Download - Neuroleptic Antipsychotics

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Davis MDCH 5210 - Antipsychotics, 2005

Treatment of Psychoses:

Schizophrenia, Depression, Manic-Depressive Disorder

Macbeth: How does your patient, doctor?Doctor: Not so sick, my lord, as she is troubled with thick-coming fantasies, that keep her from her rest.Macbeth: Cure her of that: Canst thou not minister to a mind diseas’d; pluck from the memory a rooted sorrow; raze out the written troubles of the brain; and with some sweet oblivious antidote cleanse the stuff’d bosom of that perilous stuff which weighs upon the heart?Doctor: Therein the patient must minister to himself.

-William Shakespeare, Macbeth

Neuroleptic Antipsychotics

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N

N

N

N

H

H3

C

Cl

Clozapine

N

S

CH2

CH2

CH2

N(CH3

)2

Cl

Chlorpromazine

What is a “neuroleptic”?Neuroleptic compounds are CNS depressants that do not generally cause a loss of consciousness by themselves. The can produce a state of “artificial hibernation” by themselves and in combination with anesthetics. This indicates that the patient can be aroused from this state, differentiating it from anesthesia.

Neuroleptics potentiate the action of anesthetics, and this action is a defining factor. These effects are usually thought due directly to activity at D2 receptors.

Reserpine is also an antipsychotic due to its effects on dopamine levels, but it is non-selective with many side effects.

Neuroleptic Definition

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•Modest sedative activity•Low potential for lethality•Low abuse potential, non-euphoric•Motor Inhibition•Anti-emetic due to dopamine antagonism of the chemoreceptor trigger zone (CTZ).•Diminish conditioned responses, but not unconditioned.

Conditioned: Spontaneous movement and complex behaviors. Conditioned avoidance. Think Pavlov’s dog. The bell, but not the shock.

Unconditioned: Spinal reflexes, nociceptive avoidance behaviors remain intact. The shock.

Emotional responses are reduced.

Properties of Neuroleptic Antipsychotics.

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Act at D2, D3, and D4 receptors. D2 agonist activity inhibits adenylate cyclase.

Chlorpromazine is the prototype drug in terms of SAR and in terms of activity profile.

Chlorpromazine has a 50:1 D2/D3 affinity.Clozapine (the prototype atypical antipsychotic) has a 4:1 receptor ratio. Clozapine also binds D4 about 10-fold better than D2.

Most anti-psychotics have -adrenergic antagonist activity. Chlorpromazine is more active at adrenergic receptors than haloperidol.

Clozapine, the “atypical” antipsychotic has high affinity for 5HT2, 1, and histamine H1 receptors. Actually better than D1 or D2.

All neuroleptic antipsychotics have antimuscarinic effects as well as anti-emetic activity associated with anti-dopaminergic activity.

Antipsychotic Mechanism(s). Primarily Dopamine Antagonists.

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Dopaminergic Neurons

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N

S

CH2CH2CH2NR2

X

1 2 3

2

1. Propyl Side Chain

•Propyl is best, butyl is nearly inactive, ethyl has low activity. Compounds with ethyl chains often have antihistaminic activity.•Any substituent at the first position of the side chain decreases activity.•Substitution of a methyl at position 2 of the chain is OK, phenyl is OK. Large aliphatic substituents are not tolerated.•A larger range of substitutions are tolerated at position 3. The nitrogen is often included as part of a ring.

2. Modification of X and the the Tricyclic Nucleus

•Highest activity is associated with an electron withdrawing, lipophilic substituent (halogen) at position 2. A trend in activity changes can be seen with alterations in the identity of X; increasing lipophilicity and e- withdrawing increases activity.•Disubstitution of the ring decreases activity, ring cleavage is inactivating.•Replacing S with C, O, Se, etc. decreases activity. Replacing the nitrogen eliminates activity (except in special cases.

Phenothiazine SAR

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N

S

CH2CH2CH2NR2

X

1 2 3

2

3. Modification of Side Chain Amino Group

•The highest activity is for 3° amines (pKa’s of 8-10). Methyl R groups on nitrogen have greater activity that larger aliphatic groups. The receptor is long and narrow as shown by the amino substitution and by the tolerance to phenyl substitution at C2.•The amino group can be part of a cyclic structure. The cyclic amines include pyrrolidine, piperidine, and piperazine. The piperazine substituent, in particular, generally increases potency.

Propyl dimethylamino side chain(chlorpromazine (Thorazine))

Alkyl piperdinyl and pyrrolidinyl side chain(thioridazine (Mellaril))

Propyl piperazine side chain(prochlorperazine (Compazine))

CH2

CH2

CH2

N(CH3

)2

(CH2

)3

N

(CH2

)3

N

(CH2

)3

N N R

Phenothiazine SAR - Page 2

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OH < H < OCH3

< CH3

< CCH3

~ SCH3

< Cl < SCH3

~ SCH3

~ Br ~ SCF3

< SCF3

< CF3

O O

O

O O

O

Phenothiazine Metabolism

Three major processes; all give compounds that are less active.

