Abilify (Phi)(ability)

Double play on words (Phi, Ability), comp. lexapro

 Aripiprazole

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Aripiprazole

Systematic (IUPAC) name
7-{4-[4-(2,3-dichlorophenyl)piperazin-1-yl]butoxy}-3,4-dihydroquinolin-2(1H)-one
Identifiers
CAS number	129722-12-9
ATC code	N05AX12
PubChem	CID 60795
IUPHAR ligand ID	34
DrugBank	APRD00638
ChemSpider	54790
UNII	82VFR53I78
Chemical data
Formula	C23H27Cl2N3O2
Mol. mass	448.385
SMILES	eMolecules & PubChem
Pharmacokinetic data
Bioavailability	87%
Protein binding	>99%
Metabolism	liver
Half-life	75h (active metabolite : 94h)
Excretion	feces and urine
Therapeutic considerations
Licence data	EU EMA:Link, US FDA:link
Pregnancy cat.	C (USA)
Legal status	℞ Prescription only
Routes	oral (via tablets, orodispersable tablets, and oral solution); intramuscular
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Aripiprazole (pronounced /ˌɛərɨˈpɪprəzoʊl/ AIR-i-PIP-rə-zohl; brand names: Abilify, Abilify Discmelt, Aripiprex) is an atypical antipsychotic and antidepressant used in the treatment of schizophrenia, bipolar disorder, and clinical depression. It was approved by the US Food and Drug Administration (FDA) for schizophrenia on November 15, 2002, for acute manic and mixed episodes associated with bipolar disorder on October 1, 2004, as an adjunct for major depressive disorder on November 20, 2007 and to treat irritability in children with autistic disorder in children on 20 November 2009.^[1][2] Aripiprazole was developed by Otsuka in Japan, and in the United States, Otsuka America markets it jointly with Bristol-Myers Squibb.

Contents [show] 1 Indications and usage 1.1 Schizophrenia 1.2 Bipolar disorder 1.3 Major depression (Unipolar depression) 1.4 Autism 1.5 Cocaine dependency 2 Pharmacology 3 Pharmacokinetics 4 Patent status 5 Side effects 6 Overdosage 7 Drug interactions 8 Dosage forms 9 Synthesis 10 References 11 External links

[edit] Indications and usage

[edit] Schizophrenia

Aripiprazole has been approved by the FDA for the treatment of schizophrenia.^[3]

[edit] Bipolar disorder

Aripiprazole has been approved by the FDA for the treatment of acute manic and mixed episodes, in both pediatric patients aged 10–17 and in adults.^[4] Several double-blind, placebo-controlled trials support this use.^[5][6][7][8] In addition, it is often used as maintenance therapy, either on its own or in conjunction with a mood stabilizer such as lithium or valproate. This use is also supported by a handful of studies.^[9][10]haloperidol at reducing manic symptoms,^{[11][unreliable source?]} and is much better tolerated by patients.^[12] Aripiprazole is at least as effective as
Aripiprazole’s use as a monotherapy in bipolar depression is more controversial. While a few pilot studies have found some effectiveness^[13][14] (with one finding a reduction in anhedonia symptoms^[15]), two large, double-blind, placebo-controlled studies found no difference between aripiprazole and placebo.^[16] One study reported depression as a side effect of the drug.^[17]

[edit] Major depression (Unipolar depression)

In 2007, aripiprazole was approved by the FDA for the treatment of unipolar depression when used adjunctively with an antidepressant medication.^[18] It has not been FDA-approved for use as monotherapy in unipolar depression.

[edit] Autism

In 2009, the United States FDA approved Abilify to treat irritability in persons with autism.^[19] It was approved on the basis of two studies that showed it reduced aggression towards others, self-injury, quickly changing moods, irritability, and temper tantrums in autistic males and females 6–17 years of age.

[edit] Cocaine dependency

Perhaps owing to its mechanism of action relating to dopamine receptors, there is some evidence to suggest that aripiprazole blocks cocaine-seeking behaviour in animal models without significantly affecting other rewarding behaviours (such as food self-administration). ^[20]

[edit] Pharmacology

D2 Partial Agonist (Ki = 0.34 nM) D3 Antagonist (?)

5-HT1A Partial Agonist (Ki = 0.34 nM) 5-HT2A Antagonist (Ki = 0.8 nM) 5-HT2C Partial Agonist (Ki = 15 nM) 5-HT7 Antagonist (Ki = 39 nM)

SRI (?) Antihistamine (Ki = 61 nM) α-adrenergic antagonist (Ki = 57 nM) mACh receptor antagonist (?)

