Difference between revisions of "Treatment - Pharmacotherapy Overview"

(Created page with "Pharmacotherapy consists of the decision to start an agent or to refrain for the time being. While important to consider adding a medication, it is equally as important to con...")
 
(Mood stabilizers)
 
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1) Antidepressants
+
===Antidepressants===
  
a. SSRIs – generally equivalent in efficacy
+
:a. SSRIs – generally equivalent in efficacy
  
• paroxetine is avoided due to anticholinergic burden and medication interactions
+
::• paroxetine is avoided due to anticholinergic burden and medication interactions
  
• fluoxetine is helpful to avoid withdrawal in patients with nonadherence due to its long half-life
+
::• fluoxetine is helpful to avoid withdrawal in patients with nonadherence due to its long half-life
  
• fluvoxamine has been studied to be effective in patients with OCD
+
::• fluvoxamine has been studied to be effective in patients with OCD
  
b. SNRIs – if SSRI trials are failed, may consider SNRI. If there is an element of chronic pain, consider duloxetine
 
  
c. DNRI (bupropion) good to consider if there is an element of inattention / fatigue due to the dopaminergic quality, avoid in patients with seizure disorders
+
:b. SNRIs if SSRI trials are failed, may consider SNRI. If there is an element of chronic pain, consider duloxetine
  
d. TCAs this category has greater anticholinergic burden, though nortriptyline and amitriptyline may be helpful in patients with chronic headaches; clomipramine has been studied to be effective in patients with OCD
+
:c. DNRI (bupropion) good to consider if there is an element of inattention / fatigue, or if the patient is interested in the treatment of nicotine use disorder, due to the dopaminergic quality of bupropion, avoid in patients with seizure disorders, and eating disorder
  
e. MAOIs generally avoided due to diet restrictions and medication interactions
+
:d. TCAs this category has greater anticholinergic burden, though nortriptyline and amitriptyline may be helpful in patients with chronic headaches; clomipramine has been studied to be effective in patients with OCD
  
 +
:e. MAOIs – generally avoided due to diet restrictions and medication interactions
  
2) Anxiolytics
+
===Anxiolytics===
  
a. SSRIs and SNRIs – as above
+
:a. SSRIs and SNRIs – as above
  
b. Buspirone – low side-effect profile, can be taken three times a day
+
:b. Buspirone – low side-effect profile, can be taken three times a day
  
c. Benzodiazepines – helpful in short-term treatment of anxiety, but generally should be tapered off due to dyscognitive side-effects, increased fall risk, and generally ineffective for long-term use
+
:c. [[Benzodiazepines]] – helpful in short-term treatment of anxiety, but generally should be tapered off due to dyscognitive side-effects, increased fall risk, and generally ineffective for long-term use
  
d. Antiadrenergics – may be a good option for anxiety and agitation in TBI patients, caution in patients with lower blood pressure or bradycardia
+
:d. Antiadrenergics – may be a good option for anxiety and agitation in TBI patients, caution in patients with lower blood pressure or bradycardia
  
• Beta-blockers – propranolol can be used TID and eventually consolidated into once a day long-acting medication
+
::• Beta-blockers – propranolol can be used TID and eventually consolidated into once a day long-acting medication
  
• Clonidine
+
::• Clonidine
  
• Prazosin – helpful to treat PTSD associated nightmares
+
::• Prazosin – helpful to treat PTSD associated nightmares
  
 +
===Mood stabilizers===
  
3) Mood stabilizers
+
:a. Lamotrigine – slow titration to avoid Stevens-Johnson Syndrome, though beneficial for bipolar depression
  
a. Lamotrigine slow titration to avoid Steven Johnson Syndrome, though beneficial for bipolar depression
+
:b. Lithium – beneficial for both control of mania and depression in bipolar disorder, though many side effects (weight gain, polydipsia/polyuria, thyroid dysfunction, neuropathy, tremors, extrapyramidal side effects, acne, alopecia), requires blood serum monitoring
  
b. Lithium – beneficial for both control of mania and depression in bipolar disorder, though many side effects (weight gain, polydipsia/polyuria, thyroid dysfunction), requires blood serum monitoring
+
:c. Valproic acid – beneficial for control of mania or in agitation; not helpful for depression, should be avoided in women of childbearing age
  
c. Valproic acid – beneficial for control of mania or in agitation; not helpful for depression, should not be given to women of childbearing age
+
:d. Carbamazepine – beneficial for control of mania; not helpful for depression, many medication interactions, should not be given to women of childbearing age
  
d. Carbamazepine beneficial for control of mania; not helpful for depression, many medication interactions, should not be given to women of childbearing age
+
:e. Antipsychotics have mood stabilizing properties
  
e. Antipsychotics – have mood stabilizing properties
+
===Antipsychotics===
  
 +
:a. First generation – acts on dopamine
  
4) Antipsychotics
+
:b. Second generation – acts on dopamine and serotonin
  
a. First generation – acts on dopamine
+
::• Quetiapine favored by neurologists due to low dopaminergic component, however, to reach dopaminergic effects and benefit antipsychotic properties, typically doses of 400mg+ is required. It has not been shown to be effective in controlling psychosis in Parkinson disease or agitation in dementia. Also beneficial for bipolar depression
  
b. Second generation – acts on dopamine and serotonin
+
::• Clozapine is more effective in controlling psychotic symptoms though it requires weekly blood draws to monitor for possible blood dyscrasia; it also has the worst side-effect profile regarding weight gain and metabolic effects.
  