Ring hydroxylation – followed by glucuronidation N-dealkylation terminal nitrogenOxidation at S and at terminal nitrogen.

The order of potency for a “few” X substitutents are shown. The most important are indicated by arrows, and Cl of course.

N

S

CH2CH2CH2NR2

X

1 2 3

2

Identity of Phenothiazine X and Effects on Potency

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Phenothiazine/Thioxanthene Neuroleptics

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Long Acting Neuroleptics

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S

X

H CH2

CH2

NR1

R2

2

"R"

SARCis double bond compounds are much more active than trans. Double bond reduction reduces activity.

Other SAR is the same as for the phenothiazines

(CH2

)2

N N CH3

R =

X = S

O

O

N

CH3

CH3

Thiothixene (Navane) - 10x chlorpromazine

Chlorprothixene (Taractan) - 1x chlorpromazine

R = (CH2)2N(CH3)2 X = Cl

Thioxanthene Antipsychotics.

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N

NN

N

H

CH3

Cl

N

NN

N

H

H3C

Cl

O

NN

NCH3

Cl

O

NN

NCH3

Cl

Clozapine

Loxapine Loxapine

Clozapine

N

S

CH2CH2CH2N(CH3)2

Cl

Chlorpromazine

Three Dimensional SAR of Typical and Atypical Antipsychotics.

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OH

ON

N

N

S

CH3N

N

HCH3S

N

N

Cl

CH3

N

N

N

O

Cl

CH3

H

N

N

N

N

Olanzapine (Zyprexa) Atypical

LoxapineClozapine

O

FCH3

N O

N

N

N

HCl

ON

N

N

SN

Risperidone (Risperdal) Atypical

Quetiapine (Seroquel) Atypical

Ziprasidone (Geodon) Atyical

The Atypical Antipsychotics

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NOC2H5

OO

NOC2H5

O

O

CH3NOC2H5

O

NOH

O

Cl

F

Meperidine

Propophenone

200 x Meperidine as an Analgesic

ButyrophenoneAnalgesia similar to MeperidineOther activity similar to Chlorpromazine

Haloperidol (Haldol)Prototype butyrophenone antipsychotic10x Chlorpromazine

The History/Evolution of Butyrophenone Neuroleptics.

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N Y

O

X

R1

R

Phenone

butyro

• For highest potency, X is always F. –OCH3 has the lowest potency. This tells you that an electron withdrawing group, not electron donating is optimal.• Shortening, lengthening, or branching of the propyl chain decreases potency• Replacing the keto oxygen with S, carbon, OH decreases potency• A 3° N is necessary, analogous to phenothiazines• Y is usually C with two R groups, but may be N.

For example piperazine instead of piperdine.

Examples:Haloperidol: This is the prototype for this class. One variation is to esterify the OH with decanoic acid to increase the duration.Droperidol (Inapsine): Strong sedative. In combination with Fentanyl (an analgesic) is given as a preanesthetic sedative (Innovar). Droperidol is also antiemetic which is important.Trifluperiodol: Similar to Haloperidol

Butyrophenone SAR

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N

O

F

N NH

O

Droperidol (Inapsine)

NOH

O

CF3

F

Trifluperidol

N

F

N NH

O

F

H

Pimozide (Orap) "diphenylbutylpiperidine"similar to haloperidol, longer duration. Used for Tourette's Syndrome.

Butyrophenone Neuroleptics

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N

N

N

N

H

CH3

Cl

O

N

N

N

CH3

Cl

Most of the neuroleptics have anticholinergic activity. The “atypical” antipsychotics also generally have 1 adrenergic antagonist activity.

N

S

CH2

CH2

CH2

N(CH3

)2

Cl

Chlorpromazine

NCH3

OC

H

Benztropine

HNN

CH2

N OH

H3

C

Phentolamine

(Regitine) non-selective ntgonist

Anticholinergic activity

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PNAS | July 5, 2000 | vol. 97 | no. 14 | 7673-7675

Schizophrenia: More dopamine, more D2 receptorsPhilip Seeman and Shitij Kapur

Of the many contemporary theories of schizophrenia, the most enduring has been the dopamine hypothesis. As originally put by Van Rossum in 1967(ref. 1, p. 321), "When the hypothesis of dopamine blockade by neuroleptic agents can be further substantiated, it may have fargoing consequences for the pathophysiology of schizophrenia. Overstimulation of dopamine receptors could be part of the aetiology ...[emphasis added]." Indeed, this speculative sentence by Van Rossum foreshadows the title of the important work by Abi-Dargham et al. (2) in this issue of PNAS: "Increased baseline occupancy of D2 receptors by dopamine in schizophrenia."

