Test purchase, synthesis and characterization of 2- methoxydiphenidine (MXP) and differentiation from its metaand para-substituted isomers.
Date
2015-09Author
Morris, Noreen
McLaughlin, Gavin
Kavanagh, Pierce V.
Power, John D.
O'Brien, John
Talbot, Brian
Elliott, Simon P.
Wallach, Jason
Hoang, Khoa
Morris, Hamilton
Brandt, Simon D.
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Show full item recordAbstract
The structurally diverse nature of the 1,2-diphenylethylamine template provides
access to a range of substances for drug discovery work but some have attracted
attention as ‘research chemicals’. The most recent examples include diphenidine, i.e.
1-(1,2-diphenylethyl)piperidine and 2-methoxydiphenidine, i.e. 1-[1-(2-
methoxyphenyl)-2-phenylethyl]piperidine (MXP, methoxyphenidine, 2-MXP) that
have been associated with uncompetitive N-methyl-D-aspartate (NMDA) receptor
antagonist activity. Challenges encountered during chemical analysis include the
presence of positional isomers. Three powdered samples suspected to contain 2-
MXP were obtained from three Internet retailers in the United Kingdom and subjected
to analytical characterization by gas-, and high performance liquid chromatography
(GC-, HPLC) coupled to various forms of mass spectrometry (MS). Nuclear magnetic
resonance spectroscopy, infrared spectroscopy and thin layer chromatography were
also employed. This was supported by the synthesis of all three isomers (2-, 3- and
4-MXP) that were obtained from two different synthetic routes. The analytical data
obtained for the three purchased samples were consistent with the synthesized 2-
MXP standard. The differentiation between the isomers was possible. Distinct
stability differences were observed for all three isomers during in-source collisioninduced
dissociation of the protonated molecule when employing detection under
HPLC selected-ion monitoring detection, which added to the ability to differentiate
between them. Furthermore, the analysis of a 2-MXP tablet by matrix assisted inlet
ionization Orbitrap mass spectrometry confirmed that it was possible to detect the
protonated molecule of 2-MXP directly from the tablet surface following addition of 3- nitrobenzonitrile as the matrix.
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