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International Journal of Pharmaceutical Science Invention
ISSN (Online): 2319 – 6718, ISSN (Print): 2319 – 670X
www.ijpsi.org Volume 5 Issue 3 ‖ June 2016 ‖ PP.47-49
www.ijpsi.org 47 | P a g e
Synthesis and Anti-Inflammatory activity of Sulpha/substituted
1,2-Diazoles
Rigvendersingh Malik
Dept. of chemistry, R.S.M.(P.G.) College, Rampur Ghoghar, Moradabad(U.P.),INDIA.
ABSTRACT
A Novel compound namely N1
(3 Nicotinoyl) 3,5 dimethyl-4-(N-4-sulfamoyl-azo)-1,2-diazoles has been
synthesized by two step processes. Synthesis of N1
-4-sulfamoylphenylhydrazono-3,5-dimethyl propane-1,3-dione
and sulfonamide, which interacting with 3-Nicotinoyl hydrazine to form final compound. The newly synthesized
compound N1
-(3-Nicotinoyl)-3,5-dimethyl 4-(N1
-4-sulfamoyl phenyl azo) 1,2-diazoles was screened for anti-
inflammatory activity.
Keywords: synthesis, anti-inflammatory activity, sulfonamide 1,3-diketone,3-Nicotinoyl hydrazine.
I. INTRODUCTION
The organic chemists employing the art of synthesis have been responsible for the development of vast majority
of drug used in modern system of medicine. Many founding fathers of medicinal chemists were interested not
only in natural products but also on the effect of synthetic compounds in living system.
A heterocyclic compound is one which possess cyclic structures with at least one hetero atom in the ring.
Nitrogen,oxygen and sulfur are the most common hetero atoms. Heterocyclic compounds are very widely
distributed in nature and essential to the life in various ways. Vitamin C exists in the form of five
membered(furan) or six membered(pyron) rings containing one oxygen atom.Most member of Vitamin B group
possess heterocyclic ring containing nitrogen. One example is Vitamin B6 (Pyridoxime),which derivative of
pyridine essential in amino acid metabolism.
1,2-diazole is a heterocyclic compound having varied biological activity and still of great scientific now adays.
They are widely found in bioorganic and medicinal chemistry application in drug discovery. Nitrogen based
heterocyclic compounds are very important in the field of medicinal chemistry. The present diazoles were
prepared because of its good biological activity. Compounds including a 1,2-diazole nucleus and N-substituted
derivatives are known to possess various biological activity1.
Among these types of molecules have been shown to have various important biological activity such as
antibacterial,antifungal,antiviral,diuretic,antitiuberculostatic,antiHIV,antihistaminic,anticancer,anticonvulsant,an
ti-inflammatory and analgesic properties 3-7. Sulfa/substituted 1,2-diazoles may serve as the alternative sources
for the development of new anti-inflammatory agents due to their biological activity. Sulfa/substituted 1,2-
diazoles used for the treatment of anti-inflammatory in different systems of medicine have shown diuretic
activity when tested on animal models. On the basis of the use of diuretics, but no previous pharmacological
study was carried out to test anti-inflammatory the activity of sulfa/substituted 1,2-diazoles. The main aim of the
present investigation was to evaluate the claimed anti-inflammatory activity of sulfa/substituted 1,2-diazoles.
II. MATERIAL AND METHOD
The 1,3-diketones,sulfanilamide,3-Nicotinoyl hydrazine and all reference compound were purchased from
Aldrich Chemicals, Ethanol, sodium acetate, glacial acetic acid and all other reagents were purchased from S.D.
Chem. TLC was performed on pre-coated plastic sheets of silica gel G/UV-254 of 0.2 mm thickness(Macherey-
Nagel,Germany).
Melting points of the N1
-(3Nicotinoyl)3,5-dimethyl-4-(N-4-sulfamoylphenylazo)-1,2-diazole were determined
using an open-ended capillary tube method and are uncorrected. The purity of the synthesized compound was
checked by TLC. A FT-IR spectrum was recorded on a Perkin-Elmer1605 series FT-IR in a KBr disc,1H NMR
spectra was recorded at 300MHz on a Burker FT-NMR spectro-photometer using TMS as internal standard.
