88 | Chemistry 2015) عام 1العدد ( 28مجلة إبن الھيثم للعلوم الصرفة و التطبيقية المجلد Ibn Al-Haitham J. for Pure & Appl. Sci. Vol. 28 (1) 2015 Synthesis of Some New Heterocyclic Compounds Via Chalcone Derivatives Muna S. Al-Rawi Dept.of Chemistry / College of Education For Pure Sciences( Ibn Al- Haitham)/ University of Baghdad Received in: 1 September 2014, Accepted in: 7 December 2014 Abstract The chalcones 1( a,b) were prepared by the reaction of 2- acetyl benzofuran with two aromatic aldehydes in the presence of alkaline media. These chalcones are used as starting material to obtain the desired heterocyclic: pyrazolin, isoxazoline, pyrimidinthion, pyrimidinone, cyclohexanone and indazole derivatives. The structure of newly synthesized heterocyclic compounds were established on the basis of their melting points, elemental analysis(C.H.N), FTIR and 1HMNR (for some of them) spectral data . The synthesized compounds have been screened for their antibacterial activities, they exhibited good antibacterial activity against Escherichia coli (G-) and Staphylococus aureus (G+) . Key Words: chalcones, pyrazoline, isoxazoline, pyrimidinone, pyrimidinthion cyclohexanone and indazole. 89 | Chemistry 2015) عام 1العدد ( 28مجلة إبن الھيثم للعلوم الصرفة و التطبيقية المجلد Ibn Al-Haitham J. for Pure & Appl. Sci. Vol. 28 (1) 2015 Introduction Chalcones represent an essential group of natural as well as synthetic products and some of them have wide range of pharmmacological activity such as anti-inflammatory, anti-fungal, antibacterial and anti-oxidnt agents [1-3]. Chalcones were used to afford pharmacologically- interesting heterocyclic systems like pyrazolines, isoxazoles and pyrimidines, cyclohexanone . Pyrazolines for example are known to have anti-bacterial[4], anti-tumor[5], anti- histaminic[6] and anti-convulsant activity[7] , while isoxazole exhibit anti-microbial, anti- cancer[8] and analgesic activity[9]. Pyrimidines are associated with various biological activities like anti- inflammatory and analgesic activity[10]. Indole derivatives are reported to possess antibacterial, anti -cancer, anti-inflammatory[11] . Hence, it appeared of interest to prepare new derivatives of the mentioned nucleouses. Experimental Materials All chemicals were supplied from Merck , Fluka and Aldrich Chemicals Co. and used as received . Techniques FTIR spectra were recorded using potassium bromide discs on a Shimadzo (IR prestige- 21) FTIR spectrophotometer . 1HNMR spectra were carried out by company : Bruker , model: ultra shield 300 MHz , origin : Switzerland and are reported in ppm(δ), DMSO was used as a solvent with TMS as an internal standard . Elemental analysis (C.H.N.S-O) were carried out using an EuroEA Elemental Analyzser at ( The Central Service Laboratory-College of Education For Pure Sciences Ibn Al- Haitham). Uncorrected melting points were determined by using Hot-Stage, Gallen Kamp melting point apparatus . 90 | Chemistry 2015) عام 1العدد ( 28مجلة إبن الھيثم للعلوم الصرفة و التطبيقية المجلد Ibn Al-Haitham J. for Pure & Appl. Sci. Vol. 28 (1) 2015     2-6 (a,b) 1(a,b) NH2NH2.