88932-32-5

Upstream product

• 917-64-6 methyl magnesium iodide 
• 764-59-0 hex-5-en-1-al 
• 7103-09-5 4-but-1-enylmagnesium bromide 
• 15448-47-2 (R)-propylene oxide 
• 5162-44-7 1-bromo-4-butene 
• 852065-86-2 (R)-6-hepten-2-ol acetate 
• 106-95-6 allyl bromide 
• 16088-62-3 (S)-Propylene oxide 
• 121671-81-6 (5R)-5-[1-(tert-butyl)-1,1-diphenylsilyl]oxyhexan-1-ol 
• 929554-07-4 (R)-6-benzyloxy-hex-4-yn-2-yloxy-tert-butyldiphenylsilane 
• 174455-52-8 (R)-6-(benzyloxy)hex-4-yn-2-ol 
• 855256-87-0 (5R)-5-[1-(tert-butyl)-1,1-diphenylsilyl]oxyhexanal 
• 929554-08-5 (R)-tert-butyl(hept-6-en-2-yloxy)diphenylsilane 

Downstream Products

• 676604-35-6 2,4-Bis-benzyloxy-6-chloromethyl-benzoic acid (S)-1-methyl-hex-5-enyl ester 
• 944797-00-6 (R)-[[(1-methyl-5-hexenyl)oxy]methyl]-benzene 
• 402860-20-2 4-benzyloxybenzoic acid (r)-1-methyl-hex-5-enyl ester 
• 929554-08-5 (R)-tert-butyl(hept-6-en-2-yloxy)diphenylsilane 
• 1446490-37-4 C₃₄H₄₂O₆ 
• 1446490-38-5 C₆₁H₇₀O₁₁ 
• 1446490-36-3 C₃₆H₄₄O₇ 
• 1451475-96-9 (2R,3R,5R,6S)-2-(((R,E)-8-methoxy-8-oxooct-6-en-2-yl)oxy)-6-methyltetrahydro-2H-pyran-3,5-diyl dibenzoate 
• 1451476-08-6 (2R,3R,5R,6S)-2-(((R)-8-methoxy-8-oxooctan-2-yl)oxy)-6-methyltetrahydro-2H-pyran-3,5-diyl dibenzoate 
• 1451475-83-4 (2R,3R,5R,6S)-2-((R)-hept-6-en-2-yloxy)-6-methyltetrahydro-2H-pyran-3,5-diyl dibenzoate 
• 213818-72-5 (4S,8R)-4-(benzyloxy)-8-methyloxocan-2-one 
• 213818-71-4 (3S,7R)-3-(benzyloxy)-7-hydroxyoctanoic acid 

Relevant academic research and scientific papers

Total synthesis of both enantiomers of macrocyclic lactone aspergillide C

A facile approach to the total synthesis of both enantiomers of the 14-membered macrolactone aspergillide C is described. The strategy employed was also utilized for the synthesis of C4-epimers of both the enantiomers of aspergillide C. The key reactions include Sharpless kinetic resolution, Achmatowicz reaction, Ferrier type alkynylation, hydrosilylation- protodesilylation, Corey-Bakshi-Shibata (CBS) mediated reduction, and Yamaguchi macrolactonization.

Stereoselective total synthesis of diplodialide A

Abstract: An efficient stereoselective total synthesis of Diplodialide A has been achieved from inexpensive and commercially available starting material (R)-propylene oxide. This linear synthesis utilizes Wittig reaction, alkylation of 1,3-dithiane and Yamaguchi macrolactonization as key steps. Graphic abstract: [Figure not available: see fulltext.]

An alternative total synthesis of diplodialide-B

In this paper, an enantioselective synthesis of diplodialide-B has been described. To accomplish this target, a combination of regioselective ring opening of the chiral epoxide, Jacobsen hydrolytic kinetic resolution and Yamaguchi macrolactonization were used as the key steps.

Total synthesis and stereochemical revision of relgro and 10′-oxorelgro

The first asymmetric total synthesis and stereochemical assignments of 10-membered macrolactones relgro and 10′-oxorelgro are disclosed. To this end, palladium-catalyzed Stille coupling, the Mitsunobu reaction, ring-closing metathesis, EDCI promoted coupling and the Jacobsen hydrolytic kinetic resolution are used as key steps. The total synthesis followed by thorough evaluation of the optical rotation and CD spectral data led to the revision of the absolute configuration at C-6′ for both relgro and 10′-oxorelgro. Moreover, the 1H as well as 13C NMR data are reported for the first time for relgro.

A Unified Synthetic Approach to Optically Pure Curvularin-Type Metabolites

A unified and concise approach to the synthesis of nine curvularin-type metabolites and two analogues has been developed with few steps and high yields. Among them, sumalactones A-D were synthesized for the first time. The key steps in this approach inclu

Enantioselective synthesis of (2R,13R,8Z)-2,13-diacetoxy-8-heptadecene, the major component of the sex pheromone of the pear leaf midge, Dasineura pyri

The first enantioselective synthesis of (2R,13R,8Z)-2,13-diacetoxy-8-heptadecene 1, the major component of the sex pheromone of the pear leaf midge, Dasineura pyri, has been achieved. The key steps include the (R,R)-BINOL/Ti(OiPr)4catalyzed alkynylzinc addition to an unsaturated aldehyde, the ring-opening of the chiral epoxide with a Grignard reagent, and the partial reduction of an acetylenic diol ester to a (Z)-olefinic diol ester with hydrogen and P2-Ni.

Determination of the Absolute Configuration of Gliomasolide D through Total Syntheses of the C-17 Epimers

The absolute configuration at C-17, the carbon bearing the distal hydroxy group of the 14-membered natural product gliomasolide D, was assigned as R by comparison of 13C NMR shifts and specific rotation values of the epimers at C-17. The first

A concise stereoselective total synthesis of (-)-cephalosporolide D

A concise stereoselective total synthesis of eight-membered lactone (-)-cephalosporolide D has been derived from inexpensive and commercially available starting material (S)-propylene epoxide. This concise synthesis utilizes Grignard reaction, Noyori asym

Total synthesis of the Z -isomers of the proposed and revised structures of aspergillide B via an iodocyclization and ring-closing metathesis strategy

The synthesis of Z-isomers of both the proposed and revised structures of aspergillide B is described. A divergent route is employed that involves kinetically controlled ring-closing metathesis for the construction of a 14-membered macrocyclic ring, ester formation under Yamaguchi conditions, a Wacker-type oxidative cyclization for creation of the C4 stereogenic center and a previously reported diastereoselective isomerization-iodocyclization strategy for the construction of the 2,6-trans-disubstituted tetrahydropyran subunit. Georg Thieme Verlag Stuttgart, New York.

Total synthesis of nominal gobienine A

The lichen-derived glycoconjugate gobienine A is structurally more complex than most glycolipids isolated from higher plants by virtue of the all-cis substituted γ-lactone substructure embedded into its macrocyclic frame. A concise entry into this very epimerization-prone and hence challenging structural motif is presented, which relies on an enantioselective cyanohydrin formation, an intramolecular Blaise reaction, a palladium-catalyzed alkoxycarbonylation, and a diastereoselective hydrogenation of the tetrasubstituted alkene in the resulting butenolide. This strategy, in combination with ring-closing olefin metathesis for the formation of the macrocyclic perimeter, allowed the proposed structure of gobienine A (1) to be formed in high overall yield. The recorded spectral data show that the structure originally attributed to gobienine A is incorrect and that it is not the epimerization-prone ester site on the butanolide ring that is the locus of misassignment; rather, the discrepancy must be more profound. Copyright