The synthesis of S-pentafluorophenyl tris(2,4,6-trimethoxyphenyl)phosphonium acetate bromide (TMPP-AcPFP) and the novel compound (4-hydrazino-4-oxobutyl) [tris(2,4,6-trimethoxyphenyl)phosphonium bromide (TMPP-PrG) is described and the use of these compounds as derivatizing reagents for alcohols, aldehydes and ketones evaluated. Methods have been developed for the pre-column derivatization of alcohols using TMPP-AcPFP and for aldehydes and ketones using TMPP-PrG. The reactions were investigated by the use of a variety of individual test compounds containing the target functional groups. The TMPP acetyl ester and TMPP propyl hydrazone derivatives formed with their respective target analytes produced an enhanced response in electrospray ionization mass spectrometry (ESI-MS), and reproducible chromatography. The use of these two reagents to derivatize and facilitate detection of alcohols (including sugars and steroids), aldehydes and ketones (including steroids) by LC/ESI-MS was investigated.
SummaryLamotrigine is a sodium channel antagonist used for the treatment of epilepsy.
Synthesis of stable isotopically labelled (SIL) [M+7] versions of Lamotrigine(1) and its N-methylated metabolite (2) are described.
This article describes two routes toward the synthesis of cis or trans C2,3,5,7-tetrasubstituted
dihydrobenzofurans as potent and selective bromodomain and extra-terminal
BD2 inhibitors, followed by the optimization of the synthesis of the
lead molecule GSK973 to support pre-clinical efficacy and safety studies.
The use of flow chemistry for a Claisen rearrangement, extensive optimization
of the fluorination step, and high-yielding aminocarbonylation were
key to generate the required 50 g of material. The identified new
route also represents a robust starting point for further optimization.
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