This study evaluated the efficacy and safety of lacosamide in treating diabetic neuropathic pain through an 18-week double-blind trial of 370 patients with doses of 200 mg/day, 400 mg/day, and 600 mg/day compared to a placebo. The 400 mg/day dose was found to significantly improve pain scores over the placebo and had the optimal balance of efficacy and side effects. Common side effects included dizziness, tremor and headache. While lacosamide showed potential for treating diabetic neuropathic pain, the study period was short and the 600 mg/day group had a high withdrawal rate due to adverse events.
2. “EFFICACY & SAFETY OF LACOSAMIDE IN DIABETIC
NEUROPATHIC PAIN: AN 18-WEEK DOUBLE-BLIND,
PLACEBO-CONTROLLED TRIAL OF FIXED DOSE
REGIMENS”
3. The article was published in “Clin J Pain”, 2009
Article was received on: June 17, 2008
Article was accepted on: November 23, 2008
4. 1. James. P. Wymer, MD, PhD, Upstate Clinical Research, Albany, New York
2. Jeffrey Simpson, PhD, Schwarz Biosciences Inc, a member of the UCB Group,
Research Triangle Park, NC
3. David Sen, PhD, Schwarz Biosciences Inc, a member of the UCB Group,
Research Triangle Park, NC
4. Sabine Bongardt, MS, Schwarz Biosciences GmbH, a member of the UCB
Group, Monheim, Germany.
5. Painful distal diabetic neuropathy is one of the most common form of chronic
neuropathic pain
Affects approximately 30% of patients with DM
Pain is described as a steady, aching or burning pain, & characterized by
hyperalgesia, allodynia & paresthesia
Treatment of PDN is extremely difficult
Lacosamide is an investigational drug, being investigated for the treatment of
neuropathic pain & epilepsy
Lacosamide has minimal PPB, & minimal risks for drug-drug interaction, which
makes it a safer alternative for patients with neuropathic pain, on multiple
concomitant medications.
6. A. STUDY DESIGN: Randomized, double-blind, placebo-controlled, parallel-
group, multicenter study, done at 53 sites throughout the United States.
B. STUDY POPULATION: 370
7. Men & women, with the following criteria:
1. Age : Atleast 18 years
2. Diagnosis: DM(Type 1/2), with symptoms of PDN(for at least 6 months to 5
years)
3. HbA1C level: <12%
4. Optimized diabetic control for atleast 3 months before the enrollment
5. Pain of at least moderate severity, during 7 days before randomization.
8. Includes:
1. Women- Pregnant, breast-feeding, of child-bearing potential & not practicing
adequate birth-control
2. Individuals, who had participated in an investigational trial, within the past 30
days
3. Presence of any other conditions, that may interfere with the assessment of
neuropathic pain
4. Major skin ulcers
5. Clinically significant ECG abnormalities
6. Significant hepatic/renal diseases(CrCl< 50 ml/min)
7. Myocardial infarction/ clinically relevant cardiac dysfunction, within the last 12
months/ any cardiac disorder, which would predispose the patient to
MI/arrhythmia.
9. 8. QTc > 450 milliseconds(for men) , & > 470 milliseconds(in women)
9. Sitting DBP < 50 mm Hg / > 105 mm Hg
10. History of chronic alcohol/drug abuse in near history
11. Pts., expected to undergo surgery during the trial/ taking any medications for
any treatment, that might be expected to interfere with the result of the trial.
10. Include:
1. Concomitant treatment for depression, anxiety/ sleep disorders was allowed,
provided the patient was taking a stable dose, that was not expected to change
during the trial.
2. Acetaminophen, upto 2 g/day, as rescue medication for pain during the trial.
13. Lacosamide (400 mg/d) group showed statistically significant improvement in
Likert pain score over placebo
At the end of treatment 58% of patients (in lacosamide 400 mg/d group)
achieved 30% reduction in Likert pain score , as compared to 46% of placebo-
treated patients
Lacosamide (200 mg/day) group separated from placebo, but failed to show
statistical significance for any of the primary/secondary outcome measures
Lacosamide (600 mg/day group) was significantly more efficacious than placebo
in the observed cases
A relatively-high premature withdrawal rate due to adverse events that occurred
during the titration phase in the “600 mg/day” lacosamide group, was observed.
14. Overall lacosamide, at daily doses of 200-400 mg was well-tolerated, with
8% of patients discontinuing due to adverse events (in the 200 mg/day group), &
23% due to adverse events (in the 400 mg/day group), compared to the 9%
discontinuation rates in the placebo group.
Discontinuations due to adverse events were highest in the “600 mg/day group”
Most common adverse events include dizziness, tremor, headache & fatigue
Somnolence, cognitive & behavioral side effects, weight change & edema were
notably low.
15. According to safety & efficacy analyses lacosamide (400 mg/day) provided
an optimal balance between efficacy & side-effects, in patients with patient
diabetic neuropathy.
16. To summarize this study suggests that lacosamide (at 400 mg/day) provides
an optimal balance between efficacy & side-effects in patients with painful
diabetic neuropathy
Effectiveness of the drug, coupled with demonstrated low-potential for drug-drug
interactions & its proposed novel mechanism of action makes lacosamide a
potentially attractive addition to the pharmacotherapeutical strategies for painful
diabetic neuropathy.
17. Since the study was conducted for a short period of time the result obtained
could not be generalized.
In the lacosamide (600 mg/day) group there was high withdrawal rate due to
adverse events(40%)
Majority of the patients, who withdrew from study did so while still being in
the titration phase.