DOCSLIB.ORG

HYPAM Triazolam Tablets 0.125Mg and 0.25Mg

Total Page:16

File Type:pdf, Size:1020Kb

Download full-text PDF Read full-text
HYPAM Triazolam Tablets 0.125Mg and 0.25Mg NEW ZEALAND CONSUMER MEDICINE INFORMATION HYPAM Triazolam Tablets 0.125mg and 0.25mg HYPAM is available on prescription • If you have a liver or kidney What is in this leaflet from your doctor. problem • If you have sleep apnoea (when This leaflet answers some common breathing either slows or stops questions about HYPAM. Before you take for short periods while sleeping) HYPAM • If you have fits or convulsions It does not contain all the • If you have myasthenia gravis, a information available on this disease that causes severe medicine. It does not take the place When you must not take muscle weakness of talking to your doctor or it • If you have or have had pharmacist. depression or psychotic Do not take HYPAM if: tendencies All medicines have risks and • If you have glaucoma (high benefits. Your doctor has weighed • You are allergic to triazolam or pressure in the eye) the risks of using HYPAM against any of other related • If you have a history of the benefits expected it will have for benzodiazepine, or alcoholism or drug abuse you. • You are allergic to any of the • If you are pregnant or plan on other ingredients listed at the becoming pregnant If you have any concerns about end of this leaflet • If you are breastfeeding or plan using this medicine, ask your to breastfeed doctor or pharmacist. Symptoms of an allergic reaction may include shortness of breath, HYPAM is not recommended for Keep this leaflet. You may want wheezing or difficulty breathing, use in children. The safety and to read it again. swelling of the face, lips, tongue or effectiveness of HYPAM, has not other parts of the body; rash, itching been established in children. or hives on the skin. What HYPAM is Taking other medicines Do not take HYPAM if you are used for and how it taking the following medicines: If you are taking any other works medicines, including any you get • Ketoconazole and without a prescription from a itraconazole, medicines used pharmacy, supermarket or health Your HYPAM tablets contain the to treat fungal infections food shop, tell your doctor or active ingredient triazolam. • Nefazodone, a medicine used pharmacist. Triazolam belongs to a group of medicines known as to treat depression • Medicines that may interfere with benzodiazepines. They are thought Ritonavir (Norvir), lopinavir HYPAM include: to work by changing the amounts of (Kaletra), indinavir (Crixivan), certain chemicals found in the brain atazanavir (Reyataz) and darunavir (Prezista); • Other sleeping tablets, sedatives HYPAM is used to treat patients medicines to treat HIV or tranquilisers • that have problems sleeping infections Muscle relaxants • (insomnia). It should be used for Medicines used to treat fungal short-term treatment only, usually 7- These medicines and HYPAM will infections eg. voriconazole, 10 days. Continued use is not interfere with each other. miconazole etc. recommended unless advised by • Macrolide antibiotics such as your doctor. The use of Before you take it erythromycin, clarithromycin, benzodiazepines may lead to troleandomycin, used in the Tell your doctor: dependence when used long term. treatment of various infections • Cimetidine, a medicine used to • Your doctor, however, may have If you have allergies to any other treat reflux and ulcers prescribed HYPAM for another medicines or other substances • Isoniazid, a medicine used to reason. Ask your doctor if you have including foods and dyes. treat tuberculosis • any questions about why HYPAM If you have heart or lung • Medicines for depression, has been prescribed for you. problems anxiety or mood disorders eg. Page 1 of 3 sertraline, paroxetine, Taking your medicine at the same Do not stop taking HYPAM without fluvoxamine time each day may help you to first checking with your doctor. • Medicines used for various heart remember to take it regularly. If you Stopping this medicine suddenly conditions eg. diltiazem, have trouble remembering to take may cause some unwanted effects, verapamil your medicine, ask you pharmacist e.g. Rebound insomnia. The dose • Medicines used to control fits for some hints. should be lowered gradually to • Pain relievers or opioids minimize such effects. Discuss with • Medicines for allergies e.g. your doctor how this could be done. antihistamines, or cold tablets While you are taking • Medicines to control alcohol HYPAM problems, e.g. disulfiram Side effects These medicines may be affected Tell all doctors, dentists and Tell your pharmacist or doctor as by HYPAM or may affect how well pharmacists who are treating you soon as possible if you do not feel HYPAM works. You may need that you are taking HYPAM. well while you are taking HYPAM. different amounts of your medicines or you may need to take different Tell