GABAPENTIN ENCARBIL

Clinical safety rating: safe

Antacids decrease absorption May cause somnolence dizziness and respiratory depression especially with opioids.

How it works

Gabapentin encarbil is a prodrug of gabapentin, which binds to the alpha-2-delta subunit of voltage-gated calcium channels in the central nervous system, reducing calcium influx and inhibiting neurotransmitter release.

What the body does with it

Metabolism	Gabapentin encarbil is rapidly hydrolyzed by non-specific esterases in the gastrointestinal tract to gabapentin. Gabapentin is not significantly metabolized and is excreted unchanged in urine.
Excretion	Renal: Gabapentin encarbil is a prodrug of gabapentin. Following absorption, it is rapidly hydrolyzed to gabapentin. Gabapentin is primarily excreted unchanged in urine via glomerular filtration. Approximately 80-90% of a dose is recovered in urine as gabapentin, with the remainder as metabolites and minor amounts (≤1%) in feces. Biliary excretion is negligible.
Half-life	The terminal elimination half-life of gabapentin derived from gabapentin encarbil is approximately 5-7 hours in patients with normal renal function. This half-life is prolonged in patients with renal impairment (up to 132 hours in anuria). Clinically, steady-state concentrations are achieved within 1-2 days. Twice-daily dosing is effective due to sustained exposure from the prodrug formulation.
Protein binding	Gabapentin is less than 3% bound to plasma proteins. The binding proteins are albumin and α1-acid glycoprotein, but the low binding indicates that protein binding interactions are not clinically relevant.
Volume of Distribution	The volume of distribution (Vd) of gabapentin is approximately 0.6-0.8 L/kg. This indicates distribution into total body water and some peripheral tissues. In patients with normal renal function, the Vd is not significantly altered, but in renal impairment, the Vd may decrease due to reduced tissue perfusion.
Bioavailability	Oral bioavailability of gabapentin from gabapentin encarbil is approximately 100% relative to gabapentin tablets. The prodrug is designed to be absorbed via monocarboxylate transporter type 1 (MCT-1) and sodium-dependent multivitamin transporter (SMVT) in the intestine, avoiding the saturable absorption of gabapentin. Thus, bioavailability is high and dose-proportional over the therapeutic range.
Onset of Action	Oral administration: Time to peak plasma concentration (Tmax) of gabapentin is approximately 1 hour (range 0.5-3 hours) following gabapentin encarbil. Clinical onset for analgesic effect (e.g., postherpetic neuralgia) may be observed within the first week of therapy, but maximum effect may require 2-4 weeks.
Duration of Action	Duration of action for pain relief is approximately 12 hours, supporting twice-daily dosing. The extended pharmacodynamic effect is related to gabapentin's binding to the α2δ subunit of voltage-gated calcium channels, which modulates neurotransmitter release. Clinically, dosing is every 12 hours for pain indications.

Classification & Brands

Dosing & administration

Oral gabapentin encarbil 600 mg once daily with evening meal, titrated based on response and tolerability, maximum 1200 mg once daily. Alternatively, 600 mg twice daily may be used; maximum 2400 mg/day.

Dosage form	TABLET, EXTENDED RELEASE
Renal impairment	For CrCl ≥60 mL/min: no adjustment. CrCl 30-59: 600 mg once daily; CrCl 15-29: 300 mg once daily; CrCl <15: not recommended; hemodialysis: 300 mg after each dialysis session.
Liver impairment	No dose adjustment recommended for mild to moderate hepatic impairment (Child-Pugh A or B). Not studied in severe impairment (Child-Pugh C); use with caution.
Pediatric use	Approved for partial-onset seizures in patients ≥3 years: starting dose 10-15 mg/kg/day divided 3 times daily, titrate to effective dose (usual range 25-50 mg/kg/day, max 60 mg/kg/day). For gabapentin encarbil, pediatric dosing not established.
Geriatric use	Initiate at lower end of dosing range due to age-related renal function decline. Monitor for sedation, dizziness, and falls. Adjust based on creatinine clearance.

Use during pregnancy

1st trimester	Consult provider
2nd trimester	Consult provider
3rd trimester	Consult provider

Clinical note

Antacids decrease absorption May cause somnolence dizziness and respiratory depression especially with opioids.

FDA category

Animal

Breastfeeding

Gabapentin is excreted into breast milk, with a milk-to-plasma ratio of approximately 1.0 based on gabapentin data. The infant dose is estimated to be about 1-2% of the maternal weight-adjusted dose. No adverse effects have been reported in breastfed infants, but theoretical risks of sedation and poor suckling exist. Use with caution, monitoring the infant for drowsiness and adequate weight gain. The M/P ratio for gabapentin encarbil itself is not established, but it is rapidly converted to gabapentin.

