Eletriptan in the Early Treatment of Acute Migraine: Influence of Pain Intensity and Time of Dosing

Brandes, JL; Kudrow, David; Cady, Roger; Tiseo, Paul J.; Sun, Wei; Sikes, Carolyn

doi:10.1111/j.1468-2982.2005.00981.x

Cited by 95 publications

(106 citation statements)

References 12 publications

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“…Pain-free efficacy of migraine pharmacotherapy appears to be enhanced, and the incidence of adverse events appears to be reduced by the practice of early intervention [Goadsby et al 2008;Silberstein et al 2008;Mathew et al 2007;Carpay et al 2004;Brandes et al 2005;Loder et al 2005;Mathew et al 2004;Scholpp et al 2004;Cady et al 2000]. These caveats notwithstanding, the results demonstrate the better performance of sumatriptan/naproxen sodium to sumatriptan monotherapy, naproxen sodium monotherapy and placebo with respect to the rigorous clinical endpoint of sustained pain-free/no adverse events and reinforce the usefulness of utilizing this new composite endpoint.…”

Section: Discussionmentioning

confidence: 70%

Fixed-dose sumatriptan/naproxen sodium compared with each monotherapy utilizing the novel composite endpoint of sustained pain-free/no adverse events

Landy¹,

White

Lener

et al. 2009

Ther Adv Neurol Disord

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A novel composite endpoint, sustained pain-free/no adverse events, was recently proposed as a more rigorous means of capturing in a single measure the attributes of migraine pharmacotherapy that patients consider most important: rapid and sustained pain-free response with no side-effects. Using pooled data from two replicate randomized, double-blind, parallel-group, placebo-controlled studies, this post hoc analysis compared the fixed-dose combination tablet sumatriptan/naproxen sodium (n ¼ 726) with sumatriptan monotherapy (n ¼ 723), naproxen sodium monotherapy (n ¼ 720), and placebo (n ¼ 742) with respect to sustained pain-free/no adverse events and closely related composite measures. Sustained painfree/no adverse events was defined as having both a sustained pain-free response from 2 through 24 hours post-dose with no use of rescue medication and having no adverse events within up to 5 days after dosing with study medication. The percentage of patients with sustained pain-free/no adverse events was 16% with sumatriptan/naproxen sodium compared with 11%, 9% and 7% for sumatriptan, naproxen sodium and placebo, respectively (p50.01 sumatriptan/naproxen sodium versus each other treatment). Sumatriptan/naproxen sodium was also significantly more effective than sumatriptan, naproxen sodium, and placebo for other composite endpoints including the percentages of patients with (1) sustained pain-free/no adverse events within 1 day; (2) sustained pain-free/no drug-related adverse events within up to 5 days; (3) sustained pain-free/no drug-related adverse events within 1 day; (4) sustained pain relief/no adverse events within up to 5 days; and (5) sustained pain relief/no adverse events within 1 day. The results demonstrate the superiority of sumatriptan/naproxen sodium to sumatriptan monotherapy, naproxen sodium monotherapy and placebo with respect to the rigorous and clinically relevant endpoint of sustained pain-free/no adverse events and reinforce the usefulness of utilizing this new composite endpoint.

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Section: Discussionmentioning

confidence: 70%

Fixed-dose sumatriptan/naproxen sodium compared with each monotherapy utilizing the novel composite endpoint of sustained pain-free/no adverse events

Landy¹,

White

Lener

et al. 2009

Ther Adv Neurol Disord

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show abstract

“…Correspondingly, in clinical use, triptan efficacy is diminished when allodynia is present during a migraine attack [70]. Several prospective trials have demonstrated substantial improvement of efficacy outcomes when the patient was instructed to treat at a mild level of migraine pain intensity [71][72][73][74][75]. Presumably, mild pain implies that treatment took place prior to the development of cutaneous allodynia, but this cannot be certain.…”

Section: Implications Of the Neuropathic Pain Model For Migraine Treamentioning

confidence: 96%

Is migraine a neuropathic pain syndrome?

Biondi

2006

Current Science Inc

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The understanding of migraine pathophysiology has evolved from the belief that migraine is a vascular disorder, to evidence that better defines migraine as a neurogenic disorder associated with secondary changes in brain perfusion. There is evidence to suggest that the early phase of migraine pain results from neurogenic inflammation affecting cranial blood vessels and dura. Allodynia, hyperalgesia, and expansion of nociceptive fields occur during most well-established migraine attacks. These clinical features of migraine are evocative of those traditionally associated with neuropathic pain. A hypothesis that defines migraine pain as a unique neuropathic pain disorder can imply the potential for neural plasticity and may provide insight into the mechanisms that underlie the transformation of episodic to chronic forms of migraine. The neuropathic pain model of migraine pathophysiology not only paves the way for mechanism-based treatment strategies that can improve the acute and preventive management of migraine attacks, but also opens the door for the discovery of novel therapeutic targets. It also lends momentum to an understanding of clinically intriguing topics such as opiate-induced hyperalgesia and medication-overuse headache (rebound headache), opioid resistance in the treatment of chronic headache, and disease modification in defending against the potential for migraine transformation.

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“…Aufgrund von Posthoc-Auswertungen kontrollierter Studien, open-label-Studien und neuerer kontrollierter Studien mit gezielt früher Einnahme der Testmedikation bei noch milder Schmerzintensität ergibt sich heute die Empfehlung, Triptane bereits bei einsetzendem Kopfschmerz, also zu einem frü-hen Zeitpunkt der Attacke, zu verabreichen [9][10][11]. Hierdurch ergeben sich Vorteile hinsichtlich der Schnelligkeit und des Ausmaßes der Schmerzreduktion [12][13][14]. Die Progression der Attacke bis hin zum Schmerz mit starker Intensität kann so in vielen Fällen verhindert werden.…”

Section: Wann Sollten Triptane Eingenommen Werden?unclassified

Aktueller Kenntnisstand und Entwicklungen in der akuten und prophylaktischen Therapie der Migräne

Schriever

Bühlen

Broich

2014

Bundesgesundheitsbl.

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Eletriptan in the Early Treatment of Acute Migraine: Influence of Pain Intensity and Time of Dosing

Cited by 95 publications

References 12 publications

Fixed-dose sumatriptan/naproxen sodium compared with each monotherapy utilizing the novel composite endpoint of sustained pain-free/no adverse events

Fixed-dose sumatriptan/naproxen sodium compared with each monotherapy utilizing the novel composite endpoint of sustained pain-free/no adverse events

Is migraine a neuropathic pain syndrome?

Aktueller Kenntnisstand und Entwicklungen in der akuten und prophylaktischen Therapie der Migräne

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