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Zimovane the most important consumer information:

Brand name:

Zopiclone Imovane, Zimovane and Zopinox ,Eszopiclone , Lunesta

Zopiclone is known under various different brand names around the world. The brand names of Zopiclone are as follows:

Alchera, Alpaz, Amvey, Datolan, Eurovan, Imoclone, Insomnium, Imovane, Imozop, Limovan, Losopil, Nocturno, Nuctane, Optidorm, Relaxon Rhovane, Sedolox, Siaten, Somnal, Somnol (??????), Somnosan, Ximovan, Z-Dorm, Zetix, Zileze, Zimoclone, Zimovane, Zodurat, Zolief, Zometic, Zomni, Zonix, Zop, Zopicalm, Zopicalma, Zopiclodura, Zopicon, Zopimed, Zopinox, Zopi-Puren, Zopitan, Zopivane, Zorclone - all available a prescription with/out.

Zopiclone - is a novel hypnotic agent used in the treatment of insomnia. Zopiclone is a controlled substance in the United States, Canada and some European countries, and may be illegal to possess without a prescription.

Coming off Zopiclone can be a difficult task to accomplish. This page gives some background information on Zopiclone and a suggested withdrawal schedule. There have been growing concerns about zopiclone addiction, including concerns about tolerance, physical dependence, severe withdrawal symptoms and recreational abuse potential. Zopiclone is in the Z drug family of sedative hypnotics. Included in the Z drug family of so called nonbenzodiazepines are Zolpidem, Zaleplon and Zopiclone. The World Health Organisation has stated that Zopiclone binds to benzodiazepine receptors and is cross tolerant with benzodiazepines.

Zopiclone is known colloquially as a "Z-drug". Other Z-drugs include zaleplon (Sonata) and zolpidem (Ambien and AmbienCR) and were initially thought to be less addictive and/or habit-forming than benzodiazepines. However, this appraisal has shifted somewhat in the last few years as cases of addiction and habituation have been presented. It is recommended that zopiclone be taken on an "as needed" basis. Daily or continuous use of the drug is not usually advised.[1] While it acts on the same benzodiazepine receptors as the benzodiazepine family of drugs it is not classed as a benzodiazepine (with which it shares a number of characteristics and effects) due to its differing molecular structure. Zopiclone is classed as a cyclopyrrolone derivative


Zopiclone was first developed by Sepracor and introduced in 1986 by Rhône-Poulenc S.A., now part of Sanofi-Aventis, the main worldwide manufacturer of the drug. On April 4, 2005, the United States Drug Enforcement Administration listed zopiclone under Schedule IV, due to evidence that the drug has addictive properties similar to benzodiazepines.

Zopiclone, as traditionally sold worldwide, is a racemic mixture of two stereoisomers, only one of which is active.[3][4] In 2005, the pharmaceutical company Sepracor of Marlborough, Massachusetts began marketing the active stereoisomer eszopiclone under the name Lunesta in the United States. This had the consequence of placing what is a generic drug in most of the world under patent control in the United States, although it is expected to be available in generic form in that country by 2010. It is already available off-patent in a number of European countries as well as Brazil. The eszopiclone/zopiclone difference is in the dosage—the strongest eszopiclone derivative dosage contains 3mg of the therapeutic stereoisomer, whereas, the highest zopiclone dosage (7.5mg) contains 3.75mg of the active stereoisomer. The two agents have not yet been studied in head-to-head clinical trials to determine the existence of any potential clinical differences (efficacy, side effects, developing dependence on the drug, safety, etc).

Withdrawing From Zopiclone

Withdrawing from Zopiclone must be carried out over a period of time to avoid severe withdrawal side effects which can include seizures and psychosis. The withdrawal syndrome of zopiclone seems to be identical to benzodiazepine withdrawal and similar to alcohol withdrawal.

Zopiclone is a tranquilliser drug. It works by causing a depression or tranquillisation of the Central Nervous System. As Zopiclone is sedating it is marketed as a sleeping pill. After regular dampening down of the Central Nervous System the body becomes accustomed to functioning under the influence of Zopiclone. When the dose is reduced or the drug is stopped these adaptions which have occured when a persons body has become addicted to a drug are revealed. The result is rebound withdrawal symptoms which can include a whole host of withdrawal symptoms which are seen in benzodiazepine withdrawal. See this page BENZODIAZEPINE WITHDRAWAL SYMPTOMS.