Aripiprazole’s mechanism of action is different from those of the other FDA-approved atypical antipsychoticsclozapine, olanzapine, quetiapine, ziprasidone, and risperidone). Rather than antagonizing the D₂ receptor, aripiprazole acts as a D₂partial agonist (K_i = 0.34 nM).^[21][22] Aripiprazole is also a partial agonist at the 5-HT_1A receptor (K_i = 1.65 nM), and like the other atypical antipsychotics displays an antagonist profile at the 5-HT_2A receptor (K_i = 0.8 nM).^[23][24] It also antagonizes the 5-HT₇ receptor (K_i = 39 nM) and acts as a partial agonist at the 5-HT_2C receptor (K_i = 15 nM), both with high affinity. The latter action may underlie the minimal weight gain seen in the course of therapy.^[25] Aripiprazole has moderate affinity for histamine (K_i = 61 nM) and α-adrenergic (K_i = 57 nM) receptors and for the serotonin transporter, and no appreciable affinity for cholinergic muscarinic receptors.^[26] (e.g.,
D₂ and D₃ receptor occupancy levels are high, with average levels ranging between ~71% at 2 mg/day to ~96% at 40 mg/day.^[27][28] Most atypical antipsychotics bind preferentially to extrastriatal receptors, but aripiprazole appears to be less preferential in this regard, as binding rates are high throughout the brain.^[29]
Recently, it has been demonstrated that in 5-HT₇ receptor knockout mice, aripiprazole does not reduce immobility time in the forced swim test (FST), and actually increases it.^[30][31] This implicates 5-HT₇amisulpride.^[30][31][32] antagonism as playing a major role in aripiprazole’s antidepressant effects, similarly to
Aripiprazole produces 2,3-dichlorophenylpiperazine (DCPP) as a metabolite similarly to how trazodone and nefazodone reduce to 3-chlorophenylpiperazine (mCPP) and niaprazine converts to 4-fluorophenylpiperazine^[33] It is unknown whether DCPP contributes to aripiprazole’s pharmacology in any way, but the possibility cannot be excluded. (pFPP).

[edit] Pharmacokinetics

Aripiprazole displays linear kinetics and has an elimination half-life of approximately 75 hours. Steady-state plasma concentrations are achieved in about 14 days. C_max (maximum plasma concentration) is achieved 3–5 hou

rs after oral dosing. Bioavailability of the oral tablets is about 90% and the drug undergoes extensive hepatic metabolization (dehydrogenation, hydroxylation, and N-dealkylation), principally by the enzymes CYP2D6 and CYP3A4. Its only known active metabolite is dehydro-aripiprazole, which typically accumulates to approximately 40% of the aripiprazole concentration. The parenteral drug is excreted only in traces, and its metabolites, active or not, are excreted via feces and urine.^[26] When dosed daily, brain concentrations of aripiprazole will increase for a period of 10–14 days, before reaching stable constant levels. This phenomenon is due to the long half life of aripiprazole, and is responsible for many of the adverse side effects that appear after multiple days of dosing (whereas the first dose normally does not cause these side effects).

[edit] Patent status

Otsuka’s US patent on aripiprazole expires on October 20, 2014;^[34] however, due to a pediatric extension, a generic will not become available until at least April 20, 2015.^[4]Barr Laboratories (now Teva Pharmaceuticals) initiated a patent challenge under the Hatch-Waxman Act in March 2007.^[35] As of 14 August 2009, this challenge is still in court. (2009 -08-14)^[update]

[edit] Side effects

This section needs additional citations for verification. Please help improve this article by adding reliable references. Unsourced material may be challenged and removed. (April 2010)

This section may require cleanup to meet Wikipedia’s quality standards. Please improve this section if you can. The talk page may contain suggestions. (April 2010)

Akathisia^[36], headache, unusual tiredness or weakness, nausea, vomiting, an uncomfortable feeling in the stomach, constipation, light-headedness, insomnia, sleepiness, shaking, and blurred vision.
Uncontrollable twitching or jerking movements, tremors, seizure, and weight gain. Some people may feel dizzy, especially when getting up from a lying or sitting position, or may experience a fast heart rate.
Neuroleptic malignant syndrome (Combination of fever, muscle stiffness, faster breathing, sweating, reduced consciousness, and sudden change in blood pressure and heart rate.)
Aripiprazole also causes sexual dysfunction.
Tardive dyskinesia (As with all antipsychotic medication, patients using aripiprazole may develop the permanent neurological disorder tardive dyskinesia.^[37][38][39])
Stroke (While taking aripiprazole some elderly patients with dementia have suffered from stroke or ‘mini’ stroke.)
Other elderly patients may experience high blood sugar or the onset or worsening of diabetes.
Allergic reaction (such as swelling in the mouth or throat, itching, rash), increased production of saliva, speech disorder, nervousness, agitation, fainting, reports of abnormal liver test values, inflammation of the pancreas, muscle pain, weakness, stiffness, or cramps.

[edit] Overdosage

Children or adults who ingested acute overdoses have usually manifested central nervous system depression ranging from mild sedation to coma; serum concentrations of aripiprazole and dehydroaripiprazole in these patients were elevated by up to 3-4 fold over normal therapeutic levels, yet no deaths have yet been recorded.^[40]

[edit] Drug interactions

Aripiprazole is a substrate of CYP2D6 and CYP3A4. Coadministration with medications that inhibit (e.g. paroxetine, fluoxetine) or induce (e.g. carbamazepine) these metabolic enzymes are known to increase and decrease, respectively, plasma levels of aripiprazole.^[41] As such, anyone taking Abilify should be aware that their dosage of Abilify may need to be decreased.
Aripiprazole may change the subjective effects of alcohol. One study^[42] found that aripiprazole increased the sedative effect and reduced the sense of euphoria normally associated with alcohol consumption. However, another alcohol study^[43] found that there was no difference in subjective effect between a placebo group and a group taking aripiprazole.