Quetiapine favored by neurologists due to low dopaminergic component, however, to reach dopaminergic effects and benefit antipsychotic properties, typically doses of 400mg+ is required. It has not been shown to be effective in controlling psychosis in Parkinson disease or agitation in dementia. Also beneficial for bipolar depression
+
::Pimavanserin – no dopaminergic qualities, has been approved for treatment of [[Parkinson's disease psychosis]]
  
Clozapine is more effective in controlling psychotic symptoms though it requires weekly blood draws to monitor for possible blood dyscrasia; it also has the worst side-effect profile regarding weight gain and metabolic effects.
+
::Lurasidone - shown to be beneficial for bipolar depression
  
• Pimavanserin – no dopaminergic qualities, has been approved for treatment of Parkinson psychosis
+
::• Aripiprazole – partial agonist; shown to be beneficial as a potential augmenting agent for depressive disorder, long half-life
 
 
• Lurasidone - shown to be beneficial for bipolar depression
 
 
 
• Aripiprazole – partial agonist; shown to be beneficial as a potential augmenting agent for depressive disorder, long half-life
 

Latest revision as of 15:05, 5 August 2022

Pharmacotherapy consists of the decision to start an agent or to refrain for the time being. While important to consider adding a medication, it is equally as important to consider reducing medication that is either ineffective or potentially causing adverse effects.


Antidepressants

a. SSRIs – generally equivalent in efficacy
• paroxetine is avoided due to anticholinergic burden and medication interactions
• fluoxetine is helpful to avoid withdrawal in patients with nonadherence due to its long half-life
• fluvoxamine has been studied to be effective in patients with OCD


b. SNRIs – if SSRI trials are failed, may consider SNRI. If there is an element of chronic pain, consider duloxetine
c. DNRI (bupropion) – good to consider if there is an element of inattention / fatigue, or if the patient is interested in the treatment of nicotine use disorder, due to the dopaminergic quality of bupropion, avoid in patients with seizure disorders, and eating disorder
d. TCAs – this category has greater anticholinergic burden, though nortriptyline and amitriptyline may be helpful in patients with chronic headaches; clomipramine has been studied to be effective in patients with OCD
e. MAOIs – generally avoided due to diet restrictions and medication interactions

Anxiolytics

a. SSRIs and SNRIs – as above
b. Buspirone – low side-effect profile, can be taken three times a day
c. Benzodiazepines – helpful in short-term treatment of anxiety, but generally should be tapered off due to dyscognitive side-effects, increased fall risk, and generally ineffective for long-term use
d. Antiadrenergics – may be a good option for anxiety and agitation in TBI patients, caution in patients with lower blood pressure or bradycardia
• Beta-blockers – propranolol can be used TID and eventually consolidated into once a day long-acting medication
• Clonidine
• Prazosin – helpful to treat PTSD associated nightmares

Mood stabilizers

a. Lamotrigine – slow titration to avoid Stevens-Johnson Syndrome, though beneficial for bipolar depression
b. Lithium – beneficial for both control of mania and depression in bipolar disorder, though many side effects (weight gain, polydipsia/polyuria, thyroid dysfunction, neuropathy, tremors, extrapyramidal side effects, acne, alopecia), requires blood serum monitoring
c. Valproic acid – beneficial for control of mania or in agitation; not helpful for depression, should be avoided in women of childbearing age
d. Carbamazepine – beneficial for control of mania; not helpful for depression, many medication interactions, should not be given to women of childbearing age
e. Antipsychotics – have mood stabilizing properties

Antipsychotics

a. First generation – acts on dopamine
b. Second generation – acts on dopamine and serotonin
• Quetiapine favored by neurologists due to low dopaminergic component, however, to reach dopaminergic effects and benefit antipsychotic properties, typically doses of 400mg+ is required. It has not been shown to be effective in controlling psychosis in Parkinson disease or agitation in dementia. Also beneficial for bipolar depression
• Clozapine is more effective in controlling psychotic symptoms though it requires weekly blood draws to monitor for possible blood dyscrasia; it also has the worst side-effect profile regarding weight gain and metabolic effects.
• Pimavanserin – no dopaminergic qualities, has been approved for treatment of Parkinson's disease psychosis
• Lurasidone - shown to be beneficial for bipolar depression
• Aripiprazole – partial agonist; shown to be beneficial as a potential augmenting agent for depressive disorder, long half-life