PHILIP SEEMAN* , HONG-CHANG GUAN* & HUBERT H. M.VAN TOL*

Nature 365, 441 - 445 (1993)

Dopamine D4 receptors elevated in schizophrenia

http://www.pnas.org/cgi/content/full/97/14/7673#B1

http://www.pnas.org/cgi/content/full/97/14/7673#B2

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Fig. 1. Method and findings of Abi-Dargham et al. (2) to reveal an increased occupancy of dopamine D2 receptors in schizophrenia. (Top) The number of dopamine D2 receptors, measured by the [123I]IBZM binding potential (green triangles with I), were the same in the brain striata of control and schizophrenia subjects. The levels of synaptic dopamine (pink triangles with D), which is higher in patients compared to control subjects, normally occupies most of the D2 receptors, masking the difference between control and schizophrenia individuals. (Bottom) After partial depletion of endogenous brain dopamine by oral ingestion of -methylparatyrosine over 2 days, the binding of [123I]IBZM rose in both the control and schizophrenia subjects, but that for the patients rose significantly higher.

More Dopamine

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Fig. 2. Possible model to account for the increased number of dopamine D2 receptors in schizophrenia seen with [11C]methylspiperone but not with [11C]raclopride. It is known that the photolabel of spiperone ([125I]azidophenethylspiperone) primarily or selectively labels monomers of D2 receptors, whereas the benzamide photolabel ([125I]azido-iodo-nemonapride) unselectively labels monomers, dimers, and oligomers of D2 receptors (see text). These findings suggest that even if there is no increase in the total population of D2 receptors in schizophrenia, an increase in the proportion of monomers caused by the increased level of dopamine in schizophrenia (see Fig. 1) would result in an increase in the binding of [11C]methylspiperone (red triangle with S) in schizophrenia but not with [11C]raclopride (white triangle with R).

Still More Dopamine

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•Equivalent occupancy of dopamine D1 and D2 receptors with clozapine: differentiation from other atypical antipsychotics.•Tauscher J, Hussain T, Agid O, Verhoeff NP, Wilson AA, Houle S, Remington G, Zipursky RB, Kapur S.• •OBJECTIVE: Clozapine, the prototype of atypical antipsychotics, remains unique in its efficacy in the treatment of refractory schizophrenia. Its affinity for dopamine D(4) receptors, serotonin 5-HT(2A) receptor antagonism, effects on the noradrenergic system, and its relatively moderate occupancy of D(2) receptors are unlikely to be the critical mechanism underlying its efficacy. In an attempt to elucidate the molecular/synaptic mechanism underlying clozapine's distinctiveness in refractory schizophrenia, the authors studied the in vivo D(1) and D(2) receptor profile of clozapine compared with other atypical antipsychotics. •RESULTS: The ratio of striatal D(1)/D(2) occupancy was significantly higher for clozapine (0.88) relative to olanzapine (0.54), quetiapine (0.41), or risperidone (0.31).

•CONCLUSIONS: Among the atypical antipsychotics, clozapine appears to have a simultaneous and equivalent occupancy of dopamine D(1) and D(2) receptors. Whether its effect on D(1) receptors represents agonism or antagonism is not yet clear, as this issue is still unresolved in the preclinical arena. This distinctive effect on D(1)/D(2) receptors may be responsible for clozapine's unique effectiveness in patients with schizophrenia refractory to other typical and atypical antipsychotics.

Am J Psychiatry. 2004 Sep;161(9):1620-5Dopamine Receptors and

Clozapine

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=pubmed&cmd=Search&term=%22Tauscher+J%22%5BAuthor%5D

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=pubmed&cmd=Search&term=%22Hussain+T%22%5BAuthor%5D

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=pubmed&cmd=Search&term=%22Hussain+T%22%5BAuthor%5D

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=pubmed&cmd=Search&term=%22Agid+O%22%5BAuthor%5D

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=pubmed&cmd=Search&term=%22Agid+O%22%5BAuthor%5D

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What were some of the reasons that D3 and D4 receptors are attractive antipsychotic targets?

What is the status of the D3 and D4 receptors as important sites for antipsychotic action?

Do Schizophrenics have higher DA levels, or do they have a higher number of DA receptors?

How were the levels of DA and DA receptors determined in the Abi-Dargham et al. study?

What is the role of 5HT receptors in schizophrenia? Modulation of DA?

What is the status of the “Dopamine Hypothesis” according to Seeman?

Does the DA receptor binding of clozapine support the “DA hypothesis”?

What is an “atypical antipsychotic”?

Questions: Dopamine Hypothesis

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FIGURE 3. (A) Proposed model of modulation of DA cell activity by cortical projections. This model, adapted from Carlsson and colleagues,70 proposes a bimodal modulation of DA activity in the ventral tegmental area (VTA) by glutamatergic (GLU) projections originating in the frontal cortex. DA levels in cortex may be reduced in schizophrenic brain, increasing midbrain levels. Balance of positive and negative glutamate regulation is altered.

Glutamate, Dopamine, and Schizophrenia. From Pathophysiology to Treatment

MARC LARUELLE, LAWRENCE S. KEGELES and ANISSA ABI-DARGHAM. Ann. N.Y. Acad. Sci. 1003: 138-158 (2003).

Is antipsychotic therapy counterintuitive, or do we simply not understand brain function?

Do we still believe in the dopamine hypothesis? ANISSA ABI-DARGHAM. Int. J. Neuropsychoparm. (2004) 7, Supp S1-S5

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