2008
DOI: 10.1002/ardp.200700250
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Unanticipated Acyloxymethylation of Sumatriptan Indole Nitrogen Atom and its Implications in Prodrug Design

Abstract: Sumatriptan is a potent and selective 5-HT(1B) and 5-HT(1D )agonist used in the symptomatic treatment of migraine; it shows poor oral bioavailability ascribed, in part, to its low lipophilicity. In an attempt to develop acyloxymethyl prodrugs of sumatriptan suitable for oral administration, we carried out the reaction of sumatriptan with chloromethyl esters. To our surprise, acyloxymethylation occurred preferentially at the indole nitrogen rather than at sulfonamide nitrogen, reflecting a difference either in … Show more

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Cited by 2 publications
(2 citation statements)
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“…[16][17][18] Last, melatonin and indomethacin share an indole structure, which may make it effective in indomethacin-responsive disorders, 17 although this is a common structure in nature and appears in triptans and tetracylic ergolene derivatives, such as dihydroergotamine. 19,20 Melatonin's comparatively favorable side effect profile compared to indomethacin makes it a desirable treatment candidate. The side effects of melatonin are generally few and mild, even at high dosages; 17,21,22 daytime tiredness and dizziness are possible.…”
Section: Abstract: Melatonin Migraine Cluster Headache Indomethacinmentioning
confidence: 99%
“…[16][17][18] Last, melatonin and indomethacin share an indole structure, which may make it effective in indomethacin-responsive disorders, 17 although this is a common structure in nature and appears in triptans and tetracylic ergolene derivatives, such as dihydroergotamine. 19,20 Melatonin's comparatively favorable side effect profile compared to indomethacin makes it a desirable treatment candidate. The side effects of melatonin are generally few and mild, even at high dosages; 17,21,22 daytime tiredness and dizziness are possible.…”
Section: Abstract: Melatonin Migraine Cluster Headache Indomethacinmentioning
confidence: 99%
“…The mechanism of hydrolysis probably involves protonation of the 4-imino nitrogen atom, followed by alkyl C–N bond scission via an S N 1 mechanism, leading to the formation of amodiaquine and the corresponding secondary amide (Scheme ) . This mechanism is similar to that reported for the acid-catalyzed hydrolysis of N -acyloxymethyl and N -amidomethyl prodrugs and involves the formation of an iminium ion intermediate, 4 , which can alkylate biomolecules, potentially contributing to toxicity . More recently, we have disclosed a library of N -alkyl-quinolon-4(1 H )-imines (e.g., 3 , Figure ), lacking the N -Mannich base moiety, as potent antiplasmodial agents that target the liver stage of infection .…”
Section: Introductionmentioning
confidence: 53%