Step1; Synthesis of N1
-4-sulfamoylphenyl hydrazono-3,5-dimethyl propane-1,3-dione-
An ice cooled solution of 3,5-dimethyl propane-1,3-dione(0.03 mole) in ethanol containing sodium
acetate(6gms) is a diazotized solution of sulfonamide(0.05 mole) were gradually added with stirring and
cooling. The reaction mixture was further stirring for 20 minutes, the colouredhydrazono compounds
precipitated by addition of ice cold water. It was filtered off, washed with water, dried and recrystallized from
ethanol/acetic acid[Fig.1]. On analysis, it was found to be N1-4-sulfamoylphenyl hydrazono-3,5-dimethyl
propane-1,3-dione.
Synthesis and Anti-Inflammatory activity of Sulpha/substituted 1,2-Diazoles
www.ijpsi.org 48 | P a g e
Synthesis of novel N1
-(3-Nicotinoyl),5-dimethyl-4(N-4-sulfamoylphenylazo)-1,2-diazole.
Fig.1- Synthesis of N1
-4-sulfamoylphenyl hydrazono-3,5-dimethyl propane-1,3-dione.
N1
-4-sulfamoylphenyl hydrazono 3,5-dimethyl propane-1,3-dione:A yellow crystalline powder,Mp 198-200o
C,
Yield 82.34%, molecular formula C16H15O4N3S(348.76);C,55.10;H,4.34;0,18.35;N, 12.04;S,10.17.
Found:54.92;4.56;O,18.17;N,12.48; S,9.87,IR(KBr) in cm-1 1440(C-C),1560(C=C of aromatic ring), 1260(C-
N), 1680(C=O), 3087(NH), 3275(SO2NH2). 1HNMR (CdCl3) in ppm, 2.81(s, 3H CH3), 6.75-7.68(m, 9H, Ar-H),
6.929(s,2H NH2),10.43(s, 1H NH).
Step-II; Synthesis of N1
-(3-Nicotinoyl, 3,5-dimethyl-4(N-4-sulfamoyl phenylazo)-1,2-diazole:
A solution of N1
-4-sulfamoylphenyl-hydrazono 3,5-dimethyl propane-1,3-dione (0.02 mole) in glacial acetic
acid was added to 3-Nicotinoyl hydrazine (0.05 mole) refluxed on water bath for 4 hours and left overnight. On
cooling, shining recrystallized crystals, separated out which was collected by filtration, washed well with water,
dried and recrystallized from glacial acetic acid to give N1
-(3-Nicotinoyl)3,5 dimethyl-4(N-4-
sulfamoylphenylazo)-1,2-diazole.
[Fig. 2]
Fig.2: Synthesis of N1
-(3-Nicotinoyl) N1
-3,5-dimethyl-4(N-4-sulfamoylphenylazo)-1,2-diazole
N1
(3-Nicotinoyl)-3,5-dimethyl-4-(N-sulfamoylphenylazo)-1,2-diazole: A yellow crystalline powder, mp 226-
228o
C, Yield 72.13%. Molecular formula C23H20O3N5anal.Calcd for C23H20O3N6S (463.90); C,59.55;
H,4.34; O,10.35; N,18.12; S,7.64. Found: C,58.97; H,4.64; O,10.29; N,18.37; S,7.73. IR(KBr) in cm-1 740(C-
C), 1240(C-N), 1535(C=C of aromatic ring), 1585(C=N), 1460(N=N), 3055(aromatic C-H), 3135(NH),
1707(C=O), 3082(NH2). 1
HNMR(CdCl3) in ppm, 2.79(s, 3H CH3), 6.65-7.58(m, 13, Ar-H), 7.10(m, 4H NH2).
Animals: Adult’s male Wistaralbino rats, each in the weight range of 180-200 gm were used for this experiment.
They were procured from National Vertinary Research centre, Bareilly, India. The animals were randomly
allocated to six treatment groups of six animals each and kept in polypropylene cages and housed under standard
conditions of temperature, humidity, dark light cycle (12h-12h) and diet.
Anti-inflammatory activity8
:
Synthesis and Anti-Inflammatory activity of Sulpha/substituted 1,2-Diazoles
www.ijpsi.org 49 | P a g e
The activity of the newly synthesized compounds compared to indomethacin as a reference compound was
measured before and 4h after carrageenan injection. Percent of the oedema inhibition was calculated as regards
saline control group and potency was calculated as regards percentage of the change of indomethacin and tested
compounds, as depicted in Table1. All the tested compounds showed a reasonable inhibition of oedema size
ranging between a 12.5% for compound 25.4% for compound (b) 28% for compound, 32.7% for compound
sulfanomide 1,2-diazole (c), 44.4% for compound sulfapyrimidine 1,2-diazole (d) and 29.9% for indomethacin.
