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・ Desmiphora fuscosignata
・ Desmiphora hirticollis
・ Desmiphora intonsa
・ Desmiphora jullienae
・ Desmiphora kawensis
・ Desmiphora lanuginosa
・ Desmiphora lateralis
・ Desmiphora laterialba
・ Desmiphora lenkoi
・ Desmiphora lineatipennis
・ Desmiphora longipilis
・ Desmiphora maculosa
・ Desmiphora magnifica
・ Desmiphora mirim
・ Desmiphora mulsa
Desmethylprodine
・ Desmethylsertraline
・ Desmia
・ Desmia albisectalis
・ Desmia albitarsalis
・ Desmia angustalis
・ Desmia anitalis
・ Desmia bajulalis
・ Desmia benealis
・ Desmia bifidalis
・ Desmia bigeminalis
・ Desmia bourguignoni
・ Desmia ceresalis
・ Desmia chryseis
・ Desmia ciliata


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Desmethylprodine : ウィキペディア英語版
Desmethylprodine

Desmethylprodine or 1-methyl-4-phenyl-4-propionoxypiperidine (MPPP) is an opioid analgesic drug developed in the 1940s by researchers at Hoffmann-La Roche.〔 - Preparation of Esters〕 It is an analog of pethidine (meperidine) which the DEA has labeled as a Schedule I drug in the United States. Chemically, it is a reversed ester of pethidine which has about 70% of the potency of morphine.
==History==
Desmethylprodine was first synthesized in 1947 at Hoffman-LaRoche Laboratories by Albert Ziering and John Lee. They found that it produced effects similar to morphine when administered to rats. Ziering had been searching for synthetic painkillers that were less addictive than morphine. The new drug was a slight variant of pethidine. It was found to be no more effective than pethidine and was never marketed.
In 1976, a 23-year-old graduate student in chemistry named Barry Kidston was searching for a way to make a legal recreational drug. Having read the paper by Ziering and Lee, he deduced that he could make a drug with pethidine's effects without its legal restrictions, since desmethylprodine is a different molecule and had never been addressed by law. Kidston successfully synthesized and used desmethylprodine for several months, after which he suddenly came down with the symptoms of Parkinson's disease and was hospitalized. Physicians were perplexed, since Parkinson's disease would be a great rarity in someone so young, but L-dopa, the standard drug for Parkinson's, relieved his symptoms. L-dopa is a precursor for dopamine, the neurotransmitter whose lack produces Parkinson's symptoms. It was later found that his development of Parkinson's was due to a common impurity in the synthesis of MPPP called MPTP (1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine), a neurotoxin that specifically targets dopamine producing neurons. 〔〔Gibb, Barry J. (2007). ''The Rough Guide to the Brain'', Rough Guides Ltd., London, ()〕

抄文引用元・出典: フリー百科事典『 ウィキペディア(Wikipedia)
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