177555-32-7

Basic information

• Product Name: (2E,4E,10E,12E)-13-Phenyl-trideca-2,4,10,12-tetraenoic acid ethyl ester
• Synonyms: (2E,4E,10E,12E)-13-Phenyl-trideca-2,4,10,12-tetraenoic acid ethyl ester
• CAS NO: 177555-32-7
• Molecular Weight: 310.436
• Mol File: 177555-32-7.mol
• Article Data: 1

Chemical Properties

• CAS DataBase Reference: (2E,4E,10E,12E)-13-Phenyl-trideca-2,4,10,12-tetraenoic acid ethyl ester(CAS DataBase Reference)
• NIST Chemistry Reference: (2E,4E,10E,12E)-13-Phenyl-trideca-2,4,10,12-tetraenoic acid ethyl ester(177555-32-7)
• EPA Substance Registry System: (2E,4E,10E,12E)-13-Phenyl-trideca-2,4,10,12-tetraenoic acid ethyl ester(177555-32-7)

Safety Data

• Hazardous Substances Data: 177555-32-7(Hazardous Substances Data)

Upstream product

• 177555-18-9 (6E,8E)-9-Phenyl-nona-6,8-dienoic acid 3-hydroxy-propyl ester 
• 177555-30-5 (6E,8E)-9-Phenyl-nona-6,8-dien-1-ol 
• 42516-28-9 ethyl (2E)-4-(diethoxyphosphoryl)crotonate 
• 177555-31-6 (6E,8E)-9-Phenyl-nona-6,8-dienal 

Downstream Products

• 18836-52-7 (2E,4E)-N-isobutyldecadienamide 
• 177555-33-8 13-phenyltrideca-2E,4E,10E,12E-tetraenoic acid 
• 30361-33-2 (2E,4E)-deca-2,4-dienoic acid 

Relevant articles and documents

Expedient synthesis of unsaturated amide alkaloids from Piper spp: Exploring the scope of recent methodology

The Sakai aryl aldehyde - cyclic ketone aldol - Grob fragmentation sequence was extended to cinnamaldehyde and cyclohexanone, and the product was elaborated to analogues of the alkaloid piperstachine. The effects of substituents on the reaction involving cinnamaldehyde were studied. The aldol-fragmentation sequence failed with benzaldehyde when cyclooctanone or cyclobutanone was substituted for cyclohexanone or cyclopentanone, and the reasons for this failure were examined. Four-carbon Wittig homologation of the piperonal-cyclobutanone aldol-fragmentation product, a hypothetical route to alkaloids such as retrofractamide A, was thus not viable. Instead, three-carbon homologation of the readily available piperonal-cyclopentanone product, using alkyne chemistry recently disclosed by Lu and Trost, afforded these alkaloids in excellent overall yield. The alkyne isomerization was also used to effect efficient syntheses of pellitorine and several other non-aromatic 2E,4E-dienoic Piper amide alkaloids. The Sakai aryl aldehyde - cyclic ketone aldol - Grob fragmentation sequence was extended to cinnamaldehyde and cyclohexanone, and the product was elaborated to analogues of the alkaloid piperstachine. The effects of substitutents on the reaction involving cinnamaldehyde were studied. The aldol-fragmentation sequence failed with benzaldehyde when cyclooctanone or cyclobutanone was substituted for cyclohexanone or cyclopentanone, and the reasons for this failure were examined. Four-carbon Wittig homologation of the piperonal-cyclobutanone aldol-fragmentation product, a hypothetical route to alkaloids such as retrofractamide A, was thus not viable. Instead, three-carbon homologation of the readily available piperonal-cyclopentanone product, using alkyne chemistry recently disclosed by Lu and Trost, afforded these alkaloids in excellent overall yield. The alkyne isomerization was also used to effect efficient syntheses of pellitorine and several other non-aromatic 2E,4E-dienoic Piper amide alkaloids.