- R CH3COCH2COOEt COOEtO N H N O 7(a,b) 8(a,b) NH2NH2. NH2OH.HCl 9(a,b) Ar 11(a,b) H N N S NH2CONH2 NH2CSNH2 O O + H Ar O O O Ar O O O N N Ar R O N Ar Ar H N N O O O Ar O Ar 10(a,b) 1a : Ar = OCH3 Cl 2a : Ar = R = H , Ph , N C O , NH2 C O , NH2 S NaOH EtOH Scheme(1) 91 | Chemistry 2015) عام 1العدد ( 28مجلة إبن الھيثم للعلوم الصرفة و التطبيقية المجلد Ibn Al-Haitham J. for Pure & Appl. Sci. Vol. 28 (1) 2015 Synthesis Synthesis of chalcones 1-(Benzofuran-2-yl)-3-(substituted phenyl) prop-2- ene-1-one (1a,b) [1] A mixture of aromatic benzaldehyde (0.01 mol) and 2-acetyl bezofuran (0.01 mol, 1.60 g) was dissolved in (10 mL) of ethanol, an aqueous soudium hydroxide solution (5 mL, 25%) was added. The mixture was stirred for 2-3hrs. at room temperature. The mixture was kept in a refrigerator for overnight when it became quite thick. Then it was diluted with ice-cold distilled water (40 mL), filtered, washed well with cold water, dried in air and recrystallized from ethanol to give the required product (2.26 g, 82%), mp 118-120oC. Synthesis of 3-(Benzofuran-2-yl) Pyrazoline derivatives 2-6(a,b) A mixture of chalcone 1(a,b) (0.01 mol) and hydrazine hydrate 99% (5mL, 0.01 mol) or substituted hydrazine hydrate (0.01 mol) in absolute ethanol (10 mL) containing glacial acetic acid (0.5 mL ) was refluxed for 2h[2]. After cooling, the solid formed was filtered off, air dried and recrystallized form absolute ethanol. The physical data of these compoundes are listed in Table 1. Anal. Calcd for (4a) C24H18N3O3: C, 72.72 ; H, 4.54; N, 10.60. Found: C, 73.23; H, 4.95; N, 9.87. Synthesis of 3-(Benzofuran-2-yl)isoxazoline derivatives 7(a,b) [8] To a mixture of chalcone (0.01 mol) and hydroxyl amine hydrochloride (0.01 mol , 0.69 g), absolute ethanol (50mL), aqueous sodium hydroxide (10%, 6 mL) were added then the reaction mixture was heated under reflux for 8h and poured slowly into ice cold water and the product obtained was washed with water and recrystallized from absolute ethanol. The physical data of these compoundes are listed in Table 1. Anal. Calcd for (7b) C17H12NO2Cl: C, 68.45; H, 4.02; N, 4.69. Found: C, 67.95; H, 3.87; N, 4.02. Synthesis of Pyrimidinethion derivatives 8(a,b) [5] To a solution of chalcone (0.01 mol) absolute ethanol (10 mL), thiourea (0.01 mol, 0.6 g) and aqueous sodium hydroxide (10 mL, 20.0 mmol) were added. The reaction mixture was heated under reflux for 7h and poured into iced cold water the product obtained was filtered, washed with water and recrystallized from absolute ethanol . The physical data of these compoundes are listed in Table 1. Anal. Calcd for (8b) C18H11N2OSCl : C, 63.71; H, 3.24; N, 8.25; S, 9.43. Found: C, 62.95; H, 3.65; N, 7.93 ;S,9.10. Synthesis of Pyrimidinone derivatives 9 ( a,b) [5]: To a solution of (0.01 mol) of chalcone, absolute ethanol (10 mL), urea (0.01 mol, 0.6 g) of aqueous sodium hydroxide (10mL, 10 %) were added. The reaction mixture was heated under reflux for 5h and poured in ice-cold water. The product obtained was filtered washed with water and recrystallized from ethanol (95%) . The physical data of these compoundes are listed in Table 1. Synthesis of Cyclohexanone derivatives 10(a,b) [11] : A mixture of chalcones (1a,b) (0.01 mol) and ethyl acetoacetate (1.30mL, 0.01mol) in absolute ethanol (10mL) containing aqueous potassium hydroxide solution (1 mL, 10%) was refluxed for 5h and then left overnight at room temperature. The solid formed was filtered off, air dried and recrystallized form absolute ethanol. The physical data of these compoundes are listed in Table 1. Anal. Calcd for (10a) C24H20O5: C, 74.22; H, 5.15.. Found: C, 74.87; H, 5.85. 