Total synthesis of both (+)-compactin and (+)-mevinolin. A general strategy based on the use of a special titanium reagent for dicarbonyl coupling

Clive, Derrick L. J.; Murthy, K. S. Keshava; Wee, Andrew G. H.; Prasad, J. Siva; Silva, Gil Valdo José da; Majewski, Marek; Anderson, Paul C.; Evans, Claire F.; Haugen, Richard D.

doi:10.1021/ja00164a024

Cited by 88 publications

(18 citation statements)

References 3 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…As depicted in Scheme 3 , chiral homoallylic alcohol 1a was subjected to t BuOCl and NaBr in DMF at −40°C under a continuously bubbling CO 2 system to give, after crystallization, pure bromocarbonate product 2a in 76% yield, >99% ee, and >19:1 dr without column chromatography isolation. Compound 2a was then converted to acetate 7 in two steps via acetonidation ( Clive et al., 1990 , Radl et al., 2002 , Beck et al., 1995 ) followed by an S N 2 reaction with a total yield of 74%. Subsequent hydrolysis of the acetate proceeded smoothly to give Kaneka alcohol 8 in 93% yield ( Fan et al., 2011 , Sun et al., 2007 ), which could be transformed to the final rosuvastatin 9 via known procedures ( Wess et al., 1990 ).…”

Section: Resultsmentioning

confidence: 99%

Chiral Syn-1,3-diol Derivatives via a One-Pot Diastereoselective Carboxylation/ Bromocyclization of Homoallylic Alcohols

et al. 2018

View full text Add to dashboard Cite

SummaryChiral syn-1,3-diols are fundamental structural motifs in many natural products and drugs. The traditional Narasaka-Prasad diastereoselective reduction from chiral β-hydroxyketones is an important process for the synthesis of these functionalized syn-1,3-diols, but it is of limited applicability for large-scale synthesis because (1) highly diastereoselective control requires extra explosive and flammable Et2BOMe as a chelating agent under cryogenic conditions and (2) only a few functional syn-1,3-diol scaffolds are available. Those involving halogen-functionalized syn-1,3-diols are much less common. There are no reported diastereoselective reactions involving chemical fixation of CO2/bromocyclization of homoallylic alcohols to halogen-containing chiral syn-1,3-diols. Herein, we report an asymmetric synthesis of syn-1,3-diol derivatives via direct diastereoselective carboxylation/bromocyclization with both relative and absolute stereocontrol utilizing chiral homoallylic alcohols and CO2 in one pot with up to 91% yield, > 99% ee, and >19:1 dr. The power of this methodology has been demonstrated by the asymmetric synthesis of statins at the pilot plant scale.

show abstract

Section: Resultsmentioning

confidence: 99%

Chiral Syn-1,3-diol Derivatives via a One-Pot Diastereoselective Carboxylation/ Bromocyclization of Homoallylic Alcohols

et al. 2018

View full text Add to dashboard Cite

show abstract

“…At this point we could also assign the absolute configuration of the b-stereocenter generated at the initial conjugate addition reaction by chemical correlation. 3 , for the R isomer) [16] allowed us to assign a R configuration for the a stereocenter to the formyl moiety in compound 7 a and this configuration was extended to all compounds 4, 5, 6, and 7 prepared previously, in which the stereocenter had been already installed in the initial conjugate addition reaction between aldehydes 2 a-2 o and N-nitromethylphthalimide 1 by using catalyst 3. Moreover, this configuration is also in agreement with the configuration of conjugate addition products obtained in other Michael-type reactions catalyzed by 3.…”

Section: In Memory Of Our Colleague and Friend Rafael Suaumentioning

confidence: 97%

Organocatalytic Enantioselective Formal Conjugate Addition of a Hydroxymoyl Anion to α,β‐Unsaturated Aldehydes