[edit] Dosage forms

• Intramuscular injection, solution: 7.5 mg/mL (1.3 mL)
• Solution, oral: 1 mg/mL (150 mL) [contains propylene glycol, sucrose 400 mg/mL, and fructose 200 mg/mL; orange cream flavor]
• Tablet: 2 mg, 5 mg, 10 mg, 15 mg, 20 mg, 30 mg
• Tablet, orally disintegrating: 10 mg [contains phenylalanine 1.12 mg; creme de vanilla flavor]; 15 mg [contains phenylalanine 1.68 mg; creme de vanilla flavor]

[edit] Synthesis

U.S. Patent 5,006,528

)

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Pseudoephedrine

Pseudoephedrine

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Pseudoephedrine

Systematic (IUPAC) name
(R*,R*)-2-methylamino-1-phenylpropan-1-ol
Identifiers
CAS number	90-82-4
ATC code	R01BA02
PubChem	CID 7028
DrugBank	DB00852
ChemSpider	6761
Chemical data
Formula	C10H15NO
Mol. mass	165.23
Pharmacokinetic data
Bioavailability	~100%[1]
Metabolism	hepatic (10–30%)
Half-life	4.3-8 hours[1]
Excretion	43-96% renal[1]
Therapeutic considerations
Pregnancy cat.	B2(AU) C(US)
Legal status	Pharmacist Only (S3) (AU) P (UK)
Routes	oral
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Pseudoephedrine (PSE) [pronunciation: /ˌsuːdəʊɪˈfɛdɹɪn/ or /ˌsuːdoˈɛfədriːn/] is a sympathomimetic drug of the phenethylamine and amphetamine chemical classes. It is used as a nasal/sinus decongestant and stimulant, or as a wakefulness-promoting agent.

The salts pseudoephedrine hydrochloride and pseudoephedrine sulfate are found in many over-the-counter preparations either as a single ingredient or, more commonly, in combination with antihistamines, guaifenesin, dextromethorphan, paracetamol (acetaminophen), and/or NSAIDs (e.g., aspirin, ibuprofen, etc.).

Contents [show] 1 Chemistry 2 Nomenclature 3 Synthesis 4 Mechanism of action 5 Medical uses 5.1 Indications 5.2 Adverse effects 5.3 Precautions and contraindications 5.4 Common brand names 6 Alternative and illicit use 6.1 Sports 6.2 Detection of use 7 National legislation 7.1 Australia 7.2 Mexico 7.3 New Zealand 7.4 United Kingdom 7.5 United States 8 See also 9 References

[edit] Chemistry

Two pairs of enantiomers: Ephedrine (top) and Pseudoephedrine (bottom)

Pseudoephedrine is a diastereomer of ephedrine. Pseudoephedrine is a chiral molecule, meaning it occurs in both “left-handed” and “right-handed” configurations which are not superimposable.

Pseudoephedrine is a precursor of methamphetamine and methcathinone.

[edit] Nomenclature

The dextrorotary (+)- or d- enantiomer is (1S,2S)-Pseudoephedrine, whereas the levorotating (−)- or l- form is (1R,2R)-Pseudoephedrine.

In the outdated d/l system (+)-Pseudoephedrine is also referred to as l-Pseudoephedrine and (—)-Pseudoephedrine as d-Pseudoephedrine (in the Fisher projection then the phenylring is drawn at bottom). ^{[2] [3]}

Often the d/l system (with small caps) and the d/l system (with lower-case) are confused. The result is that the dextrorotary d-Pseudoephedrine is wrongly named d-Pseudoephedrine and the levorotary l-Ephedrine (the diastereomer) wrongly l-Ephedrine.

The IUPAC names of the two enantiomers are (1S,2S)- respectively (1R,2R)-2-methylamino-1-phenylpropan-1-ol. Synonyms for both are psi-Ephedrine and threo-Ephedrine.

Pseudoephedrine is the International Nonproprietary Name (INN) of the (+)-form, when used as pharmaceutical substance. ^[4]

[edit] Synthesis

Although pseudoephedrine occurs naturally as an alkaloid in certain plant species (for example, as a constituent of extracts from the ephedra species, also known as Ma Huang, in which it occurs together with other isomers of ephedrine), the majority of pseudoephedrine produced for commercial use is derived from yeast fermentation of dextrose in the presence of benzaldehyde. In this process, specialized strains of yeast (typically a variety of Candida utilis or Saccharomyces cerevisiae) are added to large vats containing water, dextrose and the enzyme pyruvate decarboxylase (such as found in beets and other plants). After the yeast has begun fermenting the dextrose, the benzaldehyde is added to the vats, and in this environment the yeast convert the ingredients to the precursor l-phenylacetylcarbinol (L-PAC). L-PAC is then chemically converted to pseudoephedrine via reductive amination.^[5]

