Better comparisons of antiepileptic drugs: what measures of efficacy?
Tóm tắt
With the licensing of new antiepileptic drugs there is an obvious need for the determination of the comparative efficacy, tolerability and overall effectiveness against standard (existing) antiepileptic drugs. Such data can only be determined within the context of well‐designed randomised clinical trials (RCTs). Such comparative monotherapy studies may form a part of phase III drug development programmes for a new antiepileptic drug. They may be commenced once there is satisfactory evidence for efficacy and safety derived from placebo‐controlled add‐on studies in more refractory populations of patients. In this manuscript definitions of outcomes such as effectiveness, efficacy, and tolerability are given. Health‐related quality of life measures are presented, and it can be argued that such measures should be a primary outcome variable. However, there is little evidence that any quality of life measures have sufficient validity and sensitivity to be a useful tool in the comparison of drug treatments for epilepsy. Different populations can be studied in ‘withdrawal to monotherapy’ designs. In such studies patients poorly controlled on their existing therapy are randomised to receive different monotherapy regimes with withdrawal of their existing antiepileptic drugs. This clinical trial design has not been used in genuine comparisons between antiepileptic drugs and the efficiency of this approach has yet to be determined. Experience from studies comparing monotherapy would suggest that differences in efficacy between antiepileptic drugs in the target populations may be difficult to detect. Differences likely exist between the incidence and profile of adverse effects between different drugs. The main benefit of new antiepileptic drugs may be in reducing the incidence and severity of adverse reactions compared to older drugs and in doing so they may prove to be more effective.
Tài liệu tham khảo
Commission for Antiepileptic Drugs. Guidelines for the Clinical Evaluation of Antiepileptic Drugs. Epilepsia 1989;30: 400–06.
Mattson RH, Cramer JA, Collins JF, et al. Comparison of carbamazepine, phenobarbital, phenytoin and primidone in partial and secondarily generalized tonic-clonic seizures. New England Journal of Medicine 1985;313: 145–51.
Mattson RH, Cramer JA, Collins JF, et al. A comparison of valproate with carbamazepine for the treatment of complex partial seizures and secondarily generalized tonic-clonic seizures in adults. New England Journal of Medicine 1992;327: 765–771.
Jacoby A, Baker GA, Steen N, Potts P, Chadwick DW. The clinical course of epilepsy and its psychological correlates: Findings from a UK Community Study. Epilepsia 1996;37 (2): 148–61.
Fraught E, Sachdeo RC, Remler MP, Chayasirisobhon S, Iragui, Madoz VJ, Ramsey RE, Sutula TP, Kanner A, Harner RN, Kuzniecky R, et al. Felbamate monotherapy for partial onset seizures: an active control trial. Neurology Apr 1993;43 (4): 688–92.
Sachdeo R, Kramer LD, Rosenberg A, and Sachdeo S. (1992) Felbamate monotherapy: controlled trial in patients with partial onset seizures. Ann Neurol. Sep 1992;32 (3): 386–92.
Heller AJ, Stewart J, Hughes E, et al. (1995) Comparative efficacy and toxicity of phenobarbital, phenytoin, carbamaze pine and valproate in adults and children with newly diagnosed previously untreated epilepsy. Journal of Neurology, Neurosurgery and Psychiatry 1995;58: 44–50.
Jones B, Jarvis P, Lewis JA, et al. Trials to assess equivalence: the importance of rigorous methods. British Medical Journal 1996; 313: 36–9.