In activity relationship point of view, the anti-inflammatory activity of the pyrimidine was found to be the
promising one. But sulfonamide also showed good anti-inflammatory activity(32.7%)
III. CONCLUSION
The present study reveals that synthesized compound N1
(3-Nicotinoyl)-3,5-dimethyl4(N-4-
sulfamoylphenylazo)-1,2-diazole possess significant at 100 and 200 mg/kgbut the effect declined at higher dose.
ACKNOWLEDGEMENT
The author expresses their sincere thanks to Dr. C. P. Singh, Head, Department of Chemistry, Sahu Jain
College,Najibabad for providing lab facilities and also thanks to CDRI Lucknow, IIT Roorkee for providing IR,
NMR spectral data and pharmacological data.
REFERENCES
[1]. Achson a, an introduction to the chemistry of heterocyclic compounds 3rd edition, Wiley interscience, India 2000.
[2]. G. capan, N. Ulusoy, N.Egenc, New 6-phenylimidazo [2,1-b]thiazolederivatives:Synthesis and antifungal activity. Montash,
Chem. (1999),130,1399.
[3]. R. U. Roy, R. Desai, K.R. Desai,”synthesis and Antimicrobial Activity of 1,2,4-Thiazoles,|E-Journal of Chemistry,(2005),2(6),1.
[4]. M.G. Vigorita, R.Ottana, F.Monforte, R. maccan,A. Trovato, M.T. Monforte, M.F.| Taviano, Synthesis and anti-inflammatory,
analgesic activity of 3,3-(1,2-ethandiyl)-bis[2-aryl-4-thiazolidione] chiral compounds Part 10
[5]. C. V. kavitha, S. basappa, S. Nanjunda, K. Mantelingu, S. Doreswamy, M.A. Sridhar, J.S. Prasad, K.S. Rangappa, Synthesis of
new bioactive venlafaxine analogs:Novelthiazolidin-|4-ones as antimicrobilasbioorg. Med. Chem. (2006), 14, 2290.
[6]. R. Ottana, R. Maccari, M. L. Bareca, G. Bruno, A. Rotondo, A. Rossi, G. Chricosta, R. Di Paola, L. Sautebin, S. Cuzzocrea,
M.G. Vigorita, 5-Aryldiene-2-imino-4-thiazolidinones: Design and synthesis of novel anti-inflammatory agents, Bioorg. Chem.
(2005),13,|4243|
[7]. G. kucukguzel, A. Kocatepe, E. De Clercq, F. Sahin, M. Gulluce, Synthesis and biological activity of 4-thiazolidinones,
thiosemicarbazides derived from diflusinalhydrazide. Eur. J. med. Chem. (2006),41,353.
[8]. Radwan, M.A.A., Rageb E.A. Saby, N.M. El-Shenaway,S.M., Potential anti-inflammatory and analgesic agents, Bioorganic and
medicinal chemistry (2007),15,3832-|3841|
[9]. Singh N, Bhatia, S.K. Kumar A, Thiazolyl/formazanyl-1,2-diazoles as potent anti-inflammatory agent, European Jour. Of
medicinal Chem., (2008), 43,2597-2609
[10]. S.Jain, R. nagwanshi, M.Bakhru and S. Bageria, Antimicrobial Activity of Heteroarylchalcones and their products, Journal of
Indian Chemical Society,(2011),88,1571-1570
[11]. T. Giresh, G. Mohiddin, Z. Khan and R.R. Kumble, Synthesis of 1,3,4-Thiazole appended to Coumarins as antimicrobial agent,
Journal of Indian Chemical Society,(2011),88,1459-1463
[12]. P. Samadhiya, Ritu Sharma, S.K. Srivastava and S. D. Sharma, Synthesis and biological evaluation of Some 2-amino-5-
Nitrothiazole derivative, Journal of Indian Chemical Society, (2013),90,231-238
[13]. R.J. Deshmukh and S.P. Deshmukh, Synthesis and antimicrobial activity of 3-aryl-thiadiazole derivative, Journal of Indian
Chemical Society,(2013),90,1027-1031
[14]. Anil kumar and C. P. Singh, Synthesis ,Characterisation and biological activity of some New Sulfa/substituted phenyl azoIndoles
IJSR,4(10),934-938(2015)

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Synthesis and Anti-Inflammatory activity of Sulpha/substituted 1,2-Diazoles

  • 1. International Journal of Pharmaceutical Science Invention ISSN (Online): 2319 – 6718, ISSN (Print): 2319 – 670X www.ijpsi.org Volume 5 Issue 3 ‖ June 2016 ‖ PP.47-49 www.ijpsi.org 47 | P a g e Synthesis and Anti-Inflammatory activity of Sulpha/substituted 1,2-Diazoles Rigvendersingh Malik Dept. of chemistry, R.S.M.