The bulk of pseudoephedrine is produced by commercial pharmaceutical manufacturers in India and China, where economic and industrial conditions favor the mass production of pseudoephedrine for export.^[6]

[edit] Mechanism of action

Pseudoephedrine is a sympathomimetic amine. Its principal mechanism of action relies on its indirect action on the adrenergic receptor system. The vasoconstriction that pseudoephedrine produces is believed to be principally an α-adrenergic receptor response. ^[7]

While it may have weak or no direct agonist activity at α- and β-adrenergic receptors, the principal mechanism is to cause the release of endogenous norepinephrine (noradrenaline) from storage vesicles in presynaptic neurons. The displaced noradrenaline is released into the neuronal synapse where it is free to activate the postsynaptic adrenergic receptors. These adrenergic receptors are located on the muscles lining the walls of blood vessels. When activated by pseudoephedrine, the muscles contract, causing the blood vessels to constrict (vasoconstriction). The constricted blood vessels now allow less fluid to leave the blood vessels and enter the nose, throat and sinus linings, which results in decreased inflammation of nasal membranes as well as decreased mucus production. Thus, by constriction of blood vessels, mainly those located in the nasal passages, pseudoephedrine causes a decrease in the symptoms of nasal congestion.

October 15, 2010 Posted by archmichaelangelo | 1:1, Science and medicine, The war, Uncategorized | disinformation, info, Legislated in conspiracy, Pseudoephedrine, Regulated in conspiarcy, Sympathomimetic drug, Uncategorized | Leave a comment

Chemical restraint

Chemical restraint

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A chemical restraint is a form of medical restraint in which a drug is used to restrict the freedom or movement of a patient or in some cases to sedate a patient. These are used in emergency, acute, and psychiatric settings to control unruly patients who are interfering with their care or who are otherwise harmful to themselves or others in their vicinity.

Drugs that are often used as chemical restraints include benzodiazepines (such as Lorazepam (Ativan), Midazolam (Versed), or Diazepam (Valium)^[1]. Haloperidol (Haldol) is a drug chemically unrelated to benzodiazepines and is also popular for chemical restraint, without the potentially dangerous side effects of benzodiazepine drugs.

In the United States, no drugs are presently approved by the U.S. Food and Drug Administration (FDA) for use as chemical restraints^[2].

The use of chemical restraint has been criticized. It has been found to be mismanaged by health care workers for the convenience of the staff rather than the benefit of the patient, as workers use them to prevent patients from resisting care rather than improving the health of the patient^[3]. This has been found to cause more confusion in patients, thereby slowing their recovery^[4].

October 15, 2010 Posted by archmichaelangelo | C, Science and medicine, The war | Chemical restraints, disinformation, False imprisonment, info, medicine, psychotropic | Leave a comment

Risperdal (psedoscience and the psychiatric equivalent to AIDS/HIV/H4)

Risperidone

From Wikipedia, the free encyclopediaControversy, lawsuits and settlementsOn 11 April 2012, Johnson & Johnson and its subsidiary, Janssen Pharmaceuticals Inc., were fined about $1.2 billion by an Arkansas judge.^[28] The jury found that the companies had downplayed multiple risks associated with Risperidone (Risperdal). The Judge held that nearly 240,000 violations of the state’s Medicaid fraud law had been committed. Each violation carried a fine of $5,000. The companies were also fined $11 million for more than 4,500 violations of the state’s ‘deceptive practices laws’.

[edit] Brand names

It is sold under the trade name Risperdal in the Netherlands, United States, Canada, Australia, United Kingdom, Portugal, Spain, Israel, Turkey, New Zealand, Saudi Arabia, Venezuela, Ireland^[1] and several other countries, Risperdal or Ridal in New Zealand and Venezuela, Sizodon or Riscalin or Risdone in India, Rispolept in Eastern Europe and Russia,Zepidone in Nigeria, Riperidone in South Korea, Risperidona in Spain and Belivon, or Rispen elsewhere.

[edit] References

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Risperidone

Systematic (IUPAC) name
4-[2-[4-(6-fluorobenzo[d]isoxazol-3-yl)- 1-piperidyl]ethyl]-3-methyl- 2,6-diazabicyclo[4.4.0]deca-1,3-dien-5-one
Identifiers
CAS number	106266-06-2
ATC code	N05AX08
PubChem	CID 5073
IUPHAR ligand ID	96
DrugBank	DB00734
ChemSpider	4895
Chemical data
Formula	C23H27FN4O2
Mol. mass	410.485 g/mol
SMILES	eMolecules & PubChem
Pharmacokinetic data
Bioavailability	70% (oral)
Metabolism	Hepatic (CYP2D6-mediated)
Half-life	3–20 hours
Excretion	Urinary
Therapeutic considerations
Pregnancy cat.	C
Legal status	℞ Prescription only
Routes	Oral and extended-release intramuscular injection
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Risperidone (pronounced Ris-PEAR-rǐ-dōne) is an atypical antipsychotic used to treat schizophreniaschizoaffective disorder, the mixed and manic states associated with bipolar disorder, and irritability in children with autism. The drug was developed by Janssen-Cilag and first released in 1994^[1]. It is sold under the trade name Risperdal in the Netherlands, United States, Canada, Australia, United Kingdom, Portugal, Spain, Turkey, New Zealand and several other countries, Risperdal or Ridal in New Zealand, Sizodon or Riscalin in India, Rispolept in Eastern Europe, and Russia, and Belivon, or Rispen elsewhere. (including adolescent schizophrenia),

