Research Journal of Chemical Sciences ______________________________________________ ISSN 2231-606X Vol. 4(11), 18-22, November (2014) Res. J. Chem. Sci.International Science Congress Association 18 Synthesis and Characterization of Derivative derived from 1, 4-Dihydropyrimidine Shaikh Saad Salim and Shaikh Saud SalimAKI Poona College of Arts, Commerce and Science, Camp Pune-411001, Maharashtra, INDIA Gokhale Education Society Arts, Commerce and Science College Shrivardhan-402110, Maharashtra, INDIAAvailable online at: www.isca.in, www.isca.me Received 10th October 2014, revised 2nd November 2014, accepted 11th November 2014 AbstractIn our present work A new modification in biginelli product has been developed and formation as well as characterization of ethyl 2-(butylsulfanyl)-4- (4-hydroxyphenyl) -6-methyl-1, 4-dihydropyrimidine-5- carboxylate, ethyl-4- (4-bromophenyl)-2- (butylsulfanyl)-6-methyl-1, 4-dihydropyrimidine-5-carboxylate, ethyl-2-(butylsulfanyl)-6-methyl-4-phenyl-1, 4-dihydropyrimidine-5-carboxylate, ethyl2-(butylsulfanyl)-4- (4-fluorophenyl)-6-methyl-1, 4-dihydropyrimidine-5-carboxylate, ethyl-2-(butylsulfanyl)-6-methyl-4 (3-nitrophenyl)-1, 4-dihydropyrimidine-5-carboxylate. Involving linkage of n-butyl group to Sulphur atom which is having the same biological activity. The compound obtain in the first stage was subjected for further reaction with n-butyl bromide in presence of weak base pyridine. Keywords: Dihydropyrimidine, pyridine, AlCl3, EAA, thiourea, methanol, ethanol. Introduction Multicomponent reaction are the reactions which are having less hazardous impact on environment, because of which this reaction plays dominating role in chemical science, this are the reaction in which more than two component react in at a same time to give a product with effective atom economy so far manufacturing units are concerned the reaction was first proposed by bignelliand is referred to as Biginelli Reaction, multicomponent reaction is an important tool in designing the drug such as dihydropyrimidine DHPM which are having Anti carcinogenic, antiviral anti mitotic properties. Various modifications are done since biginelli first proposed it involving various catalyst for improving the rate of reaction many such catalyst are AlCl3, FeCl3. 6HO, Lewis Acid catalyst including Mg(ClO) lanthanide series catalyst the nano catalyst were also used to improve rate and yield of the given reaction. The vast biological activities of this drug have attracted the attention of synthetic organic chemist to synthesize this molecule. As a part of our research in synthesizing the compound derive from DHPM4 in our present work we have carried out the reaction involving DHPM and n butyl bromide linking the n Butyl group to sulphur atom in dihydro pyrimidine-2-thione ,and this compound also shows same biological activity such as DHPMExperimental details: The Chemicals used Are SD Fine Chemicals and are used without purifying them. The melting Point of synthesize compound was recorded in capillary sealed at one end and were uncorrectedH NMR (200MHz) spectra was recorded using AVANCE200 spectrophotometer having chloroform-d the solvent and tri methyl silane as standard reference, IR Spectrum was recorded on Nicolet IS5 FTIR using Germanium CrystalMethodology General Procedure of Synthesis Butyl Derivative of Di Hydro Pyrimidine, Stage 1: A mixture of the substituted derivative of benz aldehyde 1mol, Thiourea 1.2mol, ethyl acetoacetate (EAA) 1.0mol was taken in a round bottom flask fitted with a condenser and caped with a guard tube added a catalytic amount of AlCl and HCl 0.2mol, the solvent used was methanol the reaction mixture was heated and stirred and monitor the reaction using TLC till the product gets formed pour the reaction mixture in an ice cooled distilled water and stir until the product get precipitate outs as a white powder dry the compound and recrystallized it by hot ethanol and record the melting point. Stage 2: Taken the compound obtain in first stage in 1mol, butyl bromide 1mol, methanol as solvent in a round bottom flask and sonicate by adding 6-8 drops of pyridine in a reaction mixture and monitor the reaction using TLC once the reaction gets complete separate it in an ice cold distilled water and dry the product and recrystallize by hot ethanol. Results and Discussion Spectral analysis of the synthesized compound: Spectral Data of Compound 4a: IR 3300-3150 cm-1 (NH), 1680-1653cm-1 (C=O, ester), 1611-1530cm-1 (Aromatic ring), 1495cm-1(C-O), 1130-1151cm-1(C-C): 1H NMR 7.25 ppm (s, Research Journal of Chemical Sciences ___________________________________________________________ ISSN 2231-606XVol. 4(11), 18-22, November (2014) Res. J. Chem. Sci. International