(P.G.) College, Rampur Ghoghar, Moradabad(U.P.),INDIA. ABSTRACT A Novel compound namely N1 (3 Nicotinoyl) 3,5 dimethyl-4-(N-4-sulfamoyl-azo)-1,2-diazoles has been synthesized by two step processes. Synthesis of N1 -4-sulfamoylphenylhydrazono-3,5-dimethyl propane-1,3-dione and sulfonamide, which interacting with 3-Nicotinoyl hydrazine to form final compound. The newly synthesized compound N1 -(3-Nicotinoyl)-3,5-dimethyl 4-(N1 -4-sulfamoyl phenyl azo) 1,2-diazoles was screened for anti- inflammatory activity. Keywords: synthesis, anti-inflammatory activity, sulfonamide 1,3-diketone,3-Nicotinoyl hydrazine. I. INTRODUCTION The organic chemists employing the art of synthesis have been responsible for the development of vast majority of drug used in modern system of medicine. Many founding fathers of medicinal chemists were interested not only in natural products but also on the effect of synthetic compounds in living system. A heterocyclic compound is one which possess cyclic structures with at least one hetero atom in the ring. Nitrogen,oxygen and sulfur are the most common hetero atoms. Heterocyclic compounds are very widely distributed in nature and essential to the life in various ways. Vitamin C exists in the form of five membered(furan) or six membered(pyron) rings containing one oxygen atom.Most member of Vitamin B group possess heterocyclic ring containing nitrogen. One example is Vitamin B6 (Pyridoxime),which derivative of pyridine essential in amino acid metabolism. 1,2-diazole is a heterocyclic compound having varied biological activity and still of great scientific now adays. They are widely found in bioorganic and medicinal chemistry application in drug discovery. Nitrogen based heterocyclic compounds are very important in the field of medicinal chemistry. The present diazoles were prepared because of its good biological activity. Compounds including a 1,2-diazole nucleus and N-substituted derivatives are known to possess various biological activity1. Among these types of molecules have been shown to have various important biological activity such as antibacterial,antifungal,antiviral,diuretic,antitiuberculostatic,antiHIV,antihistaminic,anticancer,anticonvulsant,an ti-inflammatory and analgesic properties 3-7. Sulfa/substituted 1,2-diazoles may serve as the alternative sources for the development of new anti-inflammatory agents due to their biological activity. Sulfa/substituted 1,2- diazoles used for the treatment of anti-inflammatory in different systems of medicine have shown diuretic activity when tested on animal models. On the basis of the use of diuretics, but no previous pharmacological study was carried out to test anti-inflammatory the activity of sulfa/substituted 1,2-diazoles. The main aim of the present investigation was to evaluate the claimed anti-inflammatory activity of sulfa/substituted 1,2-diazoles. II. MATERIAL AND METHOD The 1,3-diketones,sulfanilamide,3-Nicotinoyl hydrazine and all reference compound were purchased from Aldrich Chemicals, Ethanol, sodium acetate, glacial acetic acid and all other reagents were purchased from S.D. Chem. TLC was performed on pre-coated plastic sheets of silica gel G/UV-254 of 0.2 mm thickness(Macherey- Nagel,Germany). Melting points of the N1 -(3Nicotinoyl)3,5-dimethyl-4-(N-4-sulfamoylphenylazo)-1,2-diazole were determined using an open-ended capillary tube method and are uncorrected. The purity of the synthesized compound was checked by TLC. A FT-IR spectrum was recorded on a Perkin-Elmer1605 series FT-IR in a KBr disc,1H NMR spectra was recorded at 300MHz on a Burker FT-NMR spectro-photometer using TMS as internal standard. Step1; Synthesis of N1 -4-sulfamoylphenyl hydrazono-3,5-dimethyl propane-1,3-dione- An ice cooled solution of 3,5-dimethyl propane-1,3-dione(0.03 mole) in ethanol containing sodium acetate(6gms) is a diazotized solution of sulfonamide(0.05 mole) were gradually added with stirring and cooling. The reaction mixture was further stirring for 20 minutes, the colouredhydrazono compounds precipitated by addition of ice cold water. It was filtered off, washed with water, dried and recrystallized from ethanol/acetic acid[Fig.1]. On analysis, it was found to be N1-4-sulfamoylphenyl hydrazono-3,5-dimethyl propane-1,3-dione.