Contents [show] 1 Indications and Uses 2 Availability 3 Side effects 4 Pharmacology 5 References 6 External links

[edit] Indications and Uses

• treatment of schizophrenia in adults
• treatment of schizophrenia in adolescents aged 13-17 years
• alone or in combination with lithium or valproate, for the short-term treatment of acute manic or mixed episodes associated with Bipolar I Disorder in adults
• alone in the short-term treatment of acute manic or mixed episodes associated with Bipolar I Disorder in children and adolescents aged 10-17 years
• treatment of irritability associated with autistic disorder in children and young adults
• it has also been used as a control drug for people with tourette syndrome and other tic disorders.
• treatment of major depression with psychotic features
• cure persistent or intractable hiccups^[2]

Risperidone was approved by the United States Food and Drug Administration (FDA) in 1993 for the treatment of schizophrenia.^[3]

On August 22, 2007, risperidone was approved as the only drug agent available for treatment of schizophrenia in youth ages 13–17; it was also approved that same day for treatment of bipolar disorder in youth and children ages 10–17, joining lithium. Risperidone contains the functional groups of benzisoxazolepiperidine as part of its molecular structure. In 2003 the FDA approved risperidone for the short-term treatment of the mixed and manic states associated with bipolar disorder. In 2006 the FDA approved risperidone for the treatment of irritability in children and adolescents with autism.^[4] The FDA’s decision was based in part on a study of autistic children with severe and enduring problems of violent meltdowns, aggression, and self-injury; risperidone is not recommended for autistic children with mild aggression and explosive behavior without an enduring pattern.^[5] Like other atypical antipsychotics, risperidone has also been used off-label for the treatment of anxiety disorders, such as obsessive-compulsive disorder; severe, treatment-resistant depression with or without psychotic features; tourette syndrome; disruptive behavior disorders in children; and eating disorders, among others. In two small studies risperidone was reported to successfully treat the symptoms of phencyclidine (PCP) psychosis due to acute intoxication^[6] and chronic use.^[7] and

A 2009 Cochrane Library review found no evidence from randomized controlled trials that risperidone is effective for the treatment of attention-deficit hyperactivity disorder (ADHD) in people with intellectual disabilities.^[8] A multi-year UK study by the Alzheimer’s Research Trust suggested that this and other neuroleptic anti-psychotic drugs commonly given to Alzheimer’s patients with mild behavioural problems often made their condition worse. The study concluded that:

“

For most patients with AD, withdrawal of neuroleptics had no overall detrimental effect on functional and cognitive status and by some measures improved functional and cognitive status. Neuroleptics may have some value in the maintenance treatment of more severe neuropsychiatric symptoms, but this possibility must be weighed against the unwanted effects of therapy.[9]

”

[edit] Availability

Risperdal 4 mg tablets (UK)

Janssen’s patent on Risperdal expired on December 29, 2003, opening the market for cheaper generic versions of the drug from other companies, and Janssen’s exclusive marketing rights expired on June 29, 2004 (the result of a pediatric extension.)

Risperidone is available as a tablet in 0.25, 0.5, 1, 2, 3 and 4 mg sizes, as an oral solution (30ml, 1 mg/ml), and as a 12.5 mg, 25 mg, 37.5 mg and 50 mg ampoule Risperdal Consta, which is a depot injectionRisperdal M-Tabs and elsewhere as Risperdal Quicklets. administered once every two weeks. It is also available as a wafer known in the United States and Canada as

Risperidone became available as a generic drug in October 2008 from Teva Pharmaceuticals, Dr. Reddy’s Laboratories, Inc. and Patriot Pharmaceutics. The Patriot generic is Janssen Pharmaceutical’s “authorized generic pharmaceutical.”

[edit] Side effects

Risperidone has been associated with weight gain.^[10] Other common side effects include akathisia, sedation, dysphoria, insomnia, sexual dysfunction, low blood pressure, high blood pressure, muscle stiffness, muscletremors, increased salivation, constipation, and stuffy nose. pain,

Many antipsychotics are known to cause hyperprolactinemia which may lead to hypogonadism-induced osteoporosis, galactorrhoea, gynaecomastia, irregular menstruation and sexual dysfunction. However, risperidone is known to increase prolactin to a greater extent than other atypical antipsychotics. Although lactation is possible in both sexes using other antipsychotic drugs, risperidone is the biggest offender.^[11][12][13] It is thought that once risperidone raises prolactin, it may cause prolactinoma, a benign tumor of the pituitary gland. Tumors, in general, are not considered reversible. Medical therapy may help reduce tumor size and restore normal reproduction and pituitary function, however, dopamine agonists^[14] There is a higher association between pituitary neoplasms with use of risperidone and amisulpride than with other antipsychotic agents. are not likely to be prescribed to antipsychotic users, thus, surgery or radiation treatment may be required. This condition may recur if the patient is switched to a different antipsychotic. Risperidone has been known to cause increased thoughts of suicide.