Science Congress Association 19 chloroform-d), 7.23ppm (multiplet, 5H), 4.2ppm (quartet,2H), 3.2ppm (bs,NH), 2.8ppm (triplet, 2H, S-CH), 2.3ppm (singlet, 3H, CH), 2.15ppm (singlet, 1H, C#H), 1.6ppm (multiplet, 2H, CH), 1.3ppm (multiplet, 2H, CH) 1.1ppm (triplet, 3H. CH) 0.9 ppm (triplet, 3H, CH) (# chiral proton). Spectral Data of Compound 4b: IR 3470-3459cm-1(OH) 3300-3150 cm-1 (NH),1670-1645cm-1(C=O,ester), 1615-1540cm-1 (Aromatic ring), 1435cm-1(C-O), 1168-1126cm-1(C-C): 1H NMR 7.25ppm (singlet, chloroform-d), 7.1ppm (doublet, 2H, Ar-H), 6.75ppm (doublet, 2H, Ar-H) 5.45ppm (bs, 1H, OH) 4.4ppm (quartet, 2H), 3.1ppm (bs, NH), 2.8ppm (triplet, 2H, S-CH), 2.1ppm (singlet, 3H, CH3), 2.0ppm (singlet,1H,C#H), 1.7ppm (multiplet, 2H, CH2), 1.2ppm (multiplet,2H,CH) 1.1ppm (triplet,3H.CH) 0.9ppm(triplet,3H,CH) (# chiral proton). Spectral Data of Compound 4c: IR 3300-3150 cm-1 (NH), 1670-1655cm-1 (C=O, ester), 1610-1570cm-1 (Aromatic ring), 1465cm-1(C-O), 1170-1153cm-1(C-C) 823cm-1(C-F): 1H NMR 7.25ppm (singlet, chloroform-d), 7.1ppm (doublet, 2H, Ar-H), 6.75ppm (doublet, 2H, Ar-H), 4.2ppm (quartet, 2H), 3.3ppm (bs, NH), 2.7ppm (triplet, 2H, S-CH), 2.4ppm (singlet, 3H, CH), 2.1ppm (singlet, 1H,C#H), 1.4ppm (multiplet, 2H,CH), 1.1ppm (multiplet, 2H,CH) 0.9ppm (triplet, 3H.CH) 0.8ppm (triplet,3H,CH) (# chiral proton). Spectral Data of Compound 4d: IR 3327-3126 cm-1 (NH),1667-1641cm-1(C=O,ester),1600-1530cm-1 (Aromatic ring), 1453cm-1(C-O), 1127-1056cm-1(C-C) 8231m-1(C-F): 1H NMR 7.25ppm (singlet, chloroform-d), 7.3ppm (doublet, 2H, Ar-H), 6.55ppm (doublet, 2H, Ar-H), 4.2ppm (quartet, 2H), 3.4ppm(bs, NH), 2.8ppm(triplet, 2H, S-CH), 2.4ppm (singlet, 3H, CH3), 2.15ppm (singlet, 1H, C#H), 1.7ppm (multiplet, 2H, CH), 1.3ppm (multiplet, 2H, CH) 1.0ppm (triplet, 3H.CH) 0.9ppm (triplet, 3H, CH) (# chiral proton). Spectral Data of Compound 4e: IR 3350-3116 cm-1 (NH), 1663-1612cm-1(C=O, ester), 1603-1523cm-1 (Aromatic ring), 1423cm-1(C-O), 1157-1032cm-1(C-C) 690-781cm-1(C-F) : 1H NMR 7.25ppm (singlet, chloroform-d), 7.9ppm(doublet, 1H, Ar-H), 7.6ppm (doublet, 1H, Ar-H), 7.4ppm (double doublet, 1H, Ar-H) 6.9ppm (double doublet, 1H, Ar-H) 4.1ppm (quartet, 2H), 3.23ppm (bs,NH), 2.6ppm (triplet, 2H, S-CH), 2.4ppm (singlet, 3H, CH), 2.1ppm (singlet, 1H, C#H), 1.5ppm (multiplet, 2H, CH), 1.3ppm (multiplet, 2H, CH) 1.0ppm (triplet, 3H.CH) 0.95ppm (triplet, 3H, CH) (# chiral proton). Table-1 Physical and Analytical Data for Compound 4a-4e Compound R Reaction Time step i (hr) Reaction Time step ii ( min) Yield MpC 4a H 6.8 67 74.12% 121-122 0 C 4b p-OH 5.6 72 67.89% 132-133 0 C 4c p-F 7.2 75 39.27% 134-136 0 C 4d m-NO 2 4.3 63 47.82% 146-147 0 C 4e p-Br 5.7 52 51.23% 113-115 0 C Scheme-1 General reaction R= -H, -NO, -OH, -F, - Research Journal of Chemical Sciences ___________________________________________________________ ISSN 2231-606XVol. 4(11), 18-22, November (2014) Res. J. Chem. Sci. International Science Congress Association 20 Br 7.5 7.0 6.5 6.0 5.5 5.0 4.5 4.0 3.5 3.0 2.5 2.0 1.5 1.0 0.5 0 0 0.1 0.2 0.3 0.4 0.5 0.6 0.7 0.8 0.9 1.0 3.003.993.593.740.760.622.131.162.182.17 Chloroform-d 7.25 7.09 6.70 4.11 4.07 2.35 2.16 1.56 1.22 1.19 1.15 0.86 Figure-1 NMR Spectra of 4b at 200MHz Figure-2 IR SPECTRA of 4a Research Journal of Chemical Sciences ___________________________________________________________ ISSN 2231-606XVol. 4(11), 18-22, November (2014) Res. J. Chem. Sci. International Science Congress Association 21 Figure-3 IR SPECTRA of 4b Figure-4 IR SPECTRA of 4c Research Journal of Chemical Sciences ___________________________________________________________ ISSN 2231-606XVol. 4(11), 18-22, November (2014) Res. J. Chem. Sci. International Science Congress Association 22 A clear and most efficient way of synthesizing various derivative of dihydro pyrimidine was performed with better yield and quality, various aspect of reaction was consider such as effect of different functional group namely electron donating and withdrawing effect which in some case cause reduce in the yield of the product, the compound synthesize could be furthered tested for its biological activity with anti-bacterial anti-carcinogenic properties Conclusion In conclusion we have illustrated the new reaction modifications involving biginelli product by reacting the dihydro pyrimidine with nbutyl bromide in presence of pyridine acting as a base, the second step of the reaction was carried using sonicator, it was found that methanol was effective solvent other than water. Application of this method can be widely used in synthesizing large number of such derivative having biological importance References 1.Biginelli P., Gazz. 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