Baeyer–Villiger oxidation

[5] This migration step is also (at least in silico) assisted by two or three peroxyacid units enabling the hydroxyl proton to shuttle to its new position.

[9] Keeping this structure in mind, it makes sense that the substituent that can maintain positive charge the best would be most likely to migrate.

[16] These three reaction mechanisms can really be split into two pathways of peroxyacid attack – on either the oxygen or the carbon of the carbonyl group.

[17] In 1953, William von Eggers Doering and Edwin Dorfman elucidated the correct pathway for the reaction mechanism of the Baeyer–Villiger oxidation by using oxygen-18-labelling of benzophenone.

[22] In 1962, G. B. Payne reported that the use of hydrogen peroxide in the presence of a selenium catalyst will produce the epoxide from alkenyl ketones, while use of peroxyacetic acid will form the ester.

[24] The use of hydrogen peroxide as an oxidant would be advantageous, making the reaction more environmentally friendly as the sole byproduct is water.

[7] Benzeneseleninic acid derivatives as catalysts have been reported to give high selectivity with hydrogen peroxide as the oxidant.

[26] Among stannosilicates, particularly the zeotype Sn-beta and the amorphous Sn-MCM-41 show promising activity and close to full selectivity towards the desired product.

[23] In nature, enzymes called Baeyer-Villiger monooxygenases (BVMOs) perform the oxidation analogously to the chemical reaction.

[30] In the catalytic cycle (see figure on the right), the cellular redox equivalent NADPH first reduces the cofactor, which allows it subsequently to react with molecular oxygen.

[34] BVMOs have been widely studied due to their potential as biocatalysts, that is, for an application in organic synthesis.

[29] BVMOs in particular are interesting for application because they fulfil a range of criteria typically sought for in biocatalysis: besides their ability to catalyse a synthetically useful reaction, some natural homologs were found to have a very large substrate scope (i.e. their reactivity was not restricted to a single compound, as often assumed in enzyme catalysis),[36] they can be easily produced on a large scale, and because the three-dimensional structure of many BVMOs has been determined, enzyme engineering could be applied to produce variants with improved thermostability and/or reactivity.

[29][35] Zoapatanol is a biologically active molecule that occurs naturally in the zeopatle plant, which has been used in Mexico to make a tea that can induce menstruation and labor.

[40][41] They used the Baeyer–Villiger oxidation to make a lactone that served as a crucial building block that ultimately led to the synthesis of zoapatanol.

[40][41] In 2013, Alina Świzdor reported the transformation of the steroid dehydroepiandrosterone to anticancer agent testololactone by use of a Baeyer–Villiger oxidation induced by fungus that produces Baeyer-Villiger monooxygenases.

Baeyer-Villiger oxidation
Baeyer-Villiger oxidation
Reaction mechanism of the Baeyer-Villiger oxidation.
Reaction mechanism of the Baeyer-Villiger oxidation.
Stereoelectronic effects
Stereoelectronic effects
Resonance structures of the Criegee intermediate
Resonance structures of the Criegee intermediate
Steric bulk influencing migration
Steric bulk influencing migration
Original reactions reported by Baeyer and Villiger
Proposed Baeyer-Villiger oxidation intermediates
The different possible outcomes of Dorfman and Doering's labelling experiment
Payne reported that different reagents will give different outcomes when there are more than one functional group
Reaction mechanism of the flavin cofactor to catalyse the Baeyer-Villiger reaction in Baeyer-Villiger monooxygenase enzymes.
Kane and Doyle used a Baeyer-Villiger oxidation to synthesize zoapatanol
Świzdor reported that a Baeyer-Villiger monooxygenase could change dehydroepiandrosterone into testololactone