Efficient enantiodivergent total synthesis of (+) and (−)-bromoxone

The total synthesis of (+)-bromoxone and a formal synthesis of (?)-bromoxone were performed in a simple chemoenzymatic manner, starting from bromobenzene, and using an enantiodivergent strategy. The usefulness of chiral cyclohexadienediols derived from the biotransformations of monosubstituted-aromatic compounds as building blocks for the preparation of natural epoxyenones was confirmed.     

Asymmetric total synthesis of (+)-isocryptotanshinone and formal synthesis of (−)-cryptotanshinone

The first asymmetric total synthesis of (+)-isocryptotanshinone was achieved in 12 linear steps with 12% overall yield from commercially available dihydrobenzopyrone. The key step was a base-mediated cyclization reaction. In addition, the synthetic strategy included the formal synthesis of (−)-cryptotanshinone.     

Enantiopure N-Boc piperidine-2-ethanol for the synthesis of (+)- and (−)-dumetorine,and (+)- and (−)-epidihydropinidine

The convenient synthesis of both enantiomers of the piperidine alkaloids such as dumetorine and epidihydropinidine is described. Pure enantiomers of 2-(2-hydroxy-ethyl)-piperidine-1-carboxylic acid tert-butyl ester are used as a common starting material. The syntheses are based on a RCM reaction and on methylation of the piperidine ring according to Beak–Lee methodology, respectively.     

Stereoselective synthesis of deuterated β-cyclohexenylserine, a biosynthetic intermediate of the salinosporamides

A straightforward, highly stereoselective protocol toward the synthesis of deuterium-labeled (2R,3S,4S)-β-cyclohexenylserine has been developed. Key steps are a Nozaki-Hiyama-Kishi reaction generating the stereogenic centers and a ring-closing metathesis for the construction of the cyclohexenyl ring system. The labeled amino acid was further activated as an SNAc-ester for feeding experiments.     

Resolution of sclareolide as a key intermediate for the synthesis of Ambrox®

Sclareolide was efficiently resolved by a diastereomeric salt formation method using homochiral erythro-2-amino-1,2-diphenylethanol (ADPE) as a resolving agent.     

A convenient synthesis of (+)-albicanol based on enzymatic function: total syntheses of (+)-albicanyl acetate, (−)-albicanyl 3,4-dihydroxycinnamate, (−)-drimenol, (−)-drimenin and (−)-ambrox

By using lipase ‘PL-266’ from Alcaligenes sp. enantioselective acetylation of (±)-albicanol 4 with isopropenyl acetate gave the enantiomerically pure (+)-albicanyl acetate 3 and (+)-albicanol 4. Deprotection of (+)-3 afforded the natural (+)-albicanol 4 which was converted to the natural products (−)-albicanyl 3,4-dihydroxycinnamate 7, (−)-drimenol 8, (−)-drimenin 9 and (−)-ambrox 10.     

Stereoselective total syntheses of (−)-pseudohygrophorone A12 and (−)-pseudohygrophorone B12

Abstract

Stereoselective total syntheses of anti-fungal cyclohexenones (?)-pseudohygrophorone A¹² and (?)-pseudohygrophorone B¹² were achieved. Salient features of these syntheses are the diastereoselective addition of dodecylmagnesium bromide to highly oxygenated ketone derived from (?)-quinic acid and α-oxidation of the enone.     

Stereoselective synthesis of (−)-centrolobine

The stereoselective synthesis of (−)-centrolobine has been accomplished starting from d-glyceraldehyde acetonide by a combination of chelation-controlled diastereoselective alkylation and ring-closing metathesis. A high degree of 1,3-asymmetric induction has been realized in an ether system.     

Stereoselective total synthesis of (+)-β-conhydrine from d-mannitol

An asymmetric synthesis of the piperidine alkaloid (+)-β-conhydrine has been developed starting from (R)-protected glyceraldehyde as the chiral precursor using Barbier allylation, azide nucleophilic substitution, and ring-closing metathesis as the key steps.     

First total synthesis of (−)-aplyolide A

The first total synthesis of (−)-aplyolide A², (16S)-methyloxacyclohexadeca-(5Z,8Z,11Z,14Z)-tetraen-2-one, 1 is reported. The synthesis is based on three consecutive couplings of terminal alkynes with propargylic halides and proves the absolute configuration of the stereogenic center of the natural product.     

