deficit and were discharged from the Intensive Care Unit three days later.