Warnings & precautions

■ FDA Black Box Warning

No FDA black box warning.

Side Effect Profile

Common Effects	neuropathic pain
Serious Effects

Absolute Contraindications

None known for gabapentin encarbil; however, hypersensitivity to gabapentin or any component of the formulation is a contraindication.

Clinical Precautions

Precautions

["May cause dizziness, somnolence, and syncope; caution with concomitant CNS depressants","Renal impairment may alter drug clearance; dose adjustment required","Potential for abuse and dependence; monitor for signs of misuse","Serious skin reactions (e.g., DRESS, Stevens-Johnson syndrome) reported"]

Clinical Tips & Counseling

Drug interactions

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GABAPENTIN ENCARBIL

Clinical safety rating: safe

Antacids decrease absorption May cause somnolence dizziness and respiratory depression especially with opioids.

How it works

What the body does with it

Metabolism	Gabapentin encarbil is rapidly hydrolyzed by non-specific esterases in the gastrointestinal tract to gabapentin. Gabapentin is not significantly metabolized and is excreted unchanged in urine.
Excretion	Renal: Gabapentin encarbil is a prodrug of gabapentin. Following absorption, it is rapidly hydrolyzed to gabapentin. Gabapentin is primarily excreted unchanged in urine via glomerular filtration. Approximately 80-90% of a dose is recovered in urine as gabapentin, with the remainder as metabolites and minor amounts (≤1%) in feces. Biliary excretion is negligible.
Half-life	The terminal elimination half-life of gabapentin derived from gabapentin encarbil is approximately 5-7 hours in patients with normal renal function. This half-life is prolonged in patients with renal impairment (up to 132 hours in anuria). Clinically, steady-state concentrations are achieved within 1-2 days. Twice-daily dosing is effective due to sustained exposure from the prodrug formulation.
Protein binding	Gabapentin is less than 3% bound to plasma proteins. The binding proteins are albumin and α1-acid glycoprotein, but the low binding indicates that protein binding interactions are not clinically relevant.
Volume of Distribution	The volume of distribution (Vd) of gabapentin is approximately 0.6-0.8 L/kg. This indicates distribution into total body water and some peripheral tissues. In patients with normal renal function, the Vd is not significantly altered, but in renal impairment, the Vd may decrease due to reduced tissue perfusion.
Bioavailability	Oral bioavailability of gabapentin from gabapentin encarbil is approximately 100% relative to gabapentin tablets. The prodrug is designed to be absorbed via monocarboxylate transporter type 1 (MCT-1) and sodium-dependent multivitamin transporter (SMVT) in the intestine, avoiding the saturable absorption of gabapentin. Thus, bioavailability is high and dose-proportional over the therapeutic range.
Onset of Action	Oral administration: Time to peak plasma concentration (Tmax) of gabapentin is approximately 1 hour (range 0.5-3 hours) following gabapentin encarbil. Clinical onset for analgesic effect (e.g., postherpetic neuralgia) may be observed within the first week of therapy, but maximum effect may require 2-4 weeks.
Duration of Action	Duration of action for pain relief is approximately 12 hours, supporting twice-daily dosing. The extended pharmacodynamic effect is related to gabapentin's binding to the α2δ subunit of voltage-gated calcium channels, which modulates neurotransmitter release. Clinically, dosing is every 12 hours for pain indications.

Classification & Brands

Dosing & administration

Dosage form	TABLET, EXTENDED RELEASE
Renal impairment	For CrCl ≥60 mL/min: no adjustment. CrCl 30-59: 600 mg once daily; CrCl 15-29: 300 mg once daily; CrCl <15: not recommended; hemodialysis: 300 mg after each dialysis session.
Liver impairment	No dose adjustment recommended for mild to moderate hepatic impairment (Child-Pugh A or B). Not studied in severe impairment (Child-Pugh C); use with caution.
Pediatric use	Approved for partial-onset seizures in patients ≥3 years: starting dose 10-15 mg/kg/day divided 3 times daily, titrate to effective dose (usual range 25-50 mg/kg/day, max 60 mg/kg/day). For gabapentin encarbil, pediatric dosing not established.
Geriatric use	Initiate at lower end of dosing range due to age-related renal function decline. Monitor for sedation, dizziness, and falls. Adjust based on creatinine clearance.

Use during pregnancy

1st trimester	Consult provider
2nd trimester	Consult provider
3rd trimester	Consult provider

Clinical note

Antacids decrease absorption May cause somnolence dizziness and respiratory depression especially with opioids.

FDA category

Animal

Breastfeeding

Warnings & precautions

■ FDA Black Box Warning

No FDA black box warning.

Side Effect Profile

Common Effects	neuropathic pain
Serious Effects

Absolute Contraindications

None known for gabapentin encarbil; however, hypersensitivity to gabapentin or any component of the formulation is a contraindication.