Alonso

Reyes

Carrillo

et al. 2011

Chemistry A European J

View full text Add to dashboard Cite

In memory of our colleague and friend Rafael SuauThe conjugate addition reaction is a fundamental transformation in organic chemistry. The wide variety of reagents amenable to participate as Michael donors or acceptors makes this reaction extremely versatile, allowing the preparation of many different classes of highly functionalized compounds in a very easy and reliable way. Moreover, the conjugate addition reaction also occurs very often with the concomitant generation of one or more stereocenters and, in this context, intense research has focused on the development of catalytic enantioselective approaches for carrying out this important reaction in a stereocontrolled way.[1] Although most of the methodologies reported to date involve the use of transition-metal catalysts, several organocatalytic enantioselective variants of the conjugate addition reaction have been developed in the last few years;[2] many of which have performed excellently with regard to chemical efficiency and stereocontrol. On the other hand, many research groups have also directed their attention to finding novel reactivity patterns applied to the conjugate addition reaction by using umpoled reagents, [3] which have expanded the array of compounds which can be used as Michael donors or acceptors, to further increase the scope of this methodology. In particular, the enantioselective conjugate addition of acyl or formyl anions to a,b-unsaturated carbonyl compounds or related derivatives entails a particular interest because this transformation allows the preparation of 1,4-dicarbonyl compounds, which are classically much more difficult to access by standard C À C bond forming reactions than the corresponding 1,3-or 1,5-dicarbonyl compounds.[4] However, despite the enormous potential of the oxime moiety and the key role played by this functional group in plenty of organic reactions, the development of umpoled reagents that behave as hydroxymoyl anion equivalents remains unexploited.In fact, even for the related case of the conjugate addition of acyl/formyl anion equivalents, enantioselective versions for this particular transformation under metal-free conditions are very scarce (see Scheme 1). For example, the Stetter reaction using N-heterocyclic carbenes (NHC) as catalysts can be an extremely effective approach for the formal enantioselective conjugate addition of acyl anions, [5] but it is ineffective when trying to use formaldehyde as the Michael donor.For the particular case of the conjugate addition of a formyl anion equivalent, there is only one single example related to an enantioselective organocatalytic version; this involves the use of N,N-dialkylhydrazones as Michael donors, which undergo conjugate addition to b,g-unsaturated a-ketoesters under chiral Brønsted-acid catalysis to give moderate levels of enantioselection.[6] Another relevant example involves oxazol-5A C H T U N G T R E N N U N G (2 H)-ones as aryloyl anion equivalents in the conjugate addition to enoylphosphonates, [7] which also relies on Brønsted-acid catalysis. In...

show abstract

“…82,83 However, total or semi-synthetic chemical routes have been considered. 84,85 As an example, the preparation of lovastatin (56) and analogue compounds has been reported 86 via a regioselective enzymatic esterification of the commercially available diol (57) with the (S)-( þ )-2-methylbutyric acid (58) (Scheme 12).…”

Section: (Hmg-coa) Reductase Inhibitorsmentioning

confidence: 99%

Recent advances in the chemistry of parainfluenza‐1 (Sendai) virus inhibitors

Saladino

Ciambecchini

Nencioni

et al. 2003

Medicinal Research Reviews

View full text Add to dashboard Cite

show abstract

Total synthesis of both (+)-compactin and (+)-mevinolin. A general strategy based on the use of a special titanium reagent for dicarbonyl coupling

Cited by 88 publications

References 3 publications

Chiral Syn-1,3-diol Derivatives via a One-Pot Diastereoselective Carboxylation/ Bromocyclization of Homoallylic Alcohols

Chiral Syn-1,3-diol Derivatives via a One-Pot Diastereoselective Carboxylation/ Bromocyclization of Homoallylic Alcohols

Organocatalytic Enantioselective Formal Conjugate Addition of a Hydroxymoyl Anion to α,β‐Unsaturated Aldehydes

Recent advances in the chemistry of parainfluenza‐1 (Sendai) virus inhibitors

Contact Info

Product

Resources

About