your doctor or pharmacist that All medicines can have some medicines. you are taking HYPAM before you unwanted effects. Sometimes they start any new medicine. are serious, most of the time they Your doctor or pharmacist has more are not. You may need medical information on medicines to be Tell your doctor if you develop a treatment if you get some of the careful with or avoid while taking skin rash or hives while taking side effects. HYPAM. HYPAM. Tell your doctor or pharmacist if Do not have any grapefruit juice if Tell your doctor if you become you notice any of the following you are taking HYPAM tablets as pregnant while taking HYPAM. and they worry you: grapefruit juice may interfere with HYPAM. If you are going to have a surgery, • Drowsiness, dizziness, tell the surgeon or anaesthetist that lightheadedness you are taking HYPAM. • Difficulty concentrating How to take HYPAM If you are going to have any blood These side effects are usually mild tests, tell your doctor that you are properly and are dose related. taking HYPAM. How much to take Tell your doctor immediately if Do not take HYPAM to treat any you experience: Your doctor will tell you how much other complaints unless your doctor HYPAM you need to take each day. tells you to. • It is important that you take HYPAM Confusion, memory loss • as directed by your doctor. Do not Do not give this medicine to anyone Visual problems • take more than the recommended else, even if they have the same Nervousness, excitation or dose. condition as you. aggressive behaviour • Falling (especially in the elderly) • The usual starting dose of HYPAM HYPAM causes drowsiness and Hallucinations, sleep walking or for all patients is 0.125mg per day, tiredness and therefore may affect other behaviours while you are taken immediately before going to how alert you are. Even if you take asleep bed at night. Treatment should not HYPAM at night, you may still be • Feeling depressed continue for longer than 7 to 10 drowsy or dizzy the next day. Be • Altered mood consecutive days. A dose of careful when driving, operating • Difficulty with coordination 0.25mg should not be exceeded. machinery or performing jobs • Rebound insomnia that need you to be alert, until • Pains or cramps How long to take it you are certain that HYPAM is not • Nausea, vomiting affecting your performance. HYPAM should be used for short If any of the following happen, periods only. Continuous long-term Do not take HYPAM where a full stop taking HYPAM and tell your treatment is not recommended night’s sleep is not possible and the doctor immediately, or go to unless advised by your doctor. next day you need to be active and accident and emergency at your Long-term use may lead to functional. nearest hospital: dependence. Avoid alcohol while taking HYPAM. • Swelling of the face, lips, mouth If you forget a dose Drinking alcohol while affect how or throat which may cause well HYPAM works and can make difficulty in swallowing or If you forget a dose, just take the you more sleepy, dizzy or breathing next dose when it is due. Do not lightheaded. take more than one dose at a time to make up for missed doses. Page 2 of 3 The list of side effects mentioned above is not complete. If you Product Description should suffer from any of these side effects or any other undesired effect please tell your doctor or What HYPAM tablets pharmacist. look like HYPAM 0.125mg tablets are flat, Do not be alarmed by this list of oval shaped, white tablets that are possible side effects. You may not marked with “TZ” on one side and a experience any of them. break line on the other. HYPAM 0.25mg tablets are flat, In case of overdose oval shaped, blue tablets that are marked with a “TZ” on one side and You should only take the number of a break line on the other. tablets that you have been told. Each HYPAM tablet contains the Immediately contact your doctor active ingredient, triazolam. or the National Poisons Information Centre (0800 POISON Both HYPAM 0.125mg and HYPAM or 0800 764 766) or go to the 0.25mg tablets also contain the Emergency department at your ingredients lactose, maize starch, nearest hospital, if you think that microcrystalline cellulose, povidone, you may have taken too much, or colloidal silicon dioxide, sodium if anyone else has taken any lauryl sulphate, sodium starch HYPAM by mistake. Do this even glycollate and magnesium stearate. if there are no signs of HYPAM 0.25mg tablets also contain discomfort or poisoning. You FD & C Blue No. 2, as a colouring may need urgent medical agent. attention. Take the container of HYPAM with you if you can. HYPAM tablets do not contain gluten. Keep telephone numbers for these places handy. If you want to know Storage conditions more Do not take this medicine after the Should you have any questions expiry date shown on the label or if regarding this product, please the packaging shows signs of contact your doctor or pharmacist.