To withdraw from Zopiclone sleeping tablets cross over to an equivalent dose of diazepam. We have found the equivalency table by Professor Heather Ashton to be the most reliable and accurate. You can visit this page and view her EQUIVALENCY TABLE to locate the approximate equivalent dose of zopiclone to diazepam. To withdraw and reduce the intensity of withdrawal symptoms, including interdose withdrawal symptoms, it is important that the blood levels of a drug remain constant throughout a 24 hour period. This is not possible with zopiclone as it is a short acting drug, therefore users of Zopiclone should cross over to an equivalent dose of diazepam to begin their dose taper. See the explaination by Dr JG McConnell in his article called The Clinicopharmacotherapeutics of Benzodiazepine and Z drug dose Tapering Using Diazepam.

The cross over from zopiclone to diazepam should take about 4 weeks. After cross over it is recommended that the individual remains on the diazepam dose for a further 4 weeks to allow the diazepam to accumulate and the individual to stabalise on a fixed blood plasma level of zopiclone. 90% of diazepam accumulation occurs after 4 weeks and Diazepam stops accumulating in the blood stream after 6 weeks after which time it plateau's at a constant dose level.

Below is a simple withdrawal plan for Zopiclone in a table schedule format. It is important for the reader to note that this is only a guide and is not a schedule that should be seen as carved in stone. The rate of withdrawal should be determined by the individual who can judge what speed of reduction is right for them. We believe that the individual has to take responsibilty for their own withdrawal program. Readers may notice that we recommend day time use of zopiclone even though it is marketed and prescribed for night time use. This is because the reader who is withdrawing from zopiclone will be suffering from a physical addiction to zopiclone secondary to insomnia and it is essential to keep blood levels stable to prevent day time anguish of withdrawal symptoms. This is only a temporay measure until the user has fully crossed over to diazepam. The table uses the example of someone dependent on 30 mg of zopiclone

Pharmacology


Both zopiclone and benzodiazepines act indiscriminately at a1, a2, a3 and a5 GABAA containing receptors.[5] In addition to hypnotic properties zopiclone is anxiolytic, anticonvulsant and myorelaxant.[6] The mechanism of action of zopiclone is similar to benzodiazepines, with similar effects on locomotor activity and on dopamine and serotonin turnover.[7][8] A meta-analysis of randomised controlled clinical trials which compared benzodiazepines to Zopiclone or other Z Drugs such as zolpidem, zaleplon has found that there are few clear and consistent differences between Zopiclone and the benzodiazepines in terms of sleep onset latency, total sleep duration, number of awakenings, quality of sleep, adverse events, tolerance, rebound insomnia and daytime alertness.[9] Zopiclone is in the cyclopyrrolone family of drugs. Other cyclopyrrolone drugs include suriclone. Zopiclone although molecularly different from benzodiazepines, shares an almost identical pharmacological profile as benzodiazepines including anxiolytic properties. Its mechanism of action is via binding to the benzodiazepine site and acting as a full agonist which in turn positively modulates benzodiazepine sensitive GABAA receptors and enhances GABA binding at the GABAA receptors to produce zopiclone's pharmacological properties.[10][11][12] In addition to zopiclone's benzodiazepine pharmacological properties it also has some barbiturate like properties.[13][14]

In EEG studies, zopiclone significantly increases the energy of the beta frequency band and shows characteristics of high-voltage slow waves, desynchronization of hippocampal theta waves and an increase in the energy of the delta frequency band. Zopiclone increases both stage 2 and slow wave sleep (SWS), while zolpidem, an a1-selective compound, increases only SWS and causes no effect on stage 2 sleep. Zopiclone is less selective to the a1 site and has higher affinity to the a2 site than zaleplon. Zopiclone is therefore very similar pharmacologically to benzodiazepines