A convergent approach for the total synthesis of the α-glucosidase inhibitor (−)-panaxjapyne-C

The stereoselective total synthesis of (?)-panaxjapyne-C was accomplished in a convergent fashion. The synthesis utilizes the readily available enantiomers l-(+)-diethyltartrate and d-(?)-diethyltartrate and involves a Cadiot–Chodkiewicz coupling reaction, and an Ohira–Bestmann reaction as the key steps.     

Asymmetric synthesis of (−)- and (+)-neodichroine/hydrachine A from (+)- and (−)-febrifugine

A new asymmetric approach to both enantiomers of the quinazolinone-containing natural product febrifugine is reported. Utilising a proline-mediated aminooxylation-Horner-Wadsworth-Emmons sequence provides the key optically active 2,3-disubstituted piperidine intermediate 7 in high enantioselectivity but poor overall yield (7 steps, 3%, 98% ee). This intermediate has been used to prepare both naturally occurring (+)-febrifugine (1) and its (?)-enantiomer. In turn, each were then used to synthesise, for the first time, both enantiomers of the claimed natural product neodichroine/hydrachine A. Spectroscopic data for the synthetic compound matched the claimed structure. However, the specific rotation differed in both magnitude and sign from the isolation work.     

Asymmetric induction by sulfinyl chirality. A total synthesis of (+)-talaromycin A and (−)-talaromycin B

A total synthesis of (+)-talaromycin A and (−)-talaromycin B was accomplished by means of successive asymmetric induction of all chiral centers using a chiral sulfinyl group.     

A total synthesis of (+)-preussin and its 5-epimer

(+)-Preussin (1) and its 5-epimer were synthesized from the divmylcarbmol (3) with Sharpless asymmetric epoxidation of 3 and the oxidative cyclization of 9 with PDC as the key steps     

Enzymatic resolution of (±)-conduritol-B,a key intermediate for the synthesis of glycosidase inhibitors

Lipases from porcine pancreas, Candida cylindracea and Mucor miehei (adsorbed on support, Lipozyme^® IM) catalysed in t-butylmethylether the alcoholysis of rac-conduritol-B peracetate, (±)-1, by n-butanol to give enantiopure (2S,3S)-diacetoxy-(1R,4R)-dihydroxycyclohex-5-ene, (−)-3, and (1S,2R,3R,4S)-tetraacetoxy-cyclohex-5-ene, (+)-1. The enantioforms (+)- and (−)-conduritol-B, obtained after chemical hydrolysis of (−)-3 and (+)-1, respectively, may be employed to prepare both the enantiomers of conduritol-B epoxide and cyclophellitol, powerful inhibitors of glycosidases.     

Stereoselective synthesis of (−)-synargentolide B

A convergent, enantioselective total synthesis of (?)-synargentolide-B has been accomplished from readily available l-arabinose and d-ethyl lactate by a 10-step sequence involving Still-Gennari olefination, one-pot acidic deprotection/lactonization and olefin cross-metathesis reaction as the key step.     

First stereoselective total synthesis of (−)-stagonolide A

The first stereoselective total synthesis of the nonenolide (?)-stagonolide A is described. Olefin metathesis and epoxide opening reaction are the key steps involved.     

Enantiodivergent synthesis of (+)- and (−)-isolaurepan

The enantiodivergent synthesis of (+)-and (?)-isolaurepan was achieved from a common chiral template easily available from tri-O-acetyl-d-glucal, using as key step a diastereoselective thermal Claisen rearrangement, combined with a ring expansion reaction using trimethylsilyldiazomethane.     

Total synthesis of natural (−)- and unnatural (+)-Melearoride A

This communication details the first total synthesis of the 13-membered macrolide, (?)-Melearoride A, as well as unnatural (+)-Melearoride A. The synthesis features a concise 13 step synthesis (11 steps longest linear sequence) that offers flexible stereo-control and multiple opportunities for unnatural analog synthesis to delve into antifungal SAR. The route features a cuprate addition, an Evans asymmetric alkylation, and a ring-closing metathesis (RCM) to close the 13-membered macrocyclic core.