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Antipsychotics scribdt

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Purna Nagasree K

This ppt gives an insight about the antipsychotics drugs mechansim of action, SAR and individuals drugs usage from medicinal chemistry point of view

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MEDICINAL CHEMISTRY I B. PHARMACY II/IV (FIRST SEM) Dr. K. Purna Nagasree M.Pharm. (BITS, Pilani), Ph.D., PDF (DST, WOSA)
Antipsychotics  Tranquillizers are used primarily for the treatment of symptoms of mental diseases.  They cause sedation without inducing sleep. They are essentially used in the symptomatic treatment of psychosis, such as schizophrenia and organic psychosis.  The symptoms of schizophrenia can be divided into two types, positive and negative.  Positive symptoms are those that are not normally found in healthy individuals, including hallucinations, delusions, and thought disorder.
Antipsychotics  Negative symptoms represent the loss of qualities normally present in healthy individuals, including impoverishment of thought, blunted emotion, attention deficit, and lack of motivation or initiative. In addition, many of these drugs also act as skeletal muscle relaxants, antihypertensives, antiemetics, and antiepileptics.
Anti Psychotics  Phenothiazines: SAR, Promazine HCl, Chlopromazine HCl*, Triflupromazine, Thioridazine HCl, Piperacetazine HCl, Prochlorperazine maleate,Trifluoperazine HCl  Ring analogues of phenothiazines: Chlorprothixene, Thiothixene, Loxapine succinate, Clozapine  Fluorobutyrophenones: Haloperidol, Droperidol, Risperidone  Beta amino ketones: Molindone HCl  Benzamides: Sulpiride
classification 1. Phenothiazine derivatives Piperacetazine
2. Ring analogues of phenothiazines  Thioxanthenes  Dibenzoxazepines Loxapine succinate  Dibenzodiazepines Clozapine Xanthene
3. Fluorobutyrophenones  Benzisoxazoles - Risperidone
4.Beta amino ketones: Dihydroindolones-Molindone HCl 5.Benzamides: Sulpiride
6. Benzodiazepines – Chlordiazepoxide, lorazepam 7. Rauwolfia alkaloids – Reserpine, Reserpidine 8. Diphenyl butyl piperidines – Pimozide 9.Thienbenzodiazepines a. Olanzapine 10. Propanediol carbamates a. Meprobamate 11. Miscellaneous a.Oxypertine b. Quetiapine c. Seretindole
Antipsychotics: MOA All antipsychotics except cloazapine have potent dopamine (D2) receptor blocking action. Phenothiazines and thioxanthanes also block D1, D3, and D4 receptors and have correlation with antipsychotic or tranquillizing property. Blockade of the dopaminergic projections to the temporal and the prefrontal area constitutes the limbic system, and in the mesocortical area, it is probably responsible for antipsychotic action.
Antipsychotics : MOA  However, over a period of time, this subsides and gives away diminished activity, especially in the basal to ganglia corresponding to the emergency of Parkinsons disease.  Clozapine, Flurobutyrophenones and sulpiride and other atypical antipsychotics have significant 5-HT2 and α1 blocking action and are relatively selective for D4 receptor.  Thus, antipsychotic property depends on a specific profile of action of the drugs on several neurotransmitter receptors.
Promazine HCl  It is a white or almost white crystalline powder, slightly hygroscopic in nature.  well soluble in water, alcohol, and methylene chloride.  It has low clinical potency, medium extrapyramidal toxicity, high sedative effect, and high hypotensive action.  It is used as dopamine receptor antagonist and neuroleptic.
Chlopromazine HCl*  Metabolism: It is demethylated, sulphoxidized, hydroxylated, and glucuronidated to yield 7-o-glu-nor chlorpromazine.  Properties and uses: It is a white or almost white crystalline powder, freely soluble in ethanol and well soluble in water.  The drug has significant sedative and hypotensive properties, possibly reflecting central and peripheral α1-noradrenergic blocking activity and also effects the peripheral anticholinergic activity  Used as dopamine receptor antagonist and neuroleptic.
Triflupromazine  It is a white to pale yellow, crystalline powder, hygroscopic in nature, soluble in alcohol and freely soluble in water.  It has lower sedative and hypotensive effects than chlorpromazine, and greater milligram potency as an antipsychotic  used as dopamine receptor antagonist and neuroleptic.