Load more

Recommended publications
  • Early Morning Insomnia, Daytime Anxiety, and Organic Mental Disorder Associated with Triazolam
    Early Morning Insomnia, Daytime Anxiety, and Organic Mental Disorder Associated with Triazolam Tjiauw-Ling Tan, MD, Edward 0. Bixler, PhD, Anthony Kales, MD, Roger J. Cadieux, MD, and Amy L. Goodman, MD Hershey, Pennsylvania A psychiatric syndrome characterized by agita­ Sleep Disorders Clinic. He began taking triazolam tion, paranoid ideation, depersonalization, and de­ at bedtime in a 0.5-mg dose eight months before pression, as well as paresthesias and hyperacusis, his referral. Although the drug was effective ini­ has been attributed to administration of triazolam tially, tolerance developed, causing the patient to (Halcion).1 The occurrence of these reactions led gradually increase the dosage until eventually he to the removal of the drug from the market in the was taking a total of 1.5 mg nightly. Netherlands. Isolated behavioral side effects that The physical examination revealed no contribu­ include amnesia2-4 and hallucinations5 have also tory conditions. However, assessment of the pa­ been reported with administration of triazolam. tient’s mental status revealed that he was extreme­ Rebound insomnia6 and early morning insom­ ly guarded and suspicious and preoccupied with nia,7 both associated with increases in daytime his sleeplessness to the degree that this hypochon­ anxiety,7,8 are withdrawal syndromes known driacal concern had a delusional quality. He also to occur with rapidly eliminated benzodiazepine described two episodes indicating memory impair­ hypnotics such as triazolam. Rebound insomnia ment; both incidents occurred in the late afternoon consists of a marked increase in wakefulness and involved preparing to eat certain foods, which above baseline levels following drug withdrawal.
    [Show full text]
  • Triazolam (Halcion®) Instructions
    Mark Sebastian, DMD 33516 Ninth Ave. South, #2 Federal Way, WA 98003 (253) 941-6242 --or -- (253) 952-2005 [email protected] www.MarkSebastianDMD.com Triazolam (Halcion®) instructions If prescribed, take the diazepam (Valium®) pill just before bed the night before your dental surgery for a better night’s sleep. If you take other sleeping medications, take those instead of the diazepam (Valium®). Do not mix the two. If you have a morning appointment, you should to fast from solid foods after midnight. If you have an afternoon appointment, have a light breakfast. Unless you have a medical reason to eat (diabetic, etc.), do not eat anything for 6 hours before your appointment time. Water, apple juice, and black decaffeinated coffee/tea are OK for 3 hours before your appointment. Triazolam (Halcion®) is absorbed better on an empty stomach. Do not take caffeine or sugar) for 3 hours before your appointment, as all are stimulants that decrease the effectiveness of triazolam (Halcion®). No tobacco use for 8 hours before, as it is a stimulant. Take the triazolam (Halcion®) or diazepam (Valium®) pill(s) with a glass of water. Sparkling water makes them absorb better. Alcohol---do not drink within 24 hours before to 24 hours after taking triazolam (Halcion®) or diazepam (Valium®). Recreational/illegal drugs---Do not use for 7 days before your dental surgery and until 7 days after (never if you are taking narcotic pain medication). Example—using cocaine and then having local anesthetics (novocaine) can kill you. Do not take triazolam (Halcion®) or diazepam (Valium®) if you are allergic to triazolam (Halcion®), alprazolam (Xanax®), chlordiazepoxide (Librium®, Librax®), clonazepam (Klonopin®), clorazepate (Tranxene®), diazepam (Valium®), estazolam (ProSom®), flurazepam (Dalmane®), lorazepam (Ativan®), oxazepam (Serax®), prazepam (Centrax®), temazepam (Restoril®).