Risperidone can potentially cause tardive dyskinesia (TD),^[15] extrapyramidal symptoms (EPS),^[15] and neuroleptic malignant syndrome (NMS).^[15] Risperidone may also trigger diabetes and more serious conditions of glucose metabolism, including ketoacidosis and hyperosmolar coma, according to an FDA Warning Letter issued to Janssen Pharmaceutica, Inc. on 19-Apr-04.^[16]

[edit] Pharmacology

This drug belongs to a class of antipsychotic drugs known as atypical antipsychotics that have more pronounced serotonin antagonism than dopamine antagonism, but risperidone is unique in this class because it retains dopamine antagonism. It has high affinity for D₂ dopaminergic receptors. It has actions at several 5-HT (serotonin) receptor subtypes. These are 5-HT_2C, linked to weight gain, 5-HT_2A,linked to its antipsychotic action and relief of some of the extrapyramidal side effects (EPS) experienced with the typical neuroleptics.

It reaches peak plasma levels quickly regardless of whether it is administered as a liquid or pill. Risperidone is metabolised fairly quickly, so the potential for nausea subsides usually in two to three hours. However, the active metabolite, 9-hydroxy-risperidone, which has similar pharmacodynamics to risperidone, remains in the body for much longer, and has been developed as an antipsychotic in its own right, called paliperidone.

An intramuscular preparation, marketed as Risperdal Consta, can be given once every two weeks. It is slowly released from the injection site. This method of administration may be used on sanctioned patients who are declining, or consenting patients who may have disorganized thinking and cannot remember to take their daily doses.^[17] Doses range from 12.5 to 50 mg given as an intramuscular injection once every two weeks.

October 15, 2010 Posted by archmichaelangelo | 1994, Liability, Psychiatric fraud, Science and medicine | Beheaded for the witness, Chemical internment, Deaths, Defendence production act, disinformation, info, liabilities, medicine, Murder, Pharmaceutical Industry, Pseudoscience, psychotropic, Risperdal, Symbolic misrepresentation | Leave a comment

Misinformation / Disinformation

Misinformation

Misinformation is false or inaccurate information that is spread unintentionally. It is distinguished from disinformation by motive in that misinformation is simply erroneous, while disinformation, in contrast, is intended to mislead.^[1]

Makkai proposes the distinction between misinformation and disinformation to be a defining characteristic of idioms in the English language.^[2] An utterance is only idiomatic if it involves disinformation, where the listener can decode the utterance in a logical, and lexically correct, yet erroneous way. Where the listener simply decodes the lexemes incorrectly, the utterance is simply misinformation, and not idiomatic.

Damian Thompson defines counterknowledge as “misinformation packaged to look like fact“.^[3] Using the definition above, this may refer to disinformation, as the motive is deliberate and often pecuniary.

Contents [show] 1 Examples 2 See also 3 References 4 Further reading

[edit] Examples

According to Thompson, all three of the following statements are misinformations, or counterknowledge, packaged to look like fact:

• There is a link between childhood autism and the MMR vaccine.^{[citation needed]}
• The structure of a cell is too complex to have evolved through natural selection.”^[4]

October 15, 2010 Posted by archmichaelangelo | Schemes, Uncategorized | disinformation, Expert misinformation, Misinformation, Schemes, Uncategorized | Leave a comment

Lexapro (symbolc misrepresentation)[Lexis-vocabulary, pro-(for, skilled]

Lexapro [Lexis(vocabulary) + Pro]

Escitalopram

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Escitalopram

Systematic (IUPAC) name
(S)-1-[3-(dimethylamino)propyl]-1-(4-fluorophenyl)-1,3-dihydroisobenzofuran-5-carbonitrile
Identifiers
CAS number	128196-01-0
ATC code	N06AB10
PubChem	CID 146570
DrugBank	APRD00683
ChemSpider	129277
UNII	4O4S742ANY
Chemical data
Formula	C20H21FN2O
Mol. mass	324.392 g/mol (414.43 as oxalate)
SMILES	eMolecules & PubChem
Pharmacokinetic data
Bioavailability	80%
Protein binding	~56%
Metabolism	Liver, specifically the enzymes CYP3A4 and CYP2C19
Half-life	27–32 hours
Therapeutic considerations
Pregnancy cat.	C
Legal status	Rx Only (U.S) POM (U.K)
Routes	Oral
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Lexapro tablets

Cipralex brand escitalopram package and tablet sheet

Escitalopram (trade names Lexapro, Cipralex, Seroplex, Lexamil) is an antidepressant of the selective serotonin reuptake inhibitor (SSRI) class. It is approved by the U.S. Food and Drug Administration (FDA) for the treatment in adults with major depressive disorder, generalized anxiety disorder, social anxiety disorder , or panic disorder. Escitalopram is the S-stereoisomer (enantiomer) of the earlier Lundbeck drug citalopram, hence the name escitalopram. Escitalopram is noted for its high selectivity of serotonin reuptake inhibition and has side effects typical for the SSRI class.

