Lamotrigine Er

Lamotrigine is a phenyltriazine-class anti-epileptic agent and mood stabilizer used to treat various types of seizures and delay the recurrence of mood episodes in patients with Bipolar I Disorder. It works by stabilizing neuronal membranes via sodium channel inhibition.

Dosage for lamotrigine is highly individualized and depends strictly on whether the patient is taking concurrent medications that affect its metabolism. A "slow and low" titration (gradual increase) is mandatory to minimize the risk of serious skin rashes.

• Bipolar I Disorder Maintenance: The standard target dose is 200 mg daily. For patients not taking enzyme-inducing or inhibiting drugs, the typical titration starts at 25 mg daily for weeks 1 and 2, followed by 50 mg daily for weeks 3 and 4, then 100 mg for week 5, reaching the 200 mg maintenance dose by week 6.
• Epilepsy (Adjunctive Therapy): The target dose ranges from 100 mg to 500 mg daily, often divided into two doses. If combined with valproate, the starting dose is significantly lower (12.5 mg to 25 mg every other day).
• Epilepsy (Monotherapy): The maintenance target is typically 500 mg daily, achieved through a multi-week titration schedule.

Lamotrigine is approved for children as young as 2 years for certain types of epilepsy. Dosing is strictly weight-based (mg/kg). For example, in children taking valproate, the starting dose may be as low as 0.15 mg/kg/day. Pediatric patients must be monitored closely by a specialist, as the risk of rash is statistically higher in children than in adults.

Renal Impairment

In patients with significant renal impairment (reduced kidney function), the initial dose of lamotrigine may not need adjustment, but the maintenance dose should generally be reduced. Because lamotrigine and its metabolites are cleared by the kidneys, reduced clearance can lead to drug accumulation. Healthcare providers typically reduce the maintenance dose by 25% to 50% in cases of moderate to severe renal failure.

Hepatic Impairment

For patients with moderate hepatic impairment (Child-Pugh Grade B), doses should be reduced by approximately 25%. In severe hepatic impairment (Child-Pugh Grade C), the dose should be reduced by 50%. The liver is the primary site of glucuronidation, so impaired liver function directly increases the circulating levels of the drug.

Elderly Patients

While no specific age-based dosage adjustment is universally required, clinicians often start at the lower end of the dosing range for elderly patients. This population is more susceptible to balance issues (ataxia) and cognitive side effects, and they often have age-related declines in renal or hepatic function.

• Consistency: Take lamotrigine at the same time every day to maintain stable blood levels. It can be taken with or without food.
• Swallowing: Immediate-release and extended-release tablets must be swallowed whole. Do not crush, chew, or break them, as this can interfere with the controlled release of the medication or cause a bitter taste.
• Chewable Tablets: These can be swallowed whole, chewed, or dispersed in a small amount of water or diluted fruit juice.
• ODT Tablets: Place on the tongue and allow to dissolve; they can be swallowed with or without water.
• Storage: Store at room temperature (68°F to 77°F) in a dry place away from light and moisture.

If you miss a dose, take it as soon as you remember. However, if it is almost time for your next scheduled dose, skip the missed dose and return to your regular schedule. Never take two doses at once to make up for a missed one. If you miss more than a few days of lamotrigine, do not restart at your previous dose. You must contact your doctor immediately, as you may need to restart the titration process from the lowest dose to avoid the risk of a serious rash.

Signs of a lamotrigine overdose may include ataxia (lack of muscle coordination), nystagmus (involuntary eye movement), increased seizures, coma, or heart rhythm abnormalities (intraventricular conduction delay). In the event of a suspected overdose, contact emergency services or a poison control center immediately. Emergency treatment usually involves supportive care and gastric lavage if the ingestion was recent.

> Important: Follow your healthcare provider's dosing instructions exactly. Do not adjust your dose or stop the medication without medical guidance, as sudden discontinuation can trigger seizures.

Most patients tolerate lamotrigine well, but common side effects can occur, particularly during the titration phase. These usually diminish as the body adjusts to the medication:

• Dizziness and Ataxia: A feeling of lightheadedness or being unsteady on your feet. This is one of the most frequently reported side effects.
• Headache: Often mild to moderate, occurring shortly after starting the medication.
• Somnolence (Drowsiness): While less sedating than other AEDs, some patients feel fatigued or sleepy.
• Nausea and Vomiting: Gastrointestinal upset is common but can often be mitigated by taking the drug with food.
• Diplopia (Double Vision)

Lamotrigine is a high-alert medication because of the potential for severe dermatological and immunological reactions. Patients must be educated on the "titration schedule"—the process of slowly increasing the dose. Skipping doses or restarting at a high dose after a break can be fatal due to the risk of Stevens-Johnson Syndrome.