    [Show full text]
  • Effects of Benzodiazepines on Sleep and Wakefulness
    Br. J. clin. Pharmac. (1981), 11, 31S-35S EFFECTS OF BENZODIAZEPINES ON SLEEP AND WAKEFULNESS T. ROTH, F. ZORICK, JEANNE SICKLESTEEL & E. STEPANSKI Sleep Disorders and Research Center, Henry Ford Hospital, Detroit, Michigan The differential effects of short and long acting benzodiazepines on sleeping and waking behaviour are discussed, with particular reference to hypnotic efficacy, and their effects on the structure ofsleep and daytime function. Introduction THE evaluation of any drug requires an understand- et al., 1979), and triazolam (Metzler et al., 1977) have ing of the conditions in which it is going to be used come into clinical use. The present report will present clinically. In the case of hypnotics, the most appro- the differential effects of short- and long-acting ben- priate use is symptomatic relief for the complaint of zodiazepines on sleeping and waking behaviour. insomnia. To understand fully the safety and efficacy ofthese drugs, we must first be aware of the constella- tion of symptoms associated with the complaint of Sleep parameters insomnia, as well as what these drugs do to each of these symptoms. In evaluating the effects of hypnotics on sleep, two Insomnia is a complaint. Although all of the types of parameters should be considered. The first aetiological factors which give rise to this symptom set of parameters deal with hypnotic efficacy and are not currently well understood, there is an accepted include measures such as latency to sleep onset, total diagnostic system for the various disorders associated sleep time, number and duration of awakenings, and with disturbed nocturnal sleep (Association of Sleep sleep efficiency.
    [Show full text]
  • Comparison of Short-And Long-Acting Benzodiazepine-Receptor Agonists
    J Pharmacol Sci 107, 277 – 284 (2008)3 Journal of Pharmacological Sciences ©2008 The Japanese Pharmacological Society Full Paper Comparison of Short- and Long-Acting Benzodiazepine-Receptor Agonists With Different Receptor Selectivity on Motor Coordination and Muscle Relaxation Following Thiopental-Induced Anesthesia in Mice Mamoru Tanaka1, Katsuya Suemaru1,2,*, Shinichi Watanabe1, Ranji Cui2, Bingjin Li2, and Hiroaki Araki1,2 1Division of Pharmacy, Ehime University Hospital, Shitsukawa, Toon, Ehime 791-0295, Japan 2Department of Clinical Pharmacology and Pharmacy, Neuroscience, Ehime University Graduate School of Medicine, Shitsukawa, Toon, Ehime 791-0295, Japan Received November 7, 2007; Accepted May 15, 2008 Abstract. In this study, we compared the effects of Type I benzodiazepine receptor–selective agonists (zolpidem, quazepam) and Type I/II non-selective agonists (zopiclone, triazolam, nitrazepam) with either an ultra-short action (zolpidem, zopiclone, triazolam) or long action (quazepam, nitrazepam) on motor coordination (rota-rod test) and muscle relaxation (traction test) following the recovery from thiopental-induced anesthesia (20 mg/kg) in ddY mice. Zolpidem (3 mg/kg), zopiclone (6 mg/kg), and triazolam (0.3 mg/kg) similarly caused an approximately 2-fold prolongation of the thiopental-induced anesthesia. Nitrazepam (1 mg/kg) and quazepam (3 mg/kg) showed a 6- or 10-fold prolongation of the anesthesia, respectively. Zolpidem and zopiclone had no effect on the rota-rod and traction test. Moreover, zolpidem did not affect motor coordination and caused no muscle relaxation following the recovery from the thiopental-induced anesthesia. However, zopiclone significantly impaired the motor coordination at the beginning of the recovery. Triazolam significantly impaired the motor coordination and muscle relaxant activity by itself, and these impairments were markedly exacerbated after the recovery from anesthesia.
