0
Mar 2013, Vol 167, No. 3
< Previous in this Issue  |  Next in this Issue >

Article

Published online Mar 2013

Comparative Effectiveness Research

Migraine Therapeutics in Adolescents:  A Systematic Analysis and Historic Perspectives of Triptan Trials in Adolescents
Haihao Sun, MD, PhD; Eric Bastings, MD; Jean Temeck, MD; P. Brian Smith, MD, MPH, MHS; Angela Men, MD; Veneeta Tandon, PhD; Dianne Murphy, MD; William Rodriguez, MD, PhD
[+] Author Affiliations

Author Affiliations: Office of Pediatric Therapeutics and the Center for Drug Evaluation and Research, US Food and Drug Administration, Silver Spring, Maryland (Drs Sun, Bastings, Temeck, Men, Tandon, Murphy, and Rodriguez); and Department of Pediatrics, Duke Clinical Research Institute, Duke University Medical Center, Durham, North Carolina (Dr Smith).


JAMA Pediatr. 2013;167(3):243-249. doi:10.1001/jamapediatrics.2013.872. doi:10:1001/jama.2010.920
[+] More
Article
Comments

Objectives  To conduct a systematic review and analysis of trial data submitted to the US Food and Drug Administration (FDA) to identify possible causes for the failure of pediatric trials of triptans for treatment of migraines.

Data Source  The FDA website for drug information and published literature.

Study Selection  All pediatric efficacy and pharmacokinetics trial data of drugs used for abortive treatment of migraine submitted to the FDA from January 1, 1999, through December 31, 2011.

Main Outcome Measures  Patient demographic baseline characteristics, inclusion and exclusion criteria, trial designs, efficacy end points, and pharmacokinetic profiles were analyzed and compared across drug products.

Results  We analyzed data for sumatriptan succinate nasal spray and zolmitriptan, eletriptan hydrobromide, almotriptan malate, and rizatriptan benzoate tablets. Seven efficacy trials had a randomized, double-blinded, placebo-controlled, parallel-group trial design. In 4 trials, patients were required to have a history of migraine attacks lasting at least 4 hours. High response rates for placebo were observed in all trials, with pain relief at 2 hours ranging from 53% to 57.5%. Nonrandomization of patients with an early placebo response design was used in the rizatriptan trial in 2011. Compared with the rizatriptan trial conducted in 1999, the 2011 rizatriptan trial reduced the placebo response rate by 6% for headache freedom at the 2-hour posttreatment end point owing to study design. The pharmacokinetic profiles between adolescents and adults were statistically similar.

Conclusions  High placebo response rates are consistent across all trials and may represent the principal challenge in pediatric trials of drugs for abortive treatment of migraine. Enrichment with selection of subjects with long-lasting migraine attacks is not sufficient to overcome high placebo response rates. Another enrichment strategy, the nonrandomization of patients with an early placebo response, successfully reduces the high placebo response rate for rizatriptan and is a trial design that should be considered for future pediatric trials of abortive migraine therapeutics.
Your Session has timed out. Please sign back in to continue.

Sign In to Access Full Content

Don't have Access?

Register and get free email Table of Contents alerts, saved searches, PowerPoint downloads, CME quizzes, and more

Subscribe for full-text access to content from 1998 forward and a host of useful features

Activate your current subscription (AMA members and current subscribers)

Purchase Online Access to this article for 24 hours

Figures

Tables

Interactive Graphics

Video

Correspondence

CME
Accreditation Information
The American Medical Association is accredited by the Accreditation Council for Continuing Medical Education to provide continuing medical education for physicians. The AMA designates this journal-based CME activity for a maximum of 1 AMA PRA Category 1 CreditTM per course. Physicians should claim only the credit commensurate with the extent of their participation in the activity. Physicians who complete the CME course and score at least 80% correct on the quiz are eligible for AMA PRA Category 1 CreditTM.
Note: You must get at least of the answers correct to pass this quiz.
Clear Answers | Save For Later
You have not filled in all the answers to complete this quiz
The following questions were not answered:
Sorry, you have unsuccessfully completed this CME quiz with a score of
The following questions were not answered correctly:
Commitment to Change (optional):
Indicate what change(s) you will implement in your practice, if any, based on this CME course.
Your quiz results:
The filled radio buttons indicate your responses. The preferred responses are highlighted
For CME Course: A Proposed Model for Initial Assessment and Management of Acute Heart Failure Syndromes
Indicate what changes(s) you will implement in your practice, if any, based on this CME course.
NOTE:
Citing articles are presented as examples only. In non-demo SCM6 implementation, integration with CrossRef’s “Cited By” API will populate this tab (http://www.crossref.org/citedby.html).
Compression-Only CPR: Pushing the Science Forward
Cone
AAM 2010;304:1493-1495.
All you need to read in the other general jounals
BMJ 2010;341:c5893-c1494.
Submit a Response
Articles Related By Topic
No Evidence of Efficacy or Evidence of No Efficacy
JAMA Pediatr. 2013;167(3):300-302. doi:10.1001/jamapediatrics.2013.1105.
Radiological Case of the Month
Arch Pediatr Adolesc Med. 2000;154(5):523-524. doi:10.1001/archpedi.154.5.523.
Related Topics
 Choose content to search
Sign In
© American Medical Association.
All Rights Reserved.