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Chemo methods

The past thirty years have witnessed great advances in the selective synthesis of epoxides, and numerous regio-, chemo-, enantio-, and diastereoselective methods have been developed. Discovered in 1980, the Katsuki-Sharpless catalytic asymmetric epoxidation of allylic alcohols, in which a catalyst for the first time demonstrated both high selectivity and substrate promiscuity, was the first practical entry into the world of chiral 2,3-epoxy alcohols [10, 11]. Asymmetric catalysis of the epoxidation of unfunctionalized olefins through the use of Jacobsen s chiral [(sale-i i) Mi iln] [12] or Shi s chiral ketones [13] as oxidants is also well established. Catalytic asymmetric epoxidations have been comprehensively reviewed [14, 15]. [Pg.447]

Industrial production of amino acids by fermentation and chemo-enzymatic methods... [Pg.231]

In this chapter we consider amino acid production by fermentation and by chemo-enzymatic methods. We first consider the stereochemistry of amino adds and the importance of chirality in chemical synthesis. General approaches to amino add fermentation and recovery of amino adds from fermentation broths are then dealt with, followed by a detailed consideration of the production of L-phenylalanine by direct fermentation. Later in this chapter, chemo-enzymatic methods of amino acid... [Pg.232]

Two appendices are included at the end of this chapter. The first is intended to serve as a reminder, for those of you who might need it, of the nomendature and representation of stereoisomers. The second appendix contains descriptions of various chemo-enzymatic methods of amino acid production. This appendix has been constructed largely from the recent primary literature and includes many new advances in the field. It is not necessary for you to consult the appendix to satisfy the learning objectives of the chapter, rather the information is provided to illustrate the extensive range of methodology assodated with chemo-enzymatic approaches to amino add production. It is therefore available for those of you who may wish to extend your knowledge in this area. Where available, data derived from die literature are used to illustrate methods and to discuss economic aspects of large-scale production. [Pg.233]

Encapsulation in Y zeohte was also the method chosen to immobihze Mn complexes of C2-symmetric tetradentate hgands (Fig. 24) [75]. These materials were used as catalysts for the enantioselective oxidation of sulfides to sulfoxides with NaOCl. The lack of activity when the larger io-dosylbenzene was used as an oxidant was interpreted as an indication that the reaction took place inside the zeolite microporous system. Both the chemo- and enantioselectivity were dependent on the structure of the sulfide. (2-Ethylbutyl)phenylsulfide led to better results than methylphenylsulfide, although in all cases the enantioselectivity was low (up to 21% ee). [Pg.185]

Perhaps the most interesting aspect of this set of studies is the question posed in the recent paper by Schmidt et al. (2004) and deals with the reality of the patterns they observed. Is the polymorphism observed a result of the calculation methods used in the study, neural network (NN), and multivariate statistical analysis (MVA) Would increased sampling result in a greater number of chemo-types It is entirely possible, of course, that the numbers obtained in this study are a true reflection of the biosynthetic capacities of the plants studied. The authors concluded—and this is a point made elsewhere in this review—that ... for a correct interpretation a good knowledge of the biosynthetic background of the components is needed. ... [Pg.49]


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Chemo-enzymatic methods

Oxidation chemo-enzymatic methods

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