92 | Chemistry 2015) عام 1العدد ( 28مجلة إبن الھيثم للعلوم الصرفة و التطبيقية المجلد Ibn Al-Haitham J. for Pure & Appl. Sci. Vol. 28 (1) 2015 Synthesis of Indazole derivatives 11(a,b) [11] A mixture of compounds10(a,b) (0.01 mol) and hydrazine hydrate 99% (5mL, 0.01 mol)in absolute ethanol (10 mL) containing glacial acetic acid (0.5 mL ) was refluxed for 2h. After cooling, the solid formed was filtered off, air dried and recrystallized form chloroform. The physical data of these compoundes are listed in Table 1. Anal. Calcd for (11a) C22H17N2O3: C, 73.94; H, 4.76; N, 7.84. Found: C, 73.11; H, 3.99; N, 7.21. Result and Discusion The synthesis of chalcones, pyrazoline, isoxazoline, pyrimidin -thion, pyrimidinon, cyclohexanone and Indazole derivatives were performed as shown in scheme (1). The starting chalcones, namely 1-(benzofuran-2-yl)-3-(4-methoxyphenyl) prop-2-ene-1- one (1a) and 1-(benzofuran-2-yl)-3-(2-chlorophenyl) prop-2-ene-1-one (1b), were synthesized via the Claisen- Schmidt reaction of 2-acetyl benzofuran with 4- methoxybenzaldehyde and 2- chlorobenzaldehyde, respectively, in ethanol and in the presence of aqueous soudium hydroxide at room temperature. The structural assignments of the chalcones 1(a,b) based on melting points and FTIR spectroscopy. The FTIR spectrum of chalcone (1a) indicated the appearance of two peaks at 1655cm¯¹and1573cm¯¹due to of C=O and C=C stretching vibrations ,respectively. peak at 1163 due to C-O-C . Also the FTIR spectrum of chalcone (1b) indicated the appearance of two peaks at 1666cm¯¹and1612cm¯¹due to of C=O and C=C stretching vibrations ,respectively. Reaction of chalcones 1 (a,b) with hydrazine hydrate, phenyl hydrazine, 2- pyridinecarboxylic acid hydrazide and 2-aminobenzo- hydrazide under reflux in the presence of glacial acetic acid to yield the corresponding pyrazoline derivatives 2-6(a,b), respectively. The structure of the pyrazoline derivatives 2-6(a,b) was identified by their melting point, C.H.N analysis, FTIR and 1HNMR spectroscopy. The FTIR spectra of these compounds showed the disappearce of two absorption bands of the CH=CH and C=O group , in the chalcone 1(a,b) and appearance of new absorption stretching bands of NH and C=N groups ( Table 2). 1HNMR spectrum of compound (2b), (Figure 1),  (in DMSO as a solvent) shows the following signals: a sharp singlet signal at δ 2.49ppm due to a proton of N-H group , sharp signals at δ 3.37ppm could be attributed to two protons of CH2 group- pyrazoline, a signal in the region δ 7.35ppm for furan ring conjugate with benzene ring, many signals(aromatic protons) appeared in the region δ 7.81-7.95 ppm. Isoxazoline compounds 7(a,b) were synthesized from the reaction of chalcones 1(a,b) with hydroxylamine hydrochloride in alkaline medium. The FTIR spectra of isoxazoline 7(a,b) showed the disappearance of two absorption bands of the CH=CH and C=O group in the starting material together with the appearance of new absorption bands for C=N group around 1610 cm¯¹and C-O (cyclic ether) group around 1178 cm¯1.  