Thioridazine HCl  It is a white or almost white crystalline powder, soluble in ethanol, freely soluble in water and in methanol.  The drug exerts minimum antiemetic activity and there by gives rise to minimal extrapyramidal stimulation.  The drug has sedative and hypotensive activity in common with chlorpromazine.  It is effective in the management and manifestations of psychotic disorders, used as Dopamine receptor antagonist and neuroleptic.
Piperacetazine HCl  Piperacetazine is an antipsychotic prodrug, most notably used for schizophrenia 1-[10-[3-[4-(2-hydroxyethyl)-1-piperidinyl]propyl]-2- phenothiazinyl]ethanone
Prochlorperazine maleate  It is a white or pale yellow crystalline powder, well soluble in water and alcohol.  It is more potent on a milligram basis than its alkylamino counterpart, chlorpromazine because of the high prevalence of extra-pyramidal symptom (EPS).  It is mainly used for anti-emetic effect, not for its anti- psychotic effect, used as dopamine receptor antagonist and neuroleptic.
Trifluoperazine HCl  A phenothiazine with actions similar to chlorpromazine. It is used as an antipsychotic and an antiemetic. 10-[3-(4-methylpiperazin-1-yl)propyl]-2-(trifluoromethyl)-10H-phenothiazine dihydrochloride
Chlopromazine HCl* Synthesis
Phenothiazines: SAR  It is presumed that phenothiazines (neuroleptic) mediate their pharmacological effect mainly through interaction at D2 type dopamine receptors.  Examination of X-ray structures of dopamine and chlorpromazine  substituted with chlorine shows that these two structures can be partly superimposed.  Chlorpromazine base could be superimposed on aromatic ring of dopamine base with sulphur atom aligned with p-hydroxy of dopamine.  These substances are chemically constituted by lipophilic linearly fused tricyclic system having hydrophilic basic amino alkyl side chain.  Activity of phenothazines is determined by the following:  1. Nature of alkyl side chain at C-10.  2. Amino group of side chain.  3. Substituents on aromatic ring.
SAR Phenothiazines 1. Modification of alkyl side chain  Potency is maximum when there is three carbon between two ‘N’ atom (ring and side chain N ).  Introduction of methyl group at C-1 decreases antipsychotic activity and produces imipramine-like activity.  If C-1 is incorporated into cyclopropane ring imipramine-like activity is obtained.  When oxygen is introduced into C-1 results in potent antidepressant effect. Example: Chloracizine.  Addition of –CH3 at C-2 or C-3 has very little effect on activity.  Bridging of position 3 of side chain to position 1 of phenothiazine nucleus decreases neuroleptic activity.
Phenothiazines: SAR 2. Amino group modification  3° nitrogen shows maximum potency and 2° or 1° nitrogen shows reduced or abolished activity.  N-alkylation with more than one carbon decreases activity.  Activity is decreased when dimethylamino group is replaced by pyrolidinyl, morpholinyl, or thiomorpholinyl groups. However, piperidine or piperazine is more potent than dimethylamino group.  Bridged piperidine derivates retain high degree of activity although bulky.
Phenothiazines: SAR  Piperazine and phenothiazines may be esterified with long-chain fatty acids to produce slowly absorbed long-acting lipophilic prodrugs.  Due to the slow release from oily deposition, signifi cant activity is retained  When N-4 piperazine substituents are as large as phenyl, ethyl, or p-amino phenyl ethyl (e.g.Azaspirane, Chlorspirane) are active.
Phenothiazines: SAR 3. Phenothiazine ring  Substitution at C-2 position is optimal for neuroleptic activity. In general, potency at different positions increases in the following order 1 < 4 < 3 < 2. Potency of the various groups increase in the following order OH < H< CN < CH3 < Cl < CF3.  Disubstitution (or) trisubstitution of the C-2 substituted drugs results in harmful potency.  CF3 is more potent than Cl, but EPS appears, hence, chlorpromazine is much used, rather than triflupromazine.  The electro-negative chlorine atom at C-2 is responsible for imparting asymmetry to this molecule and the attraction of the amine side chain towards the ring containing the chlorine atom indicate an important structural feature of such molecules.  Oxidation of the sulphur at 5th position of antipsychotic phenothiazine decreases activity.
Ring analogues of phenothiazines
Chlorprothixene It is a white or almost white crystalline powder, slightly soluble in methylene chloride, and soluble in water and alcohol. It is used in the treatment of acute and chronic schizophrenia, psychotic and other conditions in which anxiety, agitation, and tension predominate. Metabolism: Thioxanthines are closely related to the phenothiazine in their pharmacologic effects and there seems to be at least one major difference in metabolism, most of the thioxanthine do not form ring hydroxylated derivatives.