  • 2. Synthesis and Anti-Inflammatory activity of Sulpha/substituted 1,2-Diazoles www.ijpsi.org 48 | P a g e Synthesis of novel N1 -(3-Nicotinoyl),5-dimethyl-4(N-4-sulfamoylphenylazo)-1,2-diazole. Fig.1- Synthesis of N1 -4-sulfamoylphenyl hydrazono-3,5-dimethyl propane-1,3-dione. N1 -4-sulfamoylphenyl hydrazono 3,5-dimethyl propane-1,3-dione:A yellow crystalline powder,Mp 198-200o C, Yield 82.34%, molecular formula C16H15O4N3S(348.76);C,55.10;H,4.34;0,18.35;N, 12.04;S,10.17. Found:54.92;4.56;O,18.17;N,12.48; S,9.87,IR(KBr) in cm-1 1440(C-C),1560(C=C of aromatic ring), 1260(C- N), 1680(C=O), 3087(NH), 3275(SO2NH2). 1HNMR (CdCl3) in ppm, 2.81(s, 3H CH3), 6.75-7.68(m, 9H, Ar-H), 6.929(s,2H NH2),10.43(s, 1H NH). Step-II; Synthesis of N1 -(3-Nicotinoyl, 3,5-dimethyl-4(N-4-sulfamoyl phenylazo)-1,2-diazole: A solution of N1 -4-sulfamoylphenyl-hydrazono 3,5-dimethyl propane-1,3-dione (0.02 mole) in glacial acetic acid was added to 3-Nicotinoyl hydrazine (0.05 mole) refluxed on water bath for 4 hours and left overnight. On cooling, shining recrystallized crystals, separated out which was collected by filtration, washed well with water, dried and recrystallized from glacial acetic acid to give N1 -(3-Nicotinoyl)3,5 dimethyl-4(N-4- sulfamoylphenylazo)-1,2-diazole. [Fig. 2] Fig.2: Synthesis of N1 -(3-Nicotinoyl) N1 -3,5-dimethyl-4(N-4-sulfamoylphenylazo)-1,2-diazole N1 (3-Nicotinoyl)-3,5-dimethyl-4-(N-sulfamoylphenylazo)-1,2-diazole: A yellow crystalline powder, mp 226- 228o C, Yield 72.13%. Molecular formula C23H20O3N5anal.Calcd for C23H20O3N6S (463.90); C,59.55; H,4.34; O,10.35; N,18.12; S,7.64. Found: C,58.97; H,4.64; O,10.29; N,18.37; S,7.73. IR(KBr) in cm-1 740(C- C), 1240(C-N), 1535(C=C of aromatic ring), 1585(C=N), 1460(N=N), 3055(aromatic C-H), 3135(NH), 1707(C=O), 3082(NH2). 1 HNMR(CdCl3) in ppm, 2.79(s, 3H CH3), 6.65-7.58(m, 13, Ar-H), 7.10(m, 4H NH2). Animals: Adult’s male Wistaralbino rats, each in the weight range of 180-200 gm were used for this experiment. They were procured from National Vertinary Research centre, Bareilly, India. The animals were randomly allocated to six treatment groups of six animals each and kept in polypropylene cages and housed under standard conditions of temperature, humidity, dark light cycle (12h-12h) and diet. Anti-inflammatory activity8 :
  • 3. Synthesis and Anti-Inflammatory activity of Sulpha/substituted 1,2-Diazoles www.ijpsi.org 49 | P a g e The activity of the newly synthesized compounds compared to indomethacin as a reference compound was measured before and 4h after carrageenan injection. Percent of the oedema inhibition was calculated as regards saline control group and potency was calculated as regards percentage of the change of indomethacin and tested compounds, as depicted in Table1. All the tested compounds showed a reasonable inhibition of oedema size ranging between a 12.5% for compound 25.4% for compound (b) 28% for compound, 32.7% for compound sulfanomide 1,2-diazole (c), 44.4% for compound sulfapyrimidine 1,2-diazole (d) and 29.9% for indomethacin. In activity relationship point of view, the anti-inflammatory activity of the pyrimidine was found