The FTIR spectral data for isoxazoline 7(a,b) are listed in Table( 2). (in DMSO as a solvent), showed  , Figure (2), HNMR spectrum of compound (7a)1 many signals(protons of aromatic protons) appeared in the region δ 7.04-8.25 ppm and a signal in the region δ 6.78ppm for furan ring conjugate with benzene ring. The triplet signal at δ 3.82ppm and a doublet signal at δ 3.68ppm due to one protons C-5 and two protons C-4 in for three protons a sharp signal at δ 3.56ppm Furthermore, respectively.ring, the isoxazoline group. 3of OCH Pyrimidinethion derivatives 8(a,b) were synthesized from the reaction of chalcones1(a,b) with thiourea in basic medium .The structure of the compounds 8(a,b) are characterized by FTIR and 1HNMR spectroscopy.The characteristic FTIR adsorption band of 93 | Chemistry 2015) عام 1العدد ( 28مجلة إبن الھيثم للعلوم الصرفة و التطبيقية المجلد Ibn Al-Haitham J. for Pure & Appl. Sci. Vol. 28 (1) 2015 pyrimidinethion showed the disappearance of two absorption bands of the CH=CH and C=O groups in the chalcones and appearance of new absorption bands for NH and C=S groups around 3384cm-1and 1136cm-1, respectively. The FTIR spectral data of these compounds are shown in Table 2 . 1HNMR spectrum of pyrimidinethion (8a) , Figure (3),  exhibited eight aromatic protons appeared as many pairs of doublet at δ 6.99-7.91ppm, a singlet signal at δ6.785ppm for furan ring conjugate with benzene ring, a singlet doublet at δ 6.780ppm for proton at C-5 of pyrimidinethion ring. A sharp singlet at δ 3.36ppm due to three protons of OCH3 group. a singlet at δ 2.51ppm that could be attributed to one proton of NH group .   The pyrimidinone derivatives 9 ( a,b) were synthesized from reaction of chalcone 1(a,b) with urea in basic medium. The structure of the pyrimidinone 9(a,b) characteristic by FTIR spectra which showed the disappearance of two absorption bands and appearance of new absorption bands for NH and C=O groups around 3338cm-1and 1665cm-1, respectively. The other data of functional groups which are characteristic of these compounds are given in Table 2. 1HNMR spectrum of compound (9b), Figure (4), shows the following signals: eight aromatic protons appeared at δ (7.07-7.88) ppm, a singlet signal at δ 6.75 ppm could be attributed to the one proton of C-5pyrimidinone and a singlet at δ 5.15 ppm due to the proton of C6-pyrimidinone. Allso, singlet broad signal one proton of NH group appeared as δ3.36 ppm . The chalcones 1(a,b) were allowed to react with ethyl acetoacetate (1:1) in the presence of aqueous potassium hydroxide10% to give new cyclohexanone derivatives 10 ( a,b). The structure of the cyclohexanone 10(a,b) was identified by their melting point, C.H.N analysis, FTIR and 1HNMR spectroscopy . The FTIR spectral data of these compounds are shown in Table 2. 