Contents [show] 1 History 2 Use in depression 3 Pharmacology 4 Side effects and drug interactions 5 Discontinuation symptoms 6 Controversy 7 References 8 Cited texts 9 See also 10 External links

[edit] History

Escitalopram was developed in a close cooperation between Lundbeck and Forest Laboratories. Its development was initiated in the summer of 1997, and the resulting new drug application was submitted to the U.S. FDA in March 2001. The short time (3.5 years) it took to develop escitalopram can be attributed to the previous extensive experience of Lundbeck and Forest with citalopram, which has similar pharmacology.^[1]evergreening“^[2] (also called “lifecycle management”^[3])– the long-term strategy pharmaceutical companies use in order to extend the lifetime of a drug, in this case of the citalopram franchise. Escitalopram is an enantiopure compound of the racemic mixture citalopram, used for the same indication, and for that reason it required less investment and less time to develop. Two years after escitalopram’s launch, when the patent on citalopram expired, the escitalopram sales successfully made up for the loss. On May 23, 2006, the FDA approved a generic version of escitalopram by Teva.^[4] On July 14 of that year, however, the U.S. District Court of Delaware decided in favor of Lundbeck regarding the patent infringement dispute and ruled the patent on escitalopram valid.^[5] The FDA issued the approval of escitalopram for major depression in August 2002 and for generalized anxiety disorder in December 2003. Escitalopram can be considered an example of “

In 2006 Forest Laboratories was granted an 828 day (2 years and 3 months) extension on its US patent for escitalopram.^[6] This pushed the patent expiry from December 7, 2009 to March 14, 2012.

October 15, 2010 Posted by archmichaelangelo | Defense Production Act, L, Psychiatric fraud | Beheaded for the witness, Chemical internment, Deaths, Defendence production act, disinformation, economics, Fraud, L, Lexapro, medicine, Murder, Pharmaceutical Industry, psychotropic, Symbolic misrepresentation | Leave a comment

Geodon [geo (earth) + don(dominic)]

LORD Don, from Latin dominus, is an honorific in Spanish ([don]), Portuguese (Dom, [dõ]), and Italian ([dɔn]). The female equivalent is Doña (Spanish: [ˈdoɲa]), Dona (Portuguese: [ˈdonɐ]), and Donna (Italian: [ˈdɔnna]), abbreviated “Dª” or simply “D.“

Dominus is the Latin word for master or owner.

Ziprasidone

Ziprasidone

Systematic (IUPAC) name
5-[2-[4-(1,2-benzisothiazol-3-yl)-1-piperazinyl]ethyl]- 6-chloro-1,3-dihydro-2H-indol-2-one
Identifiers
CAS number	146939-27-7
ATC code	N05AE04
PubChem	CID 60854
IUPHAR ligand ID	59
DrugBank	DB00246
ChemSpider	54841
Chemical data
Formula	C21H21ClN4OS
Mol. mass	412.936
Pharmacokinetic data
Bioavailability	100% (intramuscular) 60% (orally)
Metabolism	hepatic (aldehyde reductase)
Half-life	7 hours
Excretion	Urine and feces
Therapeutic considerations
Licence data	US FDA:link
Pregnancy cat.	C(US)
Legal status	℞ Prescription only
Routes	oral, intramuscular
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Ziprasidone (marketed as Geodon, Zeldox by Pfizer) was the fifth atypical antipsychotic to gain FDA approval (February 2001). In the United States, Ziprasidone is Food and Drug Administration (FDA) approved for the treatment of schizophrenia, and the intramuscular injection form of ziprasidone is approved for acute agitation in schizophrenic patients. Ziprasidone has also received approval for acute treatment of mania and mixed states associated with bipolar disorder. The brand name Geodon has been suggested to bring to mind the phrase ‘down (don) to earth (geo)’ referring to the goals of the medication.

The oral form of ziprasidone is the hydrochloride salt, ziprasidone hydrochloride. The intramuscular form, on the other hand, is the mesylate salt, ziprasidone mesylate trihydrate, and is provided as a lyophilized powder.

Geodon was one of four drugs which Pfizer in 2009 pleaded guilty to misbranding “with the intent to defraud or mislead”. Pfizer agreed to pay $2.3 billion (£1.4 billion) in settlement, and entered a corporate integrity agreement. Pfizer was found to have illegally promoted four of its drugs for use in conditions that had not been approved by the FDA.^[1]

Contents [show]   1 Pharmacology 2 Pharmacokinetics 3 Adverse effects 4 Off-label uses 5 References 6 External links

[edit] Pharmacology

Ziprasidone has a high affinity for dopamine, serotonin, and alpha-adrenergic receptors and a moderate affinity for histamine receptors, where it is believed to act as an antagonist.^[2] Ziprasidone also displays some inhibition of synaptic reuptake of serotonin and norepinephrine^[2][3], although the clinical significance of this is unknown. The mechanism of action of ziprasidone is unknown. However it has been theorized that its antipsychotic activity is mediated primarily by antagonism at dopamine receptors, specifically D₂. Serotonin antagonism may also play a role in the effectiveness of ziprasidone, but the significance of 5-HT_2A antagonism is debated among researchers.^[4] Ziprasidone has perhaps the most selective affinity for 5-HT_2A receptors relative to D₂ and 5-HT_2C receptors of any neuroleptic.^[5][6] Antagonism at histaminic and alpha adrenergic receptors likely explains some of the side effects of ziprasidone, such as sedation and orthostasis.