FDA Black Box Warning Summary: Lamotrigine can cause serious, life-threatening rashes, including Stevens-Johnson Syndrome (SJS) and Toxic Epidermal Necrolysis (TEN). These rashes usually require hospitalization and discontinuation of the drug. The risk is highest in children and in those taking valproate or exceeding the recommended titration schedule. While benign rashes also occur, it is impossible to predict which rashes will become life-threatening. Therefore, the drug should ordinarily be discontinued at the first sign of a rash unless the rash is clearly not drug-related.

• Allergic Reactions / Anaphylaxis

There are few absolute contraindications for lamotrigine combinations, but use with other drugs that cause severe QT prolongation or those that have a high cross-sensitivity for SJS (like certain other AEDs) requires extreme caution. The most critical "do not use" scenario is restarting lamotrigine at a high dose after a treatment gap without a new titration.

• Valproate (Depakene, Depakote): This is the most significant interaction. Valproate inhibits the glucuronidation of lamotrigine, effectively doubling its concentration in the blood. This dramatically increases the risk of life-threatening rashes. The lamotrigine dose must be reduced by more than 50% when used with valproate.
• Enzyme Inducers (Carbamazepine, Phenytoin, Phenobarbital, Rifampin): These drugs speed up the metabolism of lamotrigine, reducing its blood levels by approximately 40-50%. This can lead to a loss of seizure control or a return of bipolar symptoms. Higher doses of lamotrigine are usually required.

Lamotrigine must NEVER be used in the following circumstances:

• Hypersensitivity: If a patient has a known history of hypersensitivity (severe allergy) to lamotrigine or any of the inactive ingredients in the tablet (such as lactose or magnesium stearate). A previous history of a lamotrigine-induced rash is an absolute contraindication to restarting the drug, as a second exposure can lead to a faster and more severe reaction.
• Severe SJS/TEN History: Patients who have experienced Stevens-Johnson Syndrome or Toxic Epidermal Necrolysis from any medication should be treated with extreme caution, and lamotrigine is generally avoided due to the high risk of cross-reactivity.

These are conditions where the benefit must clearly outweigh the risk, and intensive monitoring is required:

Lamotrigine is often considered one of the safer anti-epileptic drugs during pregnancy, but it is not without risks. It is classified as Pregnancy Category C (under the old system).

• Teratogenicity: Large pregnancy registries (like the North American Antiepileptic Drug Pregnancy Registry) suggest that lamotrigine does not significantly increase the risk of major malformations (like cleft lip/palate) compared to the general population, especially when compared to valproate.
• Physiological Changes: During pregnancy, the body clears lamotrigine much faster (up to 50-100% faster). This can lead to a drop in blood levels and a breakthrough seizure, which can be dangerous for both the mother and the fetus. Doses usually need to be increased during pregnancy and then rapidly decreased after delivery.

Lamotrigine passes into breast milk in significant amounts. The milk-to-plasma ratio is approximately 0.6. While many infants do not show adverse effects, there is a risk of the infant developing a rash or experiencing breathing problems (apnea). If breastfeeding, the infant must be monitored closely for any skin changes, drowsiness, or poor feeding. The decision to breastfeed should be a shared decision between the mother, neurologist, and pediatrician.

Lamotrigine's primary mechanism is the inhibition of voltage-gated sodium channels. It binds specifically to the inactive state of the channel, which prevents the rapid, repetitive firing of action potentials in neurons. This action is "use-dependent," meaning it targets overactive neurons while sparing normal neuronal activity. Additionally, lamotrigine inhibits the presynaptic release of glutamate, the brain's main excitatory neurotransmitter. By reducing glutamate-mediated excitability, it prevents the initiation and spread of seizure activity and stabilizes the mood fluctuations seen in Bipolar I Disorder.

Lamotrigine shows a clear dose-response relationship for both its therapeutic effects and its side effects. The onset of action for epilepsy can be seen within 1-2 weeks of reaching a therapeutic dose, but for Bipolar Disorder, the full prophylactic effect may not be evident for several weeks or months. Tolerance to the anticonvulsant effects is rarely reported, making it suitable for long-term maintenance therapy.

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