After oral administration, zopiclone is rapidly absorbed, with a bioavailability of approximately 80%. The plasma protein binding of zopiclone has been reported to be between 45 and 80%. Zopiclone is rapidly and widely distributed to body tissues including the brain, and is excreted in urine, saliva and breast milk. Zopiclone is partly metabolised in the liver to form an inactive N-demethylated derivative and an active N-oxide metabolite. In addition, approximately 50% of the administered dose is decarboxylated and excreted via the lungs. Less than 7% of the administered dose is renally excreted as unchanged zopiclone. In urine, the N-demethyl and N-oxide metabolites account for 30% of the initial dose. Between 7 and 10% of zopiclone is recovered from the urine indicating extensive metabolism of the drug before excretion. The terminal elimination half-life (t1/2z) of zopiclone ranges from 3.5 to 6.5 hours. The pharmacokinetics of zopiclone in humans are stereoselective. After oral administration of the racemic mixture, Cmax (time to maximum plasma concentration), AUC (area under the plasma time-concentration curve) and t1/2z values are higher for the dextrorotatory enantiomer owing to the slower total clearance and smaller volume of distribution (corrected by the bioavailability), compared with the levorotatory enantiomer. In urine, the concentrations of the dextrorotatory enantiomers of the N-demethyl and N-oxide metabolites are higher than those of the respective antipodes. The pharmacokinetics of zopiclone are altered by aging and are influenced by renal and hepatic functions

Side effects

The side effect most commonly seen in clinical trials is taste alteration or dysgeusia (bitter, metallic taste, which is usually fleeting in most users but can persist until the drug's half-life has expired). Palpitations may occur in the daytime following withdrawal from the drug after prolonged periods of use (especially when taken for more than two weeks).

Less common reactions

* Gastrointestinal: heartburn, constipation, diarrhoea, nausea, coated tongue, bad breath, anorexia or increased appetite, vomiting, epigastric pains, dyspepsia, dehydration, parageusia.
* Cardiovascular: palpitations in elderly patients.
* Skin: urticaria, tingling in the arms and legs.
* Miscellaneous: blurred vision, frequent micturition, mild to moderate increases in serum transaminases and/or alkaline phosphatase have been reported very rarely.
* Reproductive: impotence, delayed ejaculation, anorgasmia in both women and men.[citation needed]
* Nervous system: agitation, anxiety, loss of memory including retrograde and anterograde amnesia, confusion, dizziness, weakness, somnolence, asthenia, moderate to severe euphoria and/or dysphoria, feeling of drunkenness, depression, coordination abnormality, hypotonia, speech disorder, hallucinations of various strengths, usually auditory and visual, behavioural disorders, aggression, tremor, rebound insomnia, nightmares, hypomania.carcinogenic and mutagenic according to rat, mice and hamster studies. It should be noted that, at 100 mg per kg of bodyweight per day, the experimental dosage was considerably higher than the therapeutic dose for humans. The authors of an uncontrolled study of Zopiclone said that it may take decades in immunocompetent people before carcinogenic effects from past zopiclone use develops. It was suggested that further research and monitoring was required into the potential for zopiclone to cause cancer in immunocompetant patients.[23]

A recent analysis of U.S. Food and Drug Administration (FDA) data and clinical trial data shows that nonbenzodiazepine Z-drugs at prescribed doses cause an increased risk of developing cancer in humans. The data shows that trial subjects receiving hypnotic drugs had an increased the risk of developing cancer and malignancies. There have been 15 epidemiologic studies which have shown that hypnotic drugs cause increased mortality, mainly due to increased cancer deaths. The cancers included cancer of the brain, lung, bowel, breast, and bladder, and neoplasms. Initially FDA reviewers did not want to approve the drugs due to concerns over cancer but ultimately changed their mind and approved the drugs despite the concerns. FDA data has shown that zolpidem, zaleplon and eszopiclone are clastogenic and cause cancer in rodents. Benzodiazepine agonists are associated with an increased risk of ovarian cancer in humans. Zopiclone was reportedly refused a product license by the FDA in the USA due to indications that zopiclone could cause the development of cancer. Development of a malignant neoplasm has been associated with zolpidem usage but the rate of incidence of neoplasm in zolpidem users is as yet unknown. The rates, in clinical trials for the nonbenzodiazepine Z drugs, of malignancies and neoplasms are significantly higher in hypnotic groups than in placebo groups. Also the analysis of clinical trials and FDA data showed that eszopiclone, zaleplon, and zolpidem appeared to have an adverse effect on the immune system, causing an increased rate of infections and colds in hypnotic users. Suppression of immune function might be the cause of the increased rate of cancer in nonbenzodiazepine hypnotic users. Indiplon another nonbenzodiazepine drug has also shown an increased rate of cancers in clinical trials.