    [Show full text]
  • Red with Nitrazepam and Placebo in Acute Emergency Driving Situations and in Monotonous Simulated Driving
    109 A 1986 The Carry-over Effects of Triazolam Compa- red with Nitrazepam and Placebo in Acute Emergency Driving Situations and in Mono- tonous Simulated Driving Hans Laurell and Jan Törnroos Reprint from Acta Pharmacologica et toxicologica 1986 v Väg06/7 Efi/( Statens väg- och trafikinstitut (VTI) * 581 01 Linköping [St]tlltet Swedish Road and Traffic Research Institute * S-581 01 Linköping Sweden Acta pharmacol. et toxicol. 1986, 58, 182186. From the National Swedish Road and Traffic Research Institute, (V.T.I.), S-58 101 Linköping, Sweden The Carry-over Effects of Triazolam Compared with Nitrazepam and Placebo in Acute Emergency Driving Situations and in Monotonous Simulated Driving Hans Laurell and Jan Törnros (Received October 9, 1985; Accepted January 9, 1986) Abstract: Eighteen healthy volunteers of both sexes, aged 2034, were tested in the morning while undertaking real car driving avoidance manoeuvres and during monotonous simulated driving after 1 and 3 nights of medication with triazolam 0.25 mg, nitrazepam 5 mg or placebo. The study was a double-blind, randomized, cross-over study, where a minimum of 7 days wash-out separated the 3 treatment periods. Nitrazepam was found to impair performance in the simulated task after 1 but not after 3 nights of medication. Performance in the triazolam condition was not signicantly different from the other conditions on this task on either day. However, after one night of medication triazolam tended to score worse than placebo but better than nitrazepam. In real car driving a tendency was noted for nitrazepam to score worst, whereas the difference between placebo and triazolam was hardly noticeable.
    [Show full text]
  • Oral Sedation Instructions
    Following your child’s appointment (Cont’d) DIET DO NOT feed your child until he/she is completely awake. Begin feeding with clear, pulp-free liquids such as water, apple juice, jello, popsicles or “sports” drinks. Start your child on semi-solid foods (such as soup, noodles, porridge, INSTRUCTIONS FOR PATIENTS WHO WILL BE oatmeal) for easy chewing and digestion. Only feed your child if RECEIVING ORAL SEDATION he/she is hungry and has tolerated clear liquids without vomiting. Avoid feeding your child large portions of food or fatty foods such as French fries. Goals of conscious sedation If your child vomits, stop feeding for 30-60 minutes then gradually resume clear fluids in sips. The goals of sedation in the pediatric patient for diagnostic and therapeutic Normal diet can be resumed as soon as he/she is ready for it. procedures are: 1) to guard the patient’s safety and welfare; 2) to minimize physical discomfort and pain; 3) to control anxiety, minimize psychological PAIN trauma, and maximize the potential for amnesia; 4) to control behavior and/or movement so as to allow the safe completion of the procedure; and 5) You will be notified if local anesthetic has been used during the to return the patient to a state in which safe discharge from medical procedure. It usually takes 2-3 hours to completely wear off. Make supervision, as determined by recognized criteria, is possible. sure you monitor your child closely to avoid any soft tissue trauma. The sedatives If he/she complains of pain, regular strength children’s Tylenol or Advil/Motrin is usually sufficient.
    [Show full text]
  • HYPAM Tablet Contains 0.125 Mg Or 0.25 Mg of Triazolam
    NEW ZEALAND DATA SHEET HYPAM 1. Product Name HYPAM, 0.125 mg, 0.25mg, tablets. 2. Qualitative and Quantitative Composition Each HYPAM tablet contains 0.125 mg or 0.25 mg of triazolam. HYPAM tablets contain lactose. For the full list of excipients, see section 6.1. 3. Pharmaceutical Form HYPAM 0.125mg tablets are oval, flat, bevelled edged white tablets marked TZ on one side and scored on the other. HYPAM 0.25mg tablets are oval, flat, bevelled edged blue tablets marked TZ on one side and scored on the other. Dimensions (both strengths): 7.9mm x 5.6mm. The score line is not intended for breaking the tablet. 4. Clinical Particulars 4.1 Therapeutic indications Triazolam is useful in the management of patients with transient up to 7 days, and short term 2 to 4 weeks, severe or disabling insomnia. It is also useful as a short term, intermittent adjunctive treatment in the management of selected patients with long term insomnia. 4.2 Dose and method of administration Dose The lowest effective dose of triazolam should be used. Treatment with triazolam should not exceed 7-10 consecutive days. Use for more than 2-3 consecutive weeks requires complete re-evaluation of the patient. The starting dose in all patients should be 0.125mg; for many patients this dose immediately before retiring should be sufficient. A dose of 0.25mg should not be exceeded. For elderly or debilitated patients and patients with disturbed liver/kidney function, the dose should not exceed 0.125mg before retiring. The 0.25mg dose should be used only for exceptional patients who do not respond to a trial of the lower dose.