to be the promising one. But sulfonamide also showed good anti-inflammatory activity(32.7%) III. CONCLUSION The present study reveals that synthesized compound N1 (3-Nicotinoyl)-3,5-dimethyl4(N-4- sulfamoylphenylazo)-1,2-diazole possess significant at 100 and 200 mg/kgbut the effect declined at higher dose. ACKNOWLEDGEMENT The author expresses their sincere thanks to Dr. C. P. Singh, Head, Department of Chemistry, Sahu Jain College,Najibabad for providing lab facilities and also thanks to CDRI Lucknow, IIT Roorkee for providing IR, NMR spectral data and pharmacological data. REFERENCES [1]. Achson a, an introduction to the chemistry of heterocyclic compounds 3rd edition, Wiley interscience, India 2000. [2]. G. capan, N. Ulusoy, N.Egenc, New 6-phenylimidazo [2,1-b]thiazolederivatives:Synthesis and antifungal activity. Montash, Chem. (1999),130,1399. [3]. R. U. Roy, R. Desai, K.R. Desai,”synthesis and Antimicrobial Activity of 1,2,4-Thiazoles,|E-Journal of Chemistry,(2005),2(6),1. [4]. M.G. Vigorita, R.Ottana, F.Monforte, R. maccan,A. Trovato, M.T. Monforte, M.F.| Taviano, Synthesis and anti-inflammatory, analgesic activity of 3,3-(1,2-ethandiyl)-bis[2-aryl-4-thiazolidione] chiral compounds Part 10 [5]. C. V. kavitha, S. basappa, S. Nanjunda, K. Mantelingu, S. Doreswamy, M.A. Sridhar, J.S. Prasad, K.S. Rangappa, Synthesis of new bioactive venlafaxine analogs:Novelthiazolidin-|4-ones as antimicrobilasbioorg. Med. Chem. (2006), 14, 2290. [6]. R. Ottana, R. Maccari, M. L. Bareca, G. Bruno, A. Rotondo, A. Rossi, G. Chricosta, R. Di Paola, L. Sautebin, S. Cuzzocrea, M.G. Vigorita, 5-Aryldiene-2-imino-4-thiazolidinones: Design and synthesis of novel anti-inflammatory agents, Bioorg. Chem. (2005),13,|4243| [7]. G. kucukguzel, A. Kocatepe, E. De Clercq, F. Sahin, M. Gulluce, Synthesis and biological activity of 4-thiazolidinones, thiosemicarbazides derived from diflusinalhydrazide. Eur. J. med. Chem. (2006),41,353. [8]. Radwan, M.A.A., Rageb E.A. Saby, N.M. El-Shenaway,S.M., Potential anti-inflammatory and analgesic agents, Bioorganic and medicinal chemistry (2007),15,3832-|3841| [9]. Singh N, Bhatia, S.K. Kumar A, Thiazolyl/formazanyl-1,2-diazoles as potent anti-inflammatory agent, European Jour. Of medicinal Chem., (2008), 43,2597-2609 [10]. S.Jain, R. nagwanshi, M.Bakhru and S. Bageria, Antimicrobial Activity of Heteroarylchalcones and their products, Journal of Indian Chemical Society,(2011),88,1571-1570 [11]. T. Giresh, G. Mohiddin, Z. Khan and R.R. Kumble, Synthesis of 1,3,4-Thiazole appended to Coumarins as antimicrobial agent, Journal of Indian Chemical Society,(2011),88,1459-1463 [12]. P. Samadhiya, Ritu Sharma, S.K. Srivastava and S. D. Sharma, Synthesis and biological evaluation of Some 2-amino-5- Nitrothiazole derivative, Journal of Indian Chemical Society, (2013),90,231-238 [13]. R.J. Deshmukh and S.P. Deshmukh, Synthesis and antimicrobial activity of 3-aryl-thiadiazole derivative, Journal of Indian Chemical Society,(2013),90,1027-1031 [14]. Anil kumar and C. P. Singh, Synthesis ,Characterisation and biological activity of some New Sulfa/substituted phenyl azoIndoles IJSR,4(10),934-938(2015)