Syntheses, chemical throughput

ScHOUTEN, J. C., Rebrov, E., de Croon, M. H. J. M., Challenging prospects for microstructured reaction architectures in high-throughput catalyst screening, small scale fuel processing, and sustainable fine chemical synthesis, in Proceedings of the Micro Chemical Plant - International Workshop, pp. L5 (25-32) (4 Eebruary 2003), Kyoto, Japan. 

High throughput screening is one of the hot topics in heterogeneous catalysis. Advanced experimental techniques have been developed to screen and develop solid catalysts for gas-phase systems. However, for catalytic three-phase systems, rapid screening has got much less attention [1-6]. Three-phase catalysis is applied in numerous industrial processes, from synthesis of fine chemicals to refining of crade oil. 

The application of combinatorial principles in chemical synthesis, particularly in the search for active substances, requires analytical methods with high throughput (von dem Bussche-Hunnefeld et al. [1997]). Screening techniques can be used to analyse a large number of test samples in a short... 

The issue of parallel versus sequential synthesis using multimode or monomode cavities, respectively, deserves special comment. While the parallel set-up allows for a considerably higher throughput achievable in the relatively short timeframe of a microwave-enhanced chemical reaction, the individual control over each reaction vessel in terms of reaction temperature/pressure is limited. In the parallel mode, all reaction vessels are exposed to the same irradiation conditions. In order to ensure similar temperatures in each vessel, the same volume of the identical solvent should be used in each reaction vessel because of the dielectric properties involved [86]. As an alternative to parallel processing, the automated sequential synthesis of libraries can be a viable strategy if small focused libraries (20-200 compounds) need to be prepared. Irradiating each individual reaction vessel separately gives better control over the reaction parameters and allows for the rapid optimization of reaction conditions. For the preparation of relatively small libraries, where delicate chemistries are to be performed, the sequential format may be preferable. This is discussed in more detail in Chapter 5. 

The issue of parallel versus sequential synthesis using multimode or monomode cavities, respectively deserves special comment. While the parallel setup allows for considerable throughput that can be achieved in the relatively short timeframe of a microwave-enhanced chemical reaction, the individual control over each reaction vessel in terms of reaction temperature and/or pressure is limited. In the parallel... 

The discovery of oxazoline hydroxamates as potential inhibitors of LpxC was the result of high-throughput screening of large libraries of compounds at the Merck Research Laboratories in collaboration with the Department of Biochemistry, Duke University Medical Center [95]. The lead compound, L-573,655, was a racemic mixture of 4-carbohydroxamido-2-phenyl-2-oxazoline, which had been previously made by Stammer et al. [96] as a precursor in the chemical synthesis of cyclosporine. Namely, (R,S)-serine methyl ester hydrochloride (149) is converted into (R,S)-4-carbomethoxy-2-phenyl-2-oxazoline (150) via treatment with ethyl benzimidate using the Elliot procedure [97]. Treatment of this ester with one equivalent each of hydroxylamine and sodium methoxide in methanol at room temperature affords the desired (R,S)-4-carbohydroxamido-2-phenyl-2-oxazoline (151), as depicted in Scheme 30. 

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