Thiothixene  White, or nearly white crystalline powder with slight odour, and affected by light, soluble in water, anhydrous alcohol, or chloroform, practically insoluble in benzene, acetone, or ether.  The substituent in the second position produces Z and E isomers. The Z isomers are the more active antipsychotic isomers.  It was introduced as an antipsychotic agent useful in the management of schizophrenia and other psychotic states. It is also helpful in the management of secondary symptoms of schizophrenia, such as hallucinations, tension, and suspiciousness. It also shows antidepressant property.
Loxapine succinate  Exist as white to off-white crystalline powder, slightly soluble in water or alcohol.  It may give rise to possible anticholinergic and antiadrenergic activity. It must be employed with great caution in such patients who have either a history of glaucoma or urinary retention problems.  It has resulted from the expansion of the six-member central ring of phenothiazine followed by isosteric replacement of one or more atoms with oxygen.  Because of its seven-member central ring, the conformation of loxapine is more twisted than that of the phenothiazine rings. It is used for symptomatic control of schizophrenia.
Clozapine  It is a yellow crystalline powder, dissolves in dilute acetic acid, insoluble in water, freely soluble in methylene chloride, and soluble in alcohol.  It has more affinity for D1 and less for D2 dopamine receptors. Selective to D4  It may have its unique profile due to the blockade of D1 receptors and M1 muscarinic activity.  It has high potentially fatal agranulocytosis. Other adverse side effects include drowsiness, dizziness, and dose related seizures.  It is effective in individuals suffering from disorganization. For example, loose associations, inappropriate affect, incoherence, and reduction in rational thought processes.
Fluorobutyrophenones
Haloperidol
Droperidol
Risperidone
Beta amino ketones: Molindone HCl Exists as white crystals, freely soluble in water or alcohol It is a potent antipsychotic as trifluoperazine and all the side effects resemble those of the phenothiazines. It is used in the treatment of schizophrenia and other psychosis.
Benzamides: Sulpiride N-[(1-ethylpyrrolidin-2-yl)methyl]-2-methoxy-5- sulfamoylbenzamide A dopamine D2-receptor antagonist. It has been used therapeutically as an antidepressant, antipsychotic, and as a digestive aid.

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Antipsychotics scribdt

  • 1. MEDICINAL CHEMISTRY I B. PHARMACY II/IV (FIRST SEM) Dr. K. Purna Nagasree M.Pharm. (BITS, Pilani), Ph.D., PDF (DST, WOSA)
  • 2. Antipsychotics  Tranquillizers are used primarily for the treatment of symptoms of mental diseases.  They cause sedation without inducing sleep. They are essentially used in the symptomatic treatment of psychosis, such as schizophrenia and organic psychosis.  The symptoms of schizophrenia can be divided into two types, positive and negative.  Positive symptoms are those that are not normally found in healthy individuals, including hallucinations, delusions, and thought disorder.
  • 3. Antipsychotics  Negative symptoms represent the loss of qualities normally present in healthy individuals, including impoverishment of thought, blunted emotion, attention deficit, and lack of motivation or initiative. In addition, many of these drugs also act as skeletal muscle relaxants, antihypertensives, antiemetics, and antiepileptics.
  • 4. Anti Psychotics  Phenothiazines: SAR, Promazine HCl, Chlopromazine HCl*, Triflupromazine, Thioridazine HCl, Piperacetazine HCl, Prochlorperazine maleate,Trifluoperazine HCl  Ring analogues of phenothiazines: Chlorprothixene, Thiothixene, Loxapine succinate, Clozapine  Fluorobutyrophenones: Haloperidol, Droperidol, Risperidone  Beta amino ketones: Molindone HCl  Benzamides: Sulpiride
  • 6. 2. Ring analogues of phenothiazines  Thioxanthenes  Dibenzoxazepines Loxapine succinate  Dibenzodiazepines Clozapine Xanthene
  • 9. 6. Benzodiazepines – Chlordiazepoxide, lorazepam 7. Rauwolfia alkaloids – Reserpine, Reserpidine 8. Diphenyl butyl piperidines – Pimozide 9.Thienbenzodiazepines a. Olanzapine 10. Propanediol carbamates a. Meprobamate 11. Miscellaneous a.Oxypertine b. Quetiapine c. Seretindole
  • 10. Antipsychotics: MOA All antipsychotics except cloazapine have potent dopamine (D2) receptor blocking action. Phenothiazines and thioxanthanes also block D1, D3, and D4 receptors and have correlation with antipsychotic or tranquillizing property. Blockade of the dopaminergic projections to the temporal and the prefrontal area constitutes the limbic system, and in the mesocortical area, it is probably responsible for antipsychotic action.