    [Show full text]
  • Chloral Hydrate: Summary Report
    Chloral Hydrate: Summary Report Item Type Report Authors Yuen, Melissa V.; Gianturco, Stephanie L.; Pavlech, Laura L.; Storm, Kathena D.; Yoon, SeJeong; Mattingly, Ashlee N. Publication Date 2020-02 Keywords Compounding; Food, Drug, and Cosmetic Act, Section 503B; Food and Drug Administration; Outsourcing facility; Drug compounding; Legislation, Drug; United States Food and Drug Administration; Chloral Hydrate Rights Attribution-NoDerivatives 4.0 International Download date 26/09/2021 09:06:16 Item License http://creativecommons.org/licenses/by-nd/4.0/ Link to Item http://hdl.handle.net/10713/12087 Summary Report Chloral Hydrate Prepared for: Food and Drug Administration Clinical use of bulk drug substances nominated for inclusion on the 503B Bulks List Grant number: 2U01FD005946 Prepared by: University of Maryland Center of Excellence in Regulatory Science and Innovation (M-CERSI) University of Maryland School of Pharmacy February 2020 This report was supported by the Food and Drug Administration (FDA) of the U.S. Department of Health and Human Services (HHS) as part of a financial assistance award (U01FD005946) totaling $2,342,364, with 100 percent funded by the FDA/HHS. The contents are those of the authors and do not necessarily represent the official views of, nor an endorsement by, the FDA/HHS or the U.S. Government. 1 Table of Contents REVIEW OF NOMINATION ..................................................................................................... 4 METHODOLOGY ...................................................................................................................
    [Show full text]
  • Triazolam | Memorial Sloan Kettering Cancer Center
    PATIENT & CAREGIVER EDUCATION Triazolam This information from Lexicomp® explains what you need to know about this medication, including what it’s used for, how to take it, its side effects, and when to call your healthcare provider. Brand Names: US Halcion Warning This drug is a benzodiazepine. The use of a benzodiazepine drug along with opioid drugs has led to very bad side effects. Side effects that have happened include slowed or trouble breathing and death. Opioid drugs include drugs like codeine, oxycodone, and morphine. Opioid drugs are used to treat pain and some are used to treat cough. Talk with the doctor. If you are taking this drug with an opioid drug, get medical help right away if you feel very sleepy or dizzy; if you have slow, shallow, or trouble breathing; or if you pass out. Caregivers or others need to get medical help right away if the patient does not respond, does not answer or react like normal, or will not wake up. Benzodiazepines can put you at risk for addiction, abuse, and misuse. Misuse or abuse of this drug can lead to overdose or death, especially when used along with certain other drugs, alcohol, or street drugs. Addiction can happen even if you take this drug as your doctor has told you. Get medical help right away if you have changes in mood or behavior, suicidal thoughts or actions, seizures, or trouble breathing. You will be watched closely to make sure you do not misuse, abuse, or become addicted to this drug. Triazolam 1/7 Benzodiazepines may cause dependence.
    [Show full text]
  • Zopiclone Produces Effects on Human Performance Similar to Flurazepam, Lormetazepam and Triazolam
    Br. J. clin. Pharmac. (1986), 21, 647-653 Zopiclone produces effects on human performance similar to flurazepam, lormetazepam and triazolam A. N. GRIFFITHS', D. M. JONES2 & A. RICHENS1 'Department of Pharmacology and Therapeutics, University of Wales College of Medicine, Cardiff and 2Department of Applied Psychology, University of Wales Institute of Science and Technology, Cardiff 1 The cognitive function and psychomotor performance of 10 healthy male volunteers were measured following single oral doses of: zopiclone (7.5 mg), flurazepam (15 mg), lormetazepam (1 mg), triazolam (0.25 mg) and placebo. 2 The performance tests selected (stroop task, five choice serial reaction time, memory span, logical reasoning, mood and saccadic eye movement analysis) were thought to reflect aspects of normal daily activity. 3 The tests demonstrated a clear reduction of performance for all active treatments. No drug emerged as the most potent sedative overall, as each of the tests was affected to a different degree by each drug. 4 Drug effects were not qualitatively different between active treatments so that zopi- clone was indistinguishable from the three benzodiazepines with which it was compared. Keywords zopiclone benzodiazepines human performance saccadic eye movements Introduction Zopiclone is a cyclopyrrolone derivative which, (7.5 mg) has been shown to be effective as an although structurally unrelated to the benzodia- hypnotic (Wickstrom & Giercksky, 1980), zepines, shares their pharmacological profile. and furthermore, Lader & Denney (1983) Binding studies have shown that zopiclone binds reported this dose to be the preferred hypnotic to brain benzodiazepine receptors but is not dose. recognised by peripheral (renal) benzodiazepine The marketed benzodiazepines selected for receptors.