1HMNR spectrum of compound (10b), shows the following signals: eight aromatic protons appeared in the region δ 7.01-7.87 ppm . The quartet singnal at δ 4.42ppm that are attributed to two protons of CH2 CO groups and a triplet signal at δ 1.61 ppm is due to three protons of CH3CH2CO. Four protons of CHCHCH2 cyclohexanone appears as multiplet at δ 3.55 ppm . The reaction may have proceeded through condensation between C=O of cyclohexanone and NH2 of hydrazine, followed by cyclization by losing a molecule of ethanol. The new indazole derivatives 11(a,b) were synthesized by refluxing compounds 10(a,b) and hydrazine in the presence of glacial acetic acid. The FTIR spectra of these compounds showed the disappearce of absorption bands and appearance of new absorption bands of NH and C=N group at 3363cm¯¹ and 1603cm¯¹, respectively. Functional groups which are characteristic of these compounds are given in Table 2. Finally, the 1HNMR spectrum of compound (11a) (in DMSO),  shows the following signals: eight aromatic protons appeared in the region δ 7.20-8.73 ppm. a singlet signal at δ 6.80ppm for furan ring conjugate with benzene ring. a signal at δ 3.12 ppm that are attributed to cyclohexanone protons . Furthermore, a singlet signal at δ 2.93ppm which was assigned to proton of NH .   Biological Activity All the synthesized compounds were tested for their antimicrobial activity against Gram negative bacteria (Escherichia Coli) and Gram positive bacteria (Staphylococcus aureus) using the agar diffusion method [11]. Each compound was dissolved in DMSO to give concentration 1ppm. The plates were then incubated at 37 0C and examined after 24 hrs. The zones of inhibition formed were measured in millimeter and are represented by (-),(+), (+ +) and (+ + +) depending upon the diameter and clarity as in Table 3. All the compounds exhibit the highest or lower biological activity against both of the organisms . 94 | Chemistry 2015) عام 1العدد ( 28مجلة إبن الھيثم للعلوم الصرفة و التطبيقية المجلد Ibn Al-Haitham J. for Pure & Appl. Sci. Vol. 28 (1) 2015 All compounds showed good inhibition against the two types of the bacteria, this could be related to the presence of heterocyclic rings . References 1- Jadhav, F. Y.; Bhosale, R.B.; Shirame, S. P.; Hublikar, M. G., Sonawane, K.D. and Shaikh, R.V., (2013),"Synthesis and biological evaluation of fluro-hydroxy substituted pyrazole chalcones as anti-inflammatory, anti-oxidant and anti- bacterial agents", Int. J. Pharm.Bio Sci., 4(2),. (309-397). 2- Hassan, S. Y., (2013),"synthesis, anti-bacterial and anti-fungale activity of some new pyrazoline and pyrazole derivatives" , Molecules, 18, p.2683-2711. 3- Kalirajan, R.; Sivakumar, S. V.; Jubie, S.; Gowramma,B. and Suresh,B., (2009),"Synthesis and biological evalution of some heterocyclic derivatives of chalcones", Int. J. of Chem. Tech. Res. , 1 (1), 27-34, Jan-March,. 4- Abdulla, M. Asiri and Salman, A. Khan, (2011),"Synthesis and antibacterial activities of a bis-chalcone derived from thiophene and its bis –cyclized product", Molecules, 16,. 523- 531. 5- Nassar, E.,( 2010), "Synthesis , (invitro) antitumor and antimicrobial activity of some pyrazoline, pyridine and pyrimidine derivatives linked to indole moiety", J. of American Science, 6(8). 6- Rahman, S. A., Rangjendra, Y., Bhvvaneswari, K. and Kumar, P., (2012)," Synthesis and antihistaminic activity of novel pyrazoline derivatives, Int. J. of Chem. Tech. Res. ,.2,.1,. 16-20. 7- Iddiqui ,A. A. S.; Rahman, Md. A.; Shaharyar, Md.; Ravinesh, M., (2010),"Synthesis and anticonvulsant activity of some substituted 3,5- diphenyl -2- pyrazoline-1 carboxamide derivatives ", Chemical Science Journal, CSJ-8. 