  • 11. Antipsychotics : MOA  However, over a period of time, this subsides and gives away diminished activity, especially in the basal to ganglia corresponding to the emergency of Parkinsons disease.  Clozapine, Flurobutyrophenones and sulpiride and other atypical antipsychotics have significant 5-HT2 and α1 blocking action and are relatively selective for D4 receptor.  Thus, antipsychotic property depends on a specific profile of action of the drugs on several neurotransmitter receptors.
  • 12. Promazine HCl  It is a white or almost white crystalline powder, slightly hygroscopic in nature.  well soluble in water, alcohol, and methylene chloride.  It has low clinical potency, medium extrapyramidal toxicity, high sedative effect, and high hypotensive action.  It is used as dopamine receptor antagonist and neuroleptic.
  • 13. Chlopromazine HCl*  Metabolism: It is demethylated, sulphoxidized, hydroxylated, and glucuronidated to yield 7-o-glu-nor chlorpromazine.  Properties and uses: It is a white or almost white crystalline powder, freely soluble in ethanol and well soluble in water.  The drug has significant sedative and hypotensive properties, possibly reflecting central and peripheral α1-noradrenergic blocking activity and also effects the peripheral anticholinergic activity  Used as dopamine receptor antagonist and neuroleptic.
  • 14. Triflupromazine  It is a white to pale yellow, crystalline powder, hygroscopic in nature, soluble in alcohol and freely soluble in water.  It has lower sedative and hypotensive effects than chlorpromazine, and greater milligram potency as an antipsychotic  used as dopamine receptor antagonist and neuroleptic.
  • 15. Thioridazine HCl  It is a white or almost white crystalline powder, soluble in ethanol, freely soluble in water and in methanol.  The drug exerts minimum antiemetic activity and there by gives rise to minimal extrapyramidal stimulation.  The drug has sedative and hypotensive activity in common with chlorpromazine.  It is effective in the management and manifestations of psychotic disorders, used as Dopamine receptor antagonist and neuroleptic.
  • 16. Piperacetazine HCl  Piperacetazine is an antipsychotic prodrug, most notably used for schizophrenia 1-[10-[3-[4-(2-hydroxyethyl)-1-piperidinyl]propyl]-2- phenothiazinyl]ethanone
  • 17. Prochlorperazine maleate  It is a white or pale yellow crystalline powder, well soluble in water and alcohol.  It is more potent on a milligram basis than its alkylamino counterpart, chlorpromazine because of the high prevalence of extra-pyramidal symptom (EPS).  It is mainly used for anti-emetic effect, not for its anti- psychotic effect, used as dopamine receptor antagonist and neuroleptic.
  • 18. Trifluoperazine HCl  A phenothiazine with actions similar to chlorpromazine. It is used as an antipsychotic and an antiemetic. 10-[3-(4-methylpiperazin-1-yl)propyl]-2-(trifluoromethyl)-10H-phenothiazine dihydrochloride
  • 20. Phenothiazines: SAR  It is presumed that phenothiazines (neuroleptic) mediate their pharmacological effect mainly through interaction at D2 type dopamine receptors.  Examination of X-ray structures of dopamine and chlorpromazine  substituted with chlorine shows that these two structures can be partly superimposed.  Chlorpromazine base could be superimposed on aromatic ring of dopamine base with sulphur atom aligned with p-hydroxy of dopamine.  These substances are chemically constituted by lipophilic linearly fused tricyclic system having hydrophilic basic amino alkyl side chain.  Activity of phenothazines is determined by the following:  1. Nature of alkyl side chain at C-10.  2. Amino group of side chain.  3. Substituents on aromatic ring.
  • 21. SAR Phenothiazines 1. Modification of alkyl side chain  Potency is maximum when there is three carbon between two ‘N’ atom (ring and side chain N ).  Introduction of methyl group at C-1 decreases antipsychotic activity and produces imipramine-like activity.  If C-1 is incorporated into cyclopropane ring imipramine-like activity is obtained.  When oxygen is introduced into C-1 results in potent antidepressant effect. Example: Chloracizine.  Addition of –CH3 at C-2 or C-3 has very little effect on activity.  Bridging of position 3 of side chain to position 1 of phenothiazine nucleus decreases neuroleptic activity.