    [Show full text]
  • Drug-Facilitated Sexual Assault in the U.S
    The author(s) shown below used Federal funds provided by the U.S. Department of Justice and prepared the following final report: Document Title: Estimate of the Incidence of Drug-Facilitated Sexual Assault in the U.S. Document No.: 212000 Date Received: November 2005 Award Number: 2000-RB-CX-K003 This report has not been published by the U.S. Department of Justice. To provide better customer service, NCJRS has made this Federally- funded grant final report available electronically in addition to traditional paper copies. Opinions or points of view expressed are those of the author(s) and do not necessarily reflect the official position or policies of the U.S. Department of Justice. AWARD NUMBER 2000-RB-CX-K003 ESTIMATE OF THE INCIDENCE OF DRUG-FACILITATED SEXUAL ASSAULT IN THE U.S. FINAL REPORT Report prepared by: Adam Negrusz, Ph.D. Matthew Juhascik, Ph.D. R.E. Gaensslen, Ph.D. Draft report: March 23, 2005 Final report: June 2, 2005 Forensic Sciences Department of Biopharmaceutical Sciences (M/C 865) College of Pharmacy University of Illinois at Chicago 833 South Wood Street Chicago, IL 60612 ABSTRACT The term drug-facilitated sexual assault (DFSA) has been recently coined to describe victims who were given a drug by an assailant and subsequently sexually assaulted. Previous studies that have attempted to determine the prevalence of drugs in sexual assault complainants have had serious biases. This research was designed to better estimate the rate of DFSA and to examine the social aspects surrounding it. Four clinics were provided with sexual assault kits and asked to enroll sexual assault complainants.
    [Show full text]
  • Acute Toxic Effects of Club Drugs
    Club drugs p. 1 © Journal of Psychoactive Drugs Vol. 36 (1), September 2004, 303-313 Acute Toxic Effects of Club Drugs Robert S. Gable, J.D., Ph.D.* Abstract—This paper summarizes the short-term physiological toxicity and the adverse behavioral effects of four substances (GHB, ketamine, MDMA, Rohypnol®)) that have been used at late-night dance clubs. The two primary data sources were case studies of human fatalities and experimental studies with laboratory animals. A “safety ratio” was calculated for each substance based on its estimated lethal dose and its customary recreational dose. GHB (gamma-hydroxybutyrate) appears to be the most physiologically toxic; Rohypnol® (flunitrazepam) appears to be the least physiologically toxic. The single most risk-producing behavior of club drug users is combining psychoactive substances, usually involving alcohol. Hazardous drug-use sequelae such as accidents, aggressive behavior, and addiction were not factored into the safety ratio estimates. *Professor of Psychology, School of Behavioral and Organizational Sciences, Claremont Graduate University, Claremont, CA. Please address correspondence to Robert Gable, 2738 Fulton Street, Berkeley, CA 94705, or to [email protected]. Club drugs p. 2 In 1999, the National Institute on Drug Abuse launched its Club Drug Initiative in order to respond to dramatic increases in the use of GHB, ketamine, MDMA, and Rohypnol® (flunitrazepam). The initiative involved a media campaign and a 40% increase (to $54 million) for club drug research (Zickler, 2000). In February 2000, the Drug Enforcement Administration, in response to a Congressional mandate (Public Law 106-172), established a special Dangerous Drugs Unit to assess the abuse of and trafficking in designer and club drugs associated with sexual assault (DEA 2000).
    [Show full text]