[edit] Pharmacokinetics

The systemic bioavailability of ziprasidone administered intramuscularly is 100%, or 60%, administered orally with food. After a single dose intramuscular administration, the peak serum concentration typically occurs at about 60 minutes after the dose is administered, or earlier. Steady state plasma concentrations are achieved within one to three days. The mean half-life ranges from two to five hours. Exposure increases in a dose-related manner and following three days of intramuscular dosing, little accumulation is observed.

Ziprasidone absorption is not optimally achieved when administered without food. Without a meal preceding dose, the bioavailability of the drug is reduced by approximately 50%.^[7][8]

Ziprasidone is hepatically metabolized by aldehyde oxidase; minor metabolism occurs via cytochrome P450 3A4 (CYP3A4).^[9] Medications that induce (e.g. carbamazepine) or inhibit (e.g. ketoconazole) CYP3A4 have been shown to decrease and increase, respectively, blood levels of ziprasidone.^[10][11]

[edit] Adverse effects

Ziprasidone received a black box warning due to increased mortality in elderly patients with dementia-related psychosis.^[7] It also slightly increases the QTc interval in some patients and increases the risk of a potentially lethal type of heart arrhythmia known as torsades de pointes. Ziprasidone should be used cautiously in patients taking other medications likely to interact with ziprasidone or increase the QTc interval.^[12]

Patients in general will experience loss of focus and motivation as well as blurry vision to the point that stronger doses may cause thoughts of suicide while the medicine is in the patients system. Thoughts of suicide may occur. Typically side effects will start about an hour after ingestion and peak about four to five hours after ingestion. Patient will most likely be unable to operate machinery or drive a vehicle while the medicine is effecting the patient as blurred vision can be quite severe.

Ziprasidone may cause cause dangerous—even fatal—heartbeat irregularities.

Geodon generally adheres to the mid section of the prefrontal cortex. It derives from the ideas and thoughts process in the prefrontal cortex in which determines a treatment diagnosis for psychosis. Those who experience the symptoms of psychosis will experience on-going symptoms such as: lack of sleep, insomnia, and uncontrollable desires and experiences. Geodone adheres and corrects the prefrontal cortex by delivering an enzyme called (enzyme-B). This enzyme corrects the basal ganglia function which coorelates with the B-cortex hemispheres. In other words the enzyme delivers a vital nutrient into the system which is release by the geodome once again, called enzyme-b. The process of Geodon is somewhat confusing as it affects both the basal ganglia and prefrontal cortex. By affecting the basal ganglia the prefrontal cortex does what is called: identity change. This is a process in which enzymes are switched from one section of the brain to another. The prefrontal cortex is mainly involved in spacial recognition which will be slightly alleviated by the geodon. Those who experience spacial recognition problems usually suffer from psychosis.

Ziprasidone is known to cause activation into mania in some bipolar patients.^[13][14][15]

This medication can cause birth defects, according to animal studies, although this side effect has not been confirmed in humans.^[7]

Adverse events reported for ziprasidone include severe chest pains, impaired erectile function and stimulation, sedation, insomnia, orthostasis, life-threatening neuroleptic malignant syndrome, akathisia, and the development of permanent neurological disorder tardive dyskinesia. Rarely, temporary speech disorders may result.

Recently, the FDA required the manufacturers of some atypical antipsychotics include a warning about the risk of hyperglycemia and Type II diabetes with atypical antipsychotics. Some evidence suggests that ziprasidone may not be as bad as some of the other atypical antipsychotics (namely, olanzapine (Zyprexa)) at causing insulin resistance and weight gain.^{[16][17][18][19]} In fact, in a trial of long term therapy with ziprasidone, overweight patients (BMI > 27) actually had a mean weight loss overall.^[7] Ziprasidone, though, is not a weight loss drug. The weight loss reflected in this study on ziprasidone was really reflective of patients who had gained weight on other antipsychotics who were now trending back toward their baseline.^{[citation needed]}clozapine and olanzapine). According to the manufacturer insert, ziprasidone caused an average weight gain of 2.2 kg (4.8 lbs) (which is significantly lower than other atypicals–

[edit] Off-label uses

In addition to its antipsychotic use, ziprasidone is sometimes prescribed for the treatment of tic disorders. A small study^[20] has supported the efficacy of this use.

October 15, 2010 Posted by archmichaelangelo | 2001, Science and medicine, The war | 2001, Beheaded for the witness, Chemical internment, Deaths, Defendence production act, disinformation, economics, Fraud, Geodon, manufacturing, medicine, misrepresentation, Murder, Pharmaceutical Industry, psychotropic, Symbolic misrepresentation, wrongful deaths | Leave a comment