80267-24-9

Upstream product

• 497-03-0 2-methylbut-2-enal 
• 59414-23-2 1-methoxy-3-<(trimethylsilyl)oxy>01,3-butadiene 
• 194233-66-4 (1E)-3-{[tert-butyl(dimethyl)silyl]oxy}-N,N-dimethyl-1,3-butadien-1-amine 
• 71735-01-8 1-methoxy-[3-(tert-butyldimethylsilyl)oxy]-1,3-butadiene 
• 111724-12-0 (1R,6S)-2-Methoxy-1,6-dimethyl-4-oxo-cyclohexanecarbaldehyde 

Downstream Products

• 111724-14-2 4β-formyl-3β,4α,5α-trimethylcyclohexanone 
• 87927-55-7 4β(2'-1',3'-dithiolan)-4α,5α-dimethylcyclohex-2-enone 
• 62640-05-5 ajugarin I 
• 90020-40-9 4α,5α-dimethyl-4β-(E)-(2'-phenylsulphonyl)vinyl-1α-t-butyldimethylsilyloxycyclohex-2-ene 
• 90020-38-5 4α,5α-dimethyl-4β-formyl-1α-t-butyldimethylsilyloxycyclohex-2-ene 
• 87927-67-1 (6α,18-dihydroxy)acetonide-12-phenylsulphonylcleroda-4,13(14)-dieno-16,15-lactone 
• 111724-22-2 3-<1-phenylsulphonyl-2-(1α,6α-dimethyl-4α-t-butyldimethylsilyloxycyclohex-2-enyl)-ethyl>but-2-en-4-olide 
• 87927-66-0 4α,5α-dimethyl-<(2α-hydroxy-1α-hydroxymethyl)-acetonide>-10β-phenylselenomethyl-5β-(2''-phenylsulphonyl)ethyl-6β-bicyclo<4.4.0>decane 
• 87927-64-8 4α,5α-dimethyl-<(2α-hydroxy-1α-hydroxymethyl)-acetonide>-5β-(E)-(2''-phenylsulphonyl)vinyl-10β-vinyl-6β-bicyclo<4.4.0>decane 
• 87927-69-3 4α,5α-dimethyl-<(2α-hydroxy-1α-hydroxymethyl)-acetonide>-5β-(2''-phenylsulphonyl)ethyl-10β-vinyl-6β-bicyclo<4.4.0>decane 
• 87927-65-9 4α,5α-dimethyl-<(2α-hydroxy-1α-hydroxymethyl)-acetonide>-10β-hydroxymethyl-5β-(2''-phenylsulphonyl)ethyl-6β-bicyclo<4.4.0>decane 
• 87927-68-2 4α,5α-dimethyl-<(2α-hydroxy-1α-hydroxymethyl)-acetonide>-10-methylene-5β-(2''-phenylsulphonyl)ethyl-6β-bicyclo<4.4.0>decane 
• 111724-21-1 4α,5α-dimethyl-4β-(2'-phenylsulphonyl)ethyl-1α-t-butyldimethylsilyloxycyclohex-2-ene 
• 111724-23-3 3-<2-(1α,6α-dimethyl-4α-t-butyldimethylsilyloxycyclohex-2-enyl)ethyl>but-2-en-4-olide 

Relevant academic research and scientific papers

Total Syntheses of Scaparvins B, C, and D Enabled by a Key C-H Functionalization

The clerodane diterpene family possesses an impressive range of bioactivities and high synthetic challenge due to their unique amalgamation of rings, stereocenters, and oxygenation. Herein, we disclose the first total syntheses of three members, scaparvin

Constructing the architecturally distinctive ABD-tricycle of phomactin A through an intramolecular oxa-[3+3] annulation strategy

Our efforts in constructing the ABD-ring of phomactin A through an intramolecular oxa-[3+3] annulation strategy is described. This struggle entailed finding a practical and efficient preparation of annulation precursor, and a realization of the unexpected competing regioisomeric pathway. The success entailed accessing the A-ring through Diels-Alder cycloaddition of Rawal's diene. Furthermore, the discovery that the regioisomers from the annulation existed as atropisomers with respect to the D-ring olefin and that they could be equilibrated to the desired ABD-tricycle, allowing large quantities of tricycle to be accessed.

TOTAL SYNTHESIS OF THE INSECT ANTIFEEDANT AJUGARIN I AND DEGRADATION STUDIES OF RELATED CLERODANE DITERPENES

The first total synthesis of the diterpene clerodane insect antifeedant ajugarin I (1) has been achieved.The key step of the synthesis discloses the use of the 1,3-dithiolane unit to stereochemically direct the conjugate addition of a but-3-enyl cuprate to set in place the C-10 sp3 carbon centre.The trans-fused ring geometry was obtained by conjugate addition of a vinyl cuprate to an enone and regio and stereoselectively trapping the resulting enolate with formaldehyde.Introduction of the necessary butenolide side chain was achieved by conjugate addition of a sulphone stabilised anion to ethyl-4-(t-butyldimethylsilyloxy)but-2-ynoate followed by work-up with fluoride.Final hydroxyl directed epoxidation was not specific giving both the natural product ajugarin I and its 4-epi isomer.Chemical modification of the insect antifeedant clerodin hemiacetal afforded a series of side chain modified structures for biological evaluation.