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마이크로파를 이용한 강한 항균제인 새로운 N1-치환된 5-Cyano-pyrimidine 유도체의 합성

Microwave Assisted Synthesis of New N1-Substituted 5-Cyano-pyrimidine Derivatives as Potent Antimicrobial Agents

  • Pore, Yogesh (Department of Pharmaceutical Chemistry, Government College of Pharmacy) ;
  • Patil, Gaurav (Department of Pharmaceutical Chemistry, Government College of Pharmacy) ;
  • Tamboli, Ijaj (Department of Pharmaceutical Chemistry, Government College of Pharmacy) ;
  • Chavan, Vaibhav (Department of Pharmaceutical Chemistry, Government College of Pharmacy) ;
  • Kamble, Kirti (Department of Pharmaceutical Chemistry, Government College of Pharmacy) ;
  • Nikam, Shital (Department of Pharmaceutical Chemistry, Government College of Pharmacy) ;
  • Kuchekar, Bhanudas (Department of Pharmaceutical Chemistry, Government College of Pharmacy)
  • 발행 : 2008.02.20

초록

연구의 목적은 N1과 6번 자리에 다른 치환기를 가진 5-cyano가 치환된 pyrimidine 아날로그의 새로운 시리즈의 합성과 그것들의 항균성과 항진균성의 활성도에 대해 평가하기 위해서이다. 이 화합물은 MORE technique 를 이용한 potassium carbonate 의 존재하에서 ethylcyanoacetate, 치환된 thioureas, 적당한 알데히드의 제 3차 축합으로 합성 되어졌다. 항균성과 항진균성의 활성도는 25 mg의 농도에서 cup-plate 방법으로 측정되었다. 억제구역은 mm로 측정 되어졌다. 모든 화합물은 좋은 항균성과 항진균성을 보여주었다. P1과 P5는 S.aureus과 E.coli에 대해 최대 활성도를 보여주었고, P6은 모든 종류의 미생물에 대해 좋은 활성도를 보여주었다. P8 화합물은 C. albicans 에 대해 좋은 효과가 있음을 알아냈다. Norfloxacin와 griseofulvin는 합성된 화합물의 활성도와 비교되는 기준물질로 사용되었다. 6번 자리에 p-hydroxy와 p-methoxy로 치환된 phenyl moiety를 가진 gram-양성 미생물에 대해 강력했고, 6번 자리에 이것들이 없는 phenyl moiety 를 가진 아날로그는 gram-음성 활성도를 가졌다,6번 자리에 p-dimethylamino로 치환된 phenyl moiety를 가진 화합물은 적당한 활성을 보여준다.. 게다가 N1자리에서 단지 fluorine을 포함한 아날로그는 상당한 항진균성을 가졌음을 밝혀냈다. N1자리에서 aryl moiety 의 전자 끌게 치환과 마찬가지로 전자 주게 치환은 화합물의 결정된 능력에 중요한 역할을 함을 제시한다.

purpose of the study was to synthesize new series of 5-cyano substituted pyrimidine analogues with different substitutions at N1 and 6 positions and to evaluate them for antibacterial and antifungal activities. The desired compounds were synthesized by tertiary condensation of ethylcyanoacetate, substituted thioureas and suitable aldehyde in presence of potassium carbonate using MORE technique. The antibacterial and antifungal activities were evaluated by cup plate method in the concentration of 25 mg. The zone of inhibition was measured in mm. All the compounds have shown significant antibacterial and antifungal activities. The maximum activity was shown by P1 and P5 against S.aureus and E.coli respectively, while P6 has shown significant activity against all types of microorganisms. The compound P8 has been found to be significantly effective against C. albicans. Norfloxacin and griseofulvin were used as standards to compare the activites of synthesized compounds. It is concluded that analogues containing p-hydroxy, p-methoxy substituted phenyl moiety at 6 position have been found to be more potent against gram-positive microorganisms, while analogues lacking these substituents on phenyl moiety possessed gram-negative activity. The compounds having p-dimethylamino substituent on phenyl moiety at 6 positions have shown moderate activity. Further, only fluorine containing analogue at N1 position was found to possess appreciable antifungal activity. This suggests that electron donating substituent on aryl moiety as well as electron withdrawing substituent at N1 plays important role in determining potency of the compounds.

