Novel Route to 4-Aryl Coumarins

A novel route to 4-aryl coumarins using the palladium-catalyzed coupling ofaryl stannanes with 4-trifluoromethanesulfonyloxy coumarin is described     

A new cyclisation involving cyclopropyl ketones. A short route to 1-aryltetralones.

Activated aryl aroylcyclopropanes cyclise with Lewis acids under mild conditions to 1-aryltetralones.     

Convenient ketone synthesis via n-acylaziridines

N-Acylaziridines couple efficiently with organolithium and Grignard reagents to produce ketones in high yields.     

Reductive cleavage of cyclopropyl ketones

Aryl substituted cyclopropyl ketones are cleaved to acyclic ketones with zinc and zinc chloride or with zinc alone in refluxing alcohol.     

Bengamides revisited: new structures and antitumor studies

The structural chemistry and biological activity of the bengamide class of compounds have been further characterized. Extracts prepared from recollected Jaspis cf. coriacea from five sites in Fiji were pooled. Six new bengamides, M (7b), N (8a), O (8b), P (9a), Q (9b), and R (10), were identified, accompanied by the known bengamides A (1a), B (1b), E (3a), F (3b), Y (5), Z (6), L (7a), G (11a), H (11b), and I (12). The structures of the new compounds were determined from spectroscopic data, and some were additionally confirmed by semisynthesis. Cytotoxicity screening data were obtained from the NCI-DTP 60 cell screen for bengamides A, B, and P. Bengamides A and B were more potent than bengamide P, with average IC(50) values of 0.046, 0.011, and 2.70 FM, respectively. The in vitro antitumor activity against MDA-MB-435 human mammary carcinoma was also determined for natural bengamides A, B, E, F, P, M, O, and Z and for synthetic samples of B and O. The best activity was observed for the natural bengamides A (IC(50) = 1 nM) and O (IC(50) = 0.3 nM).     

Total syntheses of bengamides B and E

Total syntheses of the cytotoxic marine natural products bengamides B and E are described. Both bengamides are prepared via amide coupling of a protected polyhydroxylated lactone intermediate 9 with a suitably substituted aminocaprolactam intermediate. Lactone 9 is prepared in five steps from commercially available alpha-D-glucoheptonic gamma-lactone. The key reactions are a selective deprotection of a 1,2-acetonide in the presence of a 1,3-acetonide and an (E)-selective olefination of an unstable aldehyde using a gem-dichromium reagent. The bengamide B lactam intermediate 10 is prepared in seven steps from commercially available (5R)-5-hydroxy-L-lysine (12). The desired S-configuration at the gamma-OH lactam position is established using the Mitsunobu reaction.     

Alkylation of metallated ketene thioacetals. Effect of the hardness of the leaving group and electrophile

The harder the leaving group or the Lewis acid end of the alkylating agent, the higher the proportion of C-1 alkylation of lithium ketene thioacetal (6).     

Zone fluidics for measurement of octanol–water partition coefficient of drugs

A novel zone fluidics (ZF) system for the determination of the octanol–water partition coefficient (P_ow) of drugs was developed. The ZF system consisted of a syringe pump with a selection valve, a holding column, a silica capillary flow-cell and an in-line spectrophotometer. Exact microliter volumes of solvents (octanol and phosphate buffer saline) and a solution of the drug, sandwiched between air segments, were sequentially loaded into the vertically aligned holding column. Distribution of the drug between the aqueous and octanol phases occurred by the oscillation movement of the syringe pump piston. Phase separation occurred due to the difference in densities. The liquid zones were then pushed into the detection flow cell. In this method, absorbance measurements in only one of the phase (octanol or aqueous) were employed, which together with the volumes of the solvents and pure drug sample, allowed the calculation of the P_ow. The developed system was applied to the determination of the P_ow of some common drugs. The log (P_ow) values agreed well with a batch method (R² = 0.999) and literature (R² = 0.997). Standard deviations for intra- and inter-day analyses were both less than 0.1log unit. This ZF system provides a robust and automated method for screening of P_ow values in the drug discovery process.