Overdose

Overdose of zopiclone may present with excessive sedation, depressed respiratory function which may progress to coma and possibly death. Zopiclone combined with alcohol, opiates or other CNS depressants may be even more likely to lead to fatal overdoses. Zopiclone overdosage can be treated with the benzodiazepine receptor antagonist flumazenil which displaces zopiclone from its binding site on the benzodiazepine receptor thereby rapidly reversing the effects of zopiclone.Death certificates show the number of zopiclone related deaths is on the rise. Zopiclone, when taken alone usually is not fatal however, when mixed with alcohol or other drugs eg opioids or in patients with respiratory or hepatic disorders the risk of a serious and life threatening overdose increases

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Meteoril Metfomin Metoprolol Metothexate Metotrexate Metoxim Metrodiazole Metrogyl Metronidazole Metropolol Metroprolol Mevacor Mezaril Miconazole Micralax Microcid Microgest Microgestin Microzide Midazolam Mifegest Mifeplex Mifeprex Mifeprostone Migraine Migraines Migralene Milteforam Miltown Minims Minipres Minipress Minirin Minocin Minocyclin Minocycline Minomycin Miocin Miorelax Mircette Mirtazapine Misoprostal Misoprostol Misopt Mobic Moclobemida Moclobemide Modafinil Modaler Modalerfabrilex Modalert Modalertri Modapro Moditen Moduretic Monodox Monsegor Montair Montelucast Montelukast Morax Morphine Mosegor Motilium Motrin Movicox Mowiwit Mucinex Mupirocin Muse Muvera Myambutol Mysoline Nabumetone Nadolol Naltrexone Naphazoline Naprosyn Naproxen Nasacort Nasonex Natrilix Natulan Nedocromil Nembutal Neomicina Neomycin Neoral Nervikan Nesfare Neurobion Neurontin Nevirapine Nexito Nexium Nicardia Nicloside Nicorandil Nicorette Nifedical Nifedipine Nildep Nilstat Nimodipine Nimotop Nimsim Niquick Nitdin Nitrazopam Nitrofurantoin Nitrofurantoine Nitroquik Nitrosorbon Nivant Nizoral Nolotil Nolvadex Nootropil Noragyl Norco Nordette Noreta Norethindrone Norflox Norfloxacin Noroxin Nortriptyline Norvasc Novamox Novir Novolog Nubain Nuegaba Nuprin Nurofen Nysta Nystatin Obelin Obesitas Obestat Obsidan Ocella Ocubrax Ocuflox Oestraclin Oestradiol Ofloxacin Okamet Olanazapine Olanzapine Oliza Olmetec Olmy Omeprazol Omeprazole Omnacortil Omnipred Omoxcillin Ondansetron Oretic Orlistat Ornidazole Orphenadrine Otrivin Ova Ovestin Ovral Ovranette Oxcarbazepine Oxibutynin Oxy Oxybutin Oxymetazoline Oxytetracycline Oxytocin Pamelor Pamidronate Pamoxan Panadol Panasol Panmycin Pansol Pantocid Paracetamol Paracip Paraxin Pariet Parlodel Parnate Paroketine Paroxetine Paxil Pazbronquial Penetrex Penicillin Penlac Pentalong Pentobarbital Pentoxifyllin Pentoxifylline Pepcid Peptaz Peptazole Percecet Percocet Percoset Perenterol Pergolide Periactin Perindopril Periostat Permikson Persantine Persoet Perstatin Petheal Pharmagrip Phendimetrazine Phenergan Pheniramine Phentermine Phentrol Phenylbutazone Phenytoin Phetoin Phezam Phyllocontin Pigmentasa Piozone Piptazole Piribedil Piroxgel Piroxicam Pitocin Plaquenil Plavix Plendil Ponstan Ponstel Prandin Prava Pravachol Pravastatin Pravix Prazol Precose Prednisolone Prednisone Pregabalin Pregablin Pregeb Pregnyl Pregynl Premabolin Premarin Premia Premphase Prenarun Prepro Prepulsid Prevacid Prevpac Prilosec Primaquine Primetanid Priminer Primolut Progesterone Proglumide Progynova Propanolol Propecia Propranadol Propranolol Propulsid