8- Rhanage, S.; Mohite, P.; Pandhare, R. and Raju, A., (2012),"Synthesis and pharmacological evalution of isoxazole derivatives containing 1,2,4-triazole moiety", Marmara pharmaceutical Journal ,16, 134-140. 9- Runja, C.; Pavani, B.; Jaya Deepthi, G.; Sharma JVC and Vykuntam , (2013)," Synthesis characterization and an algesic activity of new osoxazole and pyrazole derivatives", J. of Pharmaceutical and Biological Sciences, 1(1), 8-11. 10- Joshi, V. D.; Kshiragar, M. D. and Singhal, S. , (2012),"Synthesis and Pharmacological study of some novel pyrmidines", Derpharmacia Sinica, 3(3), 343-348. 11- El-sawy, E. R.; Mandour, A. H.; Mahmoud, K. I. and Mohamed, H., (2012),"Synthesis, antimicrobial and anti-cancer activities of some new N-ethyl, N-benzyl and N-benzoyl-3- indolyl heterocycles ", Acta Pharm. 62 , 157-179. 95 | Chemistry 2015) عام 1العدد ( 28مجلة إبن الھيثم للعلوم الصرفة و التطبيقية المجلد Ibn Al-Haitham J. for Pure & Appl. Sci. Vol. 28 (1) 2015 Table No. (1): Physical properties of synthesized compounds 2-11(a,b) Comp. No. Namecalture Molecular Formula M.P 0C Yield % Color 2a 4,5-dihydro-3-(1-benzofuran-2-yl)-5-(4- methoxyphenyl) -1H- pyrazole C18H15N2O2 180-182 78 Pale yellow 2b 4,5-dihydro-3-(1-benzofuran-2-yl)-5-(2- chlorophenyl) - 1H- pyrazole C17H12N2OCl 91-93 72 Yellow 3a 4,5-dihydro- 3-(1-benzofuran-2-yl)-5-(2- methoxyphenyl) -1-phenyl-1H- pyrazole C24H19N2O2 223-225 68 Pale Brown 3b 4,5-dihydro-3-(1-benzofuran-2-yl)-5-(2- chlorophenyl) -1-phenyl-1H- pyrazole C23H16N2OCl 174-176 67 Orange 4a 4,5-dihydro-3-(1-benzofuran-2-yl)-5-(4- methoxyphenyl) -1 (2-pyridine carboxylic acid ) -1H- pyrazole C24H19N3O3 124-126 77 Yellowis h Brown 4b 4,5-dihydro-3-(1-benzofuran-2-yl)-5-(2- chlorophenyl -1 (2- pyridine carboxylic acid )-1H-pyrazole C23H14N3O2Cl 89-91 75 Red 5a 4,5-dihydro- 3-(1-benzofuran-2-yl)-5-(4- methoxyphenyl) -1(2-aminobenzo ) - 1H-pyrazole C25H21N3O3 200-202 60 Pale yellow 5b 4,5-dihydro-3-(1-benzofuran-2-yl)-5-(2- chlorophenyl) -1(2-aminobenzo -1H- pyrazole C24H18N3O2Cl 138-140 68 Brownish Yellow 6a 4,5-dihydro- 3-(1-benzofuran-2-yl)-5-(4- methoxy phenyl) pyrazole-1- carbothioamide C19H16N3O2S 244-246 76 Off-white 6b 4,5-dihydro- 3-(1-benzofuran-2-yl)-5-(2- chlorophenyl) pyrazole-1- carbothioamide C18H13N3OClS 228-230 72 White 7a 3-(1-benzofuran-2-yl)-5-(4-methoxy phenyl)-4,5-dihydroisoxazole C18H15NO3 83-85 70 Yellowis h brown 7b 3-(1-benzofuran-2-yl)-5-(2-chloro phenyl)-4,5-dihydroisoxazole C17H12NO2Cl 151-153 66 bright Brown 8a 6-(1-benzofuran-2-yl)-4-(4-methoxy phenyl) pyrimidine- 2(1H)- thione C19H14N2O2 S 116-118 76 Brown 8b 6-(1-benzofuran-2-yl)-4-(2-chloro phenyl) pyrimidine- 2(1H)- thione C18H11N2OClS 90-92 75 Brownish yellow 9a 6-(1-benzofuran-2-yl)-4-(4-methoxy phenyl) pyrimidin -2(1H)- one C19H14N2O3 174-176 60 Yellowis h Brown 9b 6-(1-benzofuran-2-yl)-4-(2-chloro phenyl) pyrimidin -2(1H)- one C18H11N2O2Cl 183-185 64 Light brown 10a Ethyl-4-(1-benzofuran-2-yl)- 6- ( 4- methoxyphenyl)-2-oxocyclohexa-3- enecarboxylate C24H20O5 66-68 78 Green- Yellow 10b Ethyl-4-(1-benzofuran-2-yl)- 6- ( 2- chlorophenyl)-2-oxocyclohexa-3- enecarboxylate C23H17O4 Cl 127-129 65 Pale Brown 11a 4,5-dihydro-4-(4-methoxyphenyl)- 6-(1- benzofuran-2-yl)-2H-indazol-3(H)ones C22H17N2O3 75-77 60 Off-white 11b 4,5-dihydro-4-(2-chlorophenyl)- 6-(1- benzofuran-2-yl)-2H-indazol-3(H)ones C21H14N2O2 Cl 113-115 50 Gray 96 | Chemistry 2015) عام 1العدد ( 28مجلة إبن الھيثم للعلوم الصرفة و التطبيقية المجلد Ibn Al-Haitham J. for Pure & Appl. Sci. Vol. 28 (1) 2015 Table No.