1388152-97-3

Basic information

• Product Name: C₃₂H₄₃IO₃Si
• Synonyms: C₃₂H₄₃IO₃Si
• CAS NO: 1388152-97-3
• Molecular Weight: 630.682
• Mol File: 1388152-97-3.mol

Chemical Properties

• CAS DataBase Reference: C₃₂H₄₃IO₃Si(CAS DataBase Reference)
• NIST Chemistry Reference: C₃₂H₄₃IO₃Si(1388152-97-3)
• EPA Substance Registry System: C₃₂H₄₃IO₃Si(1388152-97-3)

Safety Data

• Hazardous Substances Data: 1388152-97-3(Hazardous Substances Data)

Upstream product

• 2186-92-7 p-Anisaldehyde dimethyl acetal 
• 1388153-39-6 C₃₂H₄₄O₄Si 
• 1388153-35-2 C₂₄H₃₆O₃Si 
• 1388153-33-0 C₃₄H₄₃NO₅Si 

Downstream Products

• 1388152-99-5 C₄₈H₇₂O₇Si₂ 
• 1388153-00-1 C₄₈H₇₁BrO₇Si₂ 
• 1388153-01-2 C₄₈H₇₂O₇Si₂ 
• 1388153-41-0 C₂₆H₄₀O₇ 
• 1388153-43-2 C₅₉H₆₄O₇ 
• 1388152-98-4 C₅₆H₈₀O₈Si₂ 

Relevant articles and documents

Total synthesis and biological evaluation of (+)-gambieric acid A and its analogues

In this study, we report the first total synthesis and complete stereostructure of gambieric acid A, a potent antifungal polycyclic ether metabolite, in detail. The A/B-ring exocyclic enol ether 32 was prepared through a Suzuki-Miyaura coupling of the B-ring vinyl iodide 18 and the alkylborate 33 and subsequent closure of the A-ring by using diastereoselective bromoetherification as the key transformation. Suzuki-Miyaura coupling of 32 with acetate-derived enol phosphate 49, followed by ring-closing metathesis of the derived diene, produced the D-ring. Subsequent closure of the C-ring through a mixed thioacetalization completed the synthesis of the A/BCD-ring fragment 8. The A/BCD- and F′GHIJ-ring fragments (i.e., 8 and 9) were assembled through Suzuki-Miyaura coupling. The C25 stereogenic center was elaborated by exploiting the intrinsic conformational property of the seven-membered F′-ring. After the oxidative cleavage of the F′-ring, the E-ring was formed as a cyclic mixed thioacetal (i.e., 70) and then stereoselectively allylated by using glycosylation chemistry. Ring-closing metathesis of the diene 3 thus obtained closed the F-ring and completed the polycyclic ether skeleton. Finally, the J-ring side chain was introduced by using a Julia-Kocienski olefination in the presence of CeCl3 to complete the total synthesis of gambieric acid A (1), thereby unambiguously establishing its complete stereostructure. The present total synthesis enabled us to evaluate the antifungal and antiproliferative activities of 1 and several synthetic analogues. Copyright

Total synthesis and complete stereostructure of gambieric acid A

Total synthesis of gambieric acid A, a potent antifungal polycyclic ether metabolite, has been accomplished for the first time, which firmly established the complete stereostructure of this natural product.