Adult Dosing

Lennox-Gastaut syndrome (LGS)

• 30 kg: 5 mg daily and titrate as tolerated up to 20 mg daily
• >30 kg: 10 mg daily and titrate as tolerated up to 40 mg daily

Pediatric Dosing

Epilepsy, adjunctive

Child

• > 2 years, 30 kg: 5 mg daily and titrate as tolerated up to 20 mg daily
• > 2 years, >30 kg: 10 mg daily and titrate as tolerated up to 40 mg daily
• Max: 40 mg/day

[Outline]

• Adult Dosing
• Pediatric Dosing

• Adjunctive treatment of seizures associated with Lennox-Gastaut syndrome (LGS) in patients 2 years of age or older

• Hypersensitivity to any of the ingredients of the product
• Avoid abrupt withdrawal

• N/A

Renal Dose Adjustment

• Renal impairment: Reduce dose; amount not defined

Hepatic Dose Adjustment

• Mild-moderate hepatic impairment:
• Child-Pugh Class A or B: start 5 mg PO qd x1wk, then 5 mg PO bid x1wk, then 10 mg PO bid
• Child-Pugh Class C: not defined
• Severe hepatic impairment: Contraindicated

• Clobazam may induce somnolence and sedation particularly with concomitant use of other central nervous system depressants
• Clobazam may potentiate sedation from concomitant use with central nervous system depressants
• Abrupt discontinuation of clobazam should be avoided.Dose should be tapered by decreasing the dose every week by 5-10 mg/day until discontinuation
• Clobazam should not be given with antiepileptic drugs to minimize the risk of precipitating seizures, seizure exacerbation, or status epilepticus
• Patients with a history of substance abuse should be under careful surveillance when receiving clobazam or other psychotropic agents because of the predisposition of such patients to habituation and dependence
• Clobazam increases the risk of suicidal thoughts thus such patients should be monitored for worsening of depression, suicidal thoughts or behavior, and/or any unusual changes in mood or behavior
• Serious skin reactions including Stevens-Johnson syndrome, toxic epidermal necrolysis reported in both children and adults; monitor carefully for signs or symptoms, especially during the first 8 weeks of treatment initiation or when re-introducing therapy; discontinue at the first sign of drug related rash and do not resume

Cautions: Use cautiously in

• Renal impairment
• Hepatic impairment
• Hypotension
• CNS depressant use
• Psychosis
• Suicidal ideation
• Alcohol abuse
• Elderly population

Onfi interacts with :

	Abilify
	Abilify discmelt
	Abilify Maintena
	Amitriptyline
	Amoxapine
	Anafranil
	Aripiprazole
	Asendin
	Aventyl Hydrochloride
	Betimol
	Blocadren
	Brexpiprazole
	Bystolic
	Carvedilol
	Cerdelga
	Clomipramine
	Clozapine
	Clozaril
	Codeine
	Coreg
	Coreg CR
	Desipramine
	Dihydrocodeine
	Doxepin
	Elavil
	Eliglustat
	Fanapt
	Fazaclo ODT
	Flecainide
	Hemangeol
	Hydrocodone
	Iloperidone
	Imipramine
	Inderal
	Inderal LA
	Innopran XL
	Invega
	Invega Sustenna
	Istalol
	Lopressor
	Lortab
	Mellaril
	Metoclopramide
	Metoprolol
	Metozolv ODT
	Mexiletine
	Mexitil
	Nebivolol
	Nolvadex
	Norpramin
	Nortriptyline
	Olanzapine
	Oxecta
	Oxycodone
	Oxycontin
	OxyFast
	Paliperidone
	Pamelor
	Percocet
	Percodan
	Perphenazine
	Propafenone
	Propranolol
	Protriptyline
	Reglan
	Rexulti
	Risperdal
	Risperdal Consta
	Risperdal M-Tab
	Risperidone
	Roxicodone
	Rythmol
	Rythmol SR
	Silenor
	Sinequan
	Soltamox
	Surmontil
	Synalgos-DC
	Tambocor
	Tamoxifen
	Thioridazine
	Timolol
	Timoptic
	Timoptic in ocudose
	Timoptic-XE
	Tofranil
	Tofranil-PM
	Toprol-XL
	Trilafon
	Trimipramine
	Versacloz
	Vicodin
	Vivactil
	Zohydro ER
	Zonalon
	Zyprexa
	Zyprexa Relprevv
	Zyprexa Zydis

Pregnancy Category: c

Breastfeeding: Limited information indicates that maternal doses of clobazam up to 30 mg daily produce low levels in milk. Short-term use would not be expected to cause any adverse effects in breastfed infants, especially if the infant is older than 2 months. During long-term administration, monitor the infant for possible sedation and poor sucking.This information is based upon Lactmed database (available at http://toxnet.nlm.nih.gov/cgi-bin/sis/htmlgen?LACT last accessed 24 June 2013)

• CNS: Somnolence, sedation, withdrawal symptoms, physical and psychological dependence, suicidal behavior and ideation, lethargy, drooling, ataxia, psychomotor hyperactivity, dysarthria
• PSYCHIATRY: Aggresion
• RESP: Upper respiratory tract infections, pneumonia, bronchitis
• HEMA: Anemia, leukopenia, thrombocytopenia, cough
• GU:Urinary tract infection
• GI: Vomiting, constipation, dysphagia, decreased appetite
• MISC: Physical and/or psychological dependence, withdrawal or rebound phenomena (on discontinuation)

• Benzodiazepine; binds to benzodiazepine receptors; enhances GABA effects; potentiates GABA-ergic transmission at the level of spinal cord, hypothalamus, hippocampus, substantia nigra, cerebellar cortex and cerebral cortex
• Rapidly and extensively absorbed following oral administration
• Metabolized by liver; active metabolite: N-desmethyl clobazam
• Renally excreted: 87 % approximately 2% of the dose recovered in urine and 1% in feces as unchanged drug
• Half-life: 36-42 hours (clobazam), 71-82 hours (active metabolite N­-desmethylclobazam)

US Trade Name(s)

• Onfi

US Availability

Onfi

• TABS: 10, 20 mg
• SUSP: 2.5 mg/ml

Canadian Trade Name(s)

• Frisium

Canadian Availability

clobazam (generic)

• TABS: 10 mg

Frisium

• TABS: 10 mg

UK Trade Name(s)

• Frisium

UK Availability

clobazam (generic)

• TABS: 10 mg

Frisium

• TABS: 10 mg

Australian Trade Name(s)

• Frisium

Australian Availability

Frisium

• TABS: 10 mg

[Outline]

Neurologic

Anticonvulsants

Benzodiazepines