Difference between revisions of "Treatment - Pharmacotherapy Overview"
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| − | + | ===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, 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 | + | :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=== | ||
| − | + | :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 | |
| − | |||
| − | |||
| − | |||
| − | • 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
