Spectral examination confirmed the identity of 2 as benzyl four hydroxy three,five dimethoxy benzoate and that of 3 as benzyl 4 three,five dimethoxybenzoate. This reaction and chromatographic processes were scaled up and repeated a number of Inhibitors,Modulators,Libraries occasions to afford quantities ample to evaluate their biological actions. Derivative 2, yield, 2. 6%, IR ν max 3345, 1725, 1H NMR see Table two, supplemental information, 13C NMR see Table 2, supplemental data, Substantial resolution ESIMS m z Derivative 3, yield, 1. 3%, IR ν max 1727, 1H NMR see Table three, supplemental data, 13C NMR see Table 3, supple mental data, High resolution ESIMS m z 378. 1421. 3 Methoxybenzyl three,five dimethoxy four benzoate and three methoxybenzyl four hydroxy three,5 dimethoxybenzoate Likewise, these derivatives were synthesized as men tioned above, even so, three methoxybenzylbromide was applied, as an alternative.
Removal any other enquiries of un reacted syringic acid was achieved through adding saturated solution of sodium carbonate and extraction with chloroform. Evap oration of chloroform layer yielded 1. 03 g of a yellowish syrupy residue. This residue gave, after purification, pure derivatives 4 and five as pale yellow oils. Derivatives four and 5 identities had been deduced from their spectral information. The reaction and purification processes had been repeated to yield 93 mg of 4 and 131 mg of five. Derivative 4, yield, one. 5%, IR ν max 1727, 1H NMR see Table 3, supplemental data, 13C NMR see Table 3, supple mental data, Large resolution ESIMS m z 438. 1648. Derivative 5, yield, 3%, IR ν max 3340, supplemental data, 13C NMR see Table two, supplemental information, Large resolution ESIMS m z 318. 1110.
3,5 dimethoxybenzyl selleck kinase inhibitor four hydroxy three,five dimethoxy benzoate Following the above procedure, three,five dimethoxybenzyl bromide was utilized. This reaction was sluggish and under no circumstances went to completion. Response workup, afforded 0. 166 g of the yellowish syrupy residue which upon purification gave 5. 4 mg of 6. Derivative 6 identity was confirmed from spectral analysis to be 3,five dimethoxybenzyl 4 hydroxy 3,5 dimethoxybenzoate. Reaction scale up afforded 52 mg of pure 6. Derivative 6, yield, 1%, IR ν max 3340, 1721, 1H NMR see Table two, supplemental data, 13C NMR see Table two, supplemental information, Higher resolution ESIMS m z 348. 1200. Biological activity Cell Culture All cell lines had been obtained from ATCC. Human colorectal cancer cell lines and Human breast cancer cell lines had been cultivated in Leibovitzs L15 medium, 90%, fetal bovine serum, 10%.
L15 medium formulation is devised for use in a free of charge gasoline exchange with atmospheric air. Human melanoma cell lines were cultivated in minimum essential med ium Eagle with 2 mM L glutamine and Earles BSS ad justed to have one. 5 g L sodium bicarbonate, 0. one mM non critical amino acids, 0. one mM sodium pyruvate and Earls BSS, 90%, foetal bovine serum, 10%. Ordinary human fibroblast cells were culti vated in Eagle modified vital medium and foetal bovine serum, 10%. Dose dependent anti mitogenic impact of syringic acid derivatives The antimitogenic effects of syringic acid derivatives 2 six toward panel of various human cancer cell lines com prised of colorectal, breast, breast, and melanoma cancer cell lines too as usual human fibroblast CRL1554 cells have been examined as previously described.
Human cancer cell lines and normal hu man fibroblast cells had been plated in 96 very well microtiter plates at a cell density of 27x103cells very well. Cells were in the treatment time period, the media have been discarded and one hundred ul properly of MTT was then added and also the plate was incubated for 4 h at 37 C. The MTT resolution was then aspirated along with the formazan crystals had been dissolved in 200 ul effectively of one,1 answer of DMSO, ethanol for 20 min at ambient temperature. Transform in absorbance was deter mined at A540 and 650 nm. Derivatives 2, 5 and 6 had been retested for his or her antimitogenic actions towards human malignant melanoma cancer cell lines HTB66 and HTB68 and typical human fibroblast CRL1554 after 24 h of deal with ment as stated above.