Primidone: Difference between revisions

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{{MedTemplate

| generic = Primidone

| brand = Mysoline

| structure =

| classes = Barbiturate, ~~Anticonvulsant~~

| classes = [[:Category:Anticonvulsants|Anticonvulsant]], [[:Category:Barbiturates|Barbiturate (parent compound)]], [[:Category:Tremor medicines|Tremor medicine]]

| ~~mechanism = Metabolized to phenobarbital; sodium channel modulator~~

| uses = <vote slug="partial-seizures-monotherapy-use">Partial-onset and generalized tonic-clonic seizures (FDA)</vote>, <vote slug="essential-tremor-use">Essential tremor (widely used and AAN-guideline-supported as first-line alongside propranolol)</vote>

| uses =

| starting_dose = Seizures: 100-125 mg PO at bedtime x 3 days, then BID, then TID, escalating to 750-1500 mg/day. Essential tremor: 25-50 mg PO at bedtime, titrate slowly to 250-750 mg/day

| starting_dose =

| preparations = Tablets 50, 250 mg

| preparations =

| fda_max = 2 g/day (seizures); typically much lower for essential tremor

| fda_max =

| pill_id =

| routes =

| routes = Oral

| onset =

| onset = Anticonvulsant effect emerges with slow titration over weeks; tremor effect over weeks

| duration =

| duration = BID-TID dosing

| halflife =

| halflife = Primidone 5-15 hours; '''phenobarbital active metabolite 50-150 hours'''; PEMA (phenylethylmalonamide) active metabolite 16 hours<ref name="mysoline-label">FDA Prescribing Information, Mysoline (primidone), Bausch/various, current revision. https://www.accessdata.fda.gov/drugsatfda_docs/label/2010/009170s032lbl.pdf</ref>

~~| bioavailability =~~

| bioavailability = ~90% (oral)<ref name="mysoline-label" />

~~| pregnancy~~ =

| pregnancy = Substantial teratogenic signal (barbiturate class effects including neonatal withdrawal and hemorrhagic disease of newborn).{{citation needed}}

~~| legal~~ =

| legal = [[USLegal:Prescription only|Rx-only]] in US. '''Federally non-controlled despite being a barbiturate''', a paradoxical situation given that its primary active metabolite phenobarbital is Schedule IV<ref name="mysoline-label" />

| ~~intro =~~

| mechanism = <vote slug="primidone-mech-claim">Barbiturate that metabolizes to two active species: '''phenobarbital''' (the major contributor to seizure control, mediating GABA-A receptor potentiation) and '''PEMA (phenylethylmalonamide)''', which contributes to seizure control and is the leading candidate to explain the essential-tremor efficacy. Phenobarbital alone does not reliably suppress tremor at non-sedating doses, so PEMA's independent action is the proposed mechanism for the tremor indication.</vote> Strong CYP3A4 induction via the phenobarbital metabolite produces many interactions (reduces oral contraceptives, warfarin, many psychotropics). Essential-tremor efficacy is the unique pharmacological selling point<ref name="mysoline-label" />.

~~| pharmacokinetics~~ =

~~| pharmacodynamics~~ =

| ~~indications~~ =

| ~~dosing~~ =

~~| effects =~~

| ~~interactions~~ = ~~<pharmaInteractions~~/>

| ~~pregnancy_details =~~

~~| monitoring~~ =

~~| counseling~~ =

~~| anecdotes =~~

~~| seealso =~~

~~| references~~ =

}}

== References ==

[[Category:~~Stimulants & Wake-Promoting Agents~~]]

[[Category:Anticonvulsants]]

[[Category:Barbiturates]]

[[Category:~~Sedative-Hypnotics]]~~

[[Category:Tremor medicines]]

~~[[Category:Anticonvulsants / Antiepileptics~~]]

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