  • 22. Phenothiazines: SAR 2. Amino group modification  3° nitrogen shows maximum potency and 2° or 1° nitrogen shows reduced or abolished activity.  N-alkylation with more than one carbon decreases activity.  Activity is decreased when dimethylamino group is replaced by pyrolidinyl, morpholinyl, or thiomorpholinyl groups. However, piperidine or piperazine is more potent than dimethylamino group.  Bridged piperidine derivates retain high degree of activity although bulky.
  • 23. Phenothiazines: SAR  Piperazine and phenothiazines may be esterified with long-chain fatty acids to produce slowly absorbed long-acting lipophilic prodrugs.  Due to the slow release from oily deposition, signifi cant activity is retained  When N-4 piperazine substituents are as large as phenyl, ethyl, or p-amino phenyl ethyl (e.g.Azaspirane, Chlorspirane) are active.
  • 24. Phenothiazines: SAR 3. Phenothiazine ring  Substitution at C-2 position is optimal for neuroleptic activity. In general, potency at different positions increases in the following order 1 < 4 < 3 < 2. Potency of the various groups increase in the following order OH < H< CN < CH3 < Cl < CF3.  Disubstitution (or) trisubstitution of the C-2 substituted drugs results in harmful potency.  CF3 is more potent than Cl, but EPS appears, hence, chlorpromazine is much used, rather than triflupromazine.  The electro-negative chlorine atom at C-2 is responsible for imparting asymmetry to this molecule and the attraction of the amine side chain towards the ring containing the chlorine atom indicate an important structural feature of such molecules.  Oxidation of the sulphur at 5th position of antipsychotic phenothiazine decreases activity.
  • 26. Chlorprothixene It is a white or almost white crystalline powder, slightly soluble in methylene chloride, and soluble in water and alcohol. It is used in the treatment of acute and chronic schizophrenia, psychotic and other conditions in which anxiety, agitation, and tension predominate. Metabolism: Thioxanthines are closely related to the phenothiazine in their pharmacologic effects and there seems to be at least one major difference in metabolism, most of the thioxanthine do not form ring hydroxylated derivatives.
  • 27. Thiothixene  White, or nearly white crystalline powder with slight odour, and affected by light, soluble in water, anhydrous alcohol, or chloroform, practically insoluble in benzene, acetone, or ether.  The substituent in the second position produces Z and E isomers. The Z isomers are the more active antipsychotic isomers.  It was introduced as an antipsychotic agent useful in the management of schizophrenia and other psychotic states. It is also helpful in the management of secondary symptoms of schizophrenia, such as hallucinations, tension, and suspiciousness. It also shows antidepressant property.
  • 28. Loxapine succinate  Exist as white to off-white crystalline powder, slightly soluble in water or alcohol.  It may give rise to possible anticholinergic and antiadrenergic activity. It must be employed with great caution in such patients who have either a history of glaucoma or urinary retention problems.  It has resulted from the expansion of the six-member central ring of phenothiazine followed by isosteric replacement of one or more atoms with oxygen.  Because of its seven-member central ring, the conformation of loxapine is more twisted than that of the phenothiazine rings. It is used for symptomatic control of schizophrenia.
  • 29. Clozapine  It is a yellow crystalline powder, dissolves in dilute acetic acid, insoluble in water, freely soluble in methylene chloride, and soluble in alcohol.  It has more affinity for D1 and less for D2 dopamine receptors. Selective to D4  It may have its unique profile due to the blockade of D1 receptors and M1 muscarinic activity.  It has high potentially fatal agranulocytosis. Other adverse side effects include drowsiness, dizziness, and dose related seizures.  It is effective in individuals suffering from disorganization. For example, loose associations, inappropriate affect, incoherence, and reduction in rational thought processes.
  • 34. Beta amino ketones: Molindone HCl Exists as white crystals, freely soluble in water or alcohol It is a potent antipsychotic as trifluoperazine and all the side effects resemble those of the phenothiazines. It is used in the treatment of schizophrenia and other psychosis.
  • 35. Benzamides: Sulpiride N-[(1-ethylpyrrolidin-2-yl)methyl]-2-methoxy-5- sulfamoylbenzamide A dopamine D2-receptor antagonist. It has been used therapeutically as an antidepressant, antipsychotic, and as a digestive aid.

Editor's Notes

  1. Trifluoperazine blocks postsynaptic mesolimbic dopaminergic D1 and D2 receptors in the brain; depresses the release of hypothalamic and hypophyseal hormones and is believed to depress the reticular activating system thus affecting basal metabolism, body temperature, wakefulness, vasomotor tone, and emesis.