(2):Characteristic FTIR absorption bands of synthesized compounds 2-11(a,b) Comp. No. ν N-H ν C=O ν C=N ν C=C ν C=C aromatic ν C=S Others 2a 3394 - 1653 1610 1558 - C-OCH3: 831 2b 3441 - 1622 1600 1554 - C-Cl:750 3a - - 1620 1595 1554 - C-OCH3: 829 3b - - 1644 1597 1559 - C-Cl:750 4a - 1664 1654 1593 1573 - C-OCH3: 819 4b - 1662 1632 1601 1558 - C-Cl:752 5a - 1680 1654 1592 1573 - C-OCH3: 820 5b - 1666 1612 1591 1551 - C-Cl:750 6a - - 1610 1585 1549 1249 C-OCH3: 829 6b - - 1640 1574 1545 1257 C-Cl:751 7a - - 1653 - 1589 - C-O-N: 1251 7b - - 1647 - 1558 - C-O-N: 1342 8a 3419 - - 1671 1160 C-OCH3: 830 8b 3384 - - 1652 1136 C-Cl:751 9a 3384 1665 - 1620 1559 - C-OCH3: 819 9b 3444 1660 - 1643 1555 - C-Cl:751 10a - 1731 - 1650 1600 - C-OCH3: 836 10b - 1743 - 1645 1592 - C-Cl:750 11a 3363 1709 1602 1535 1519 - C-OCH3: 819 11b 3344 1713 1600 1590 1510 - C-Cl:773 Table No. (3) : antibacterial activity of the synthesized compounds 2-11(a,b) Comp.  No.  E.  Coli  (G‐)  Staphlococcus aurus(G+)    Comp.  No.  E.  Coli  (G‐)  Staphlococcus  aurus(G+)  2a ++ + 7a +++ +++ 2b ++ ++ 7b +++ ++ 3a + ++ 8a ++ +++ 3b + ++ 8b ++ ++ 4a ++ +++ 9a + ++ 4b +++ ++ 9b ++ ++ 5a ++ + 10a ++ + 5b ++ + 10b + + 6a +++ ++ 11a +++ +++ 6b ++ ++ 11b +++ +++ Key to symbols: Highly active = + + +(mor than)15 mm. Moderately active = + +(11-15) mm and slightly active = + (5-10) . 97 | Chemistry 2015) عام 1العدد ( 28مجلة إبن الھيثم للعلوم الصرفة و التطبيقية المجلد Ibn Al-Haitham J. for Pure & Appl. Sci. Vol. 28 (1) 2015 Figure No.(1):1HNMR spectrum of compound (2b)  Figure No.(2):1HNMR spectrum of compound (7a)  98 | Chemistry 2015) عام 1العدد ( 28مجلة إبن الھيثم للعلوم الصرفة و التطبيقية المجلد Ibn Al-Haitham J. for Pure & Appl. Sci. Vol. 28 (1) 2015 Figure No. (3):1HNMR spectrum of compound (8a) Figure No.(4):1HNMR spectrum of compound (9b) 99 | Chemistry 2015) عام 1العدد ( 28مجلة إبن الھيثم للعلوم الصرفة و التطبيقية المجلد Ibn Al-Haitham J. for Pure & Appl. Sci. Vol. 28 (1) 2015 بعض المركبات الحلقية غير المتجانسة الجديدة من مشتقات الجالكون تحضير منى سمير سعيد جامعة بغداد )/ابن الھيثم (كلية التربية للعلوم الصرفة /قسم الكيمياء 2014 كانون االول 7:قبل البحث في ،2014 ايلول 1استلم البحث في: الخالصة استيل بنزوفيوران مع اثنين من االلديھايدات االروماتية في وسط قاعدي . - 2من تفاعل (a,b)1 حضرت الجالكونات استعملت ھذه الجالكونات مادة اولية للحصول على مشتقات حلقية غير متجانسة ھي :البايروزولين , االيزوكزازولين , ثايون , والبريميدينون , والسايكلوھكسانون , واالندازول . وشخص تركيب المركبات الحلقية غير المتجانسة والبريميدين والطرائق الطيفية C.H.N)(للعناصرالجديدة المحضرة عن طريق قياس درجات اانصھارھا وتحليل العناصر الدقيق FTIR وHMNR1 مختلفة(لبعضھا ). كما درست الفعالية البايولوجية للمركبات المحضرة واظھرت فعالية بايولوجية Staphylococcus (G+) . و Echerichia coli (G-) ,ضد البكتريا بنوعيھا اندازول.,زولين,بريميدون,ثايوبريميدين,سايكلوھكسانونوكسيزجالكون,بايرازولين,ا:الكلمات المفتاحية