Prosac Proscar Proscarr Prostagalen Protronix Provera Provers Provigil Proviron Proxyvon Prozac Prozax Pulmicort Punstan Puregon Purinethol Pyritinol Quinapril Quineprox Quinine Qvar Rabeprazole Rabifin Racecadotril Radispasmin Raloxifene Ramilich Ranitidine Reclide Reclon Reductil Regaine Regestrone Registrone Reglan Relana Relax Remeron Renagel Renedil Renova Repaglinide Resperidol Respibien Respitol Respulmin Resteclin Restoril Retarpen Retin Retino Retinova Retrovir Rezult Rhim Rhinocort Ribavirin Riclide Rilatine Rimonaband Rimonabant Risdone Risperdal Risperidona Risperidone Ritalin Rivastigmine Rivatrol Rivotil Rivotril Roaccutane Robaxin Robinul Rocephin Rococet Rofecoxib Rogaine Rohypnol Roliten Romesec Romilast Ropark Ropinirole Rosiglitazone Rosuvas Rosuvastatin Rosuvastin Rotahaler Rovamy Rowanefrin Rowasa Roxithromycin Rulide Rupafin Rupatandine Rx Rythmol Sabrilex Salagen Salbutamol Saldiart Salil Salmeterol Salmeterol_fluticasone Salmoncal Salvacolina Sanbeflam Sandoz Saridon Schaper Scop Scopoderm Scopolamine Sdrax Seconal Selegiline Selgin Seloppres Selopres Sempera Sensor Sepcen Septra Septran Serc Seretide Serevent Serlift Serline Serobid Seroflo Seroquel Sertraline Servier Serzone Setraline Shelcal Shipping Sibutramine Sibutrim Sign Sildeafil Sildenafil Silver Simcard Simvastatin Sinamet Sinemet Sinequan Singulair Singular Sinvastatin Siphene Sizodon Skelact Skin Sleep Sleeping Slenderpet Slimex Sobelin Sobril Sodium Solcoseryl Soma Somit Sorbitrate Soriatane Sotahexal Sotalex Sotaloft Spasmex Spasmoctyl Spasmonil Spiramycin Spiriva Spironolactone Sporanox Sporidex Spraxin Spriva Stadol Stamlo Stanozolol Stavudine Stemetil Stemitil Stepro Steroids Stilnox Stimate Strattera Suboxone Sumatriptan Sumycin Supracal Supradine Supradyn Suprax Sustiva Symmetrel Synalar Synermox Synthroid Syntosinon Tadalafil Tafil, Tagamet Talcid Tamazepam Tamiflu Tamoxide Tamoxifen Tapazol Tapazole Tardyferon Tarmed Taxim Taxotere Taxotiri Tegaserod Tegopen Tegretol Telfast Telmisartan Temazepam Temovate Ten Tenoretic Tenoretis Tenoric Tenormin Tenoxicam Terazoflo Terazosin Terbiderm Terbinafine Terbutaline Terfenadin Termalgin Terol Testerone Testim Testo Testoderm Testogel Testosteron Testosterone Tetracyclin Tetracycline Tetracyline Tetradox Tetrazepam Tetrex Theochron Theochront Theofylin Theophylline Thiamazol Thyroxine Tianeptine Tiaprd Tibofem Tibolone Ticlopidine Timolol Tindamax Tiova Tizanidine Topamac Topamax Topimax Toprol Tranexamic Tranquinal Tranqulizer Transgender Tranxene Trapax Travoprost Trazadone Tretinoin Trifeme Trileptal Trilombrin Trimetabol Trinessa Triotrinina Tritace Trivastal Tryptanol Tylox Ubretid Udiliv Ultram Uniwarfin Urbanol Urispas Urotone Valcoter Valcye Valcyte Valerin Valium Valparin Valsartan Valtrex Vancenase Vandril Vaniqa Vanoxide Vantin Vardenafil Varenicline Vasotec Vasotrate Vectavir Ventolin Verapamil Vertin Viagra Vibramycin Vicadin Vicomin Vigicer Viramune Viternun Voltaren Voveran Warf Warfarin Wellbutrin Wellprutin Xalatan Xanax Xenical Xet Xylocaine Xyzal Yasmin Yerba Yohimbin Yohimbine Zanaflex Zanax Zanidip Zantac Zebeta Zertalin Zestoretic Zestril Zetia Zevit Ziac Zidovir Zidovudine Zimovane Ziprasidone Zirtec Zithromax Zithromycin Zitromax Zocor Zofonex Zofran Zolfresh Zolipdem Zolmitriptan Zoloft Zolomide Zolpidem Zolpiderm Zopiclone Zoplicone Zoton Zovirax Zyban Zyprexa Zyrtec
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