키워드

INTRODUCTION

Uracil derivatives play an important role in the field of medicine, as antiretroviral, agents 1,2,3. They have also been reported as potent enzyme inhibitors 4,5,6. In last few years uracil derivatives substituted either at the C-5 or C-6 position have emerged in chemotherapy as several pyrimidine derivatives have been found to possess antileishmanial and antimicrobial activity.7,8 In case of pyrimidine nucleus structure activity relationship studies have shown that C-6 position is important determinant for the activity. The most general route for the synthesis of pyrimidines is a reagent containing N-C-N and C-C-C skeleton. The N-C-N skeleton containing reagents are urea, thiourea or guanidine whereas C-C-C skeleton can be obtained from 1,3-diketones, diesters and dinitriles.8 A facile synthesis of 2-thiocytosines has been reported using piperidine in place of potassium carbonate.9 Pyrimidines have been also synthesized by regiospecific cyclization of 1,3-dicarbonitriles,10 from ketene dithioacetals11 and from alkyl N-cyanoimidates or cyanoacetamides. 12 However these classical methods resulted in poor yield of pyrimidine compounds. Therefore, in order to obtain new potent therapeutic agents, various 5-cyano, 6-substituted (alkyl/aryl) pyrimidine derivatives were synthesized using one- pot reaction of aryl substituted thiourea, aldehyde and ethylcyanoacetate utilizing microwave irradiation to get various N1-substituted and 6-aryl/substituted aryl pyrimidines in better yield. These compounds were evaluated for their antibacterial and antifungal activities.

 

RESULTS

Chemistry

Pyrimidines have been synthesized by microwave irradiation and found to give higher yields of compounds13. The synthesis of substituted 5-cyano, 2-thiouracil derivatives (P1-P10) was accomplished by reacting various aldehydes with equimolar amount of appropriate substituted thioureas, ethylcyanoacetate and potassium carbonate in small amount of ethanol utilizing microwave irradiation (Scheme 1). Unlike the conventional methods9-12 where the reaction time required was 5-7 hrs and with yields of 26-75%, microwave-assisted reactions were very facile (4-8 min. with few minutes of interval) and provided very good yields (65-83%). The purity of the compounds was checked by TLC and elemental analysis. Melting points and % yields of synthesized compounds are reported in Table 1. Both analytical and spectral data of all the synthesized compounds were in full agreement with the proposed structures.

Scheme 1.

Table 1.Physical data of synthesized compounds

Antibacterial and antifungal activities

The synthesized compounds were evaluated for their antibacterial and antifungal activities by cupplate method against S. aureus, B. subtilis, E. coli, P. aeruginosa, and C. albicans in the concentration of 25 μg. The activites were compared with standard antibiotics; norfloxacin and griseofulvin. The synthesized compounds exhibited zone of inhibition of 09-22 mm in diameter whereas standard norfloxacin and griseofulvin exhibited zone of 25-28 mm in diameter. All the compounds have shown significant antibacterial and antifungal activities. The maximum activity was shown by P1 and P5 against S.aureus and E. coli respectively, while P6 has shown significant activity against all types of microorganisms. The compound P8 has been found to be significantly effective against C. albicans. All other compounds have shown moderate antimicrobial activities. The results of antimicrobial activities are expressed in Table 2.

Table 2.Zone of inhibition: + = 5-10 mm, ++ = 11-15 mm, +++ = 16-20 mm, ++++ = More than 20 mm.

 

DISCUSSION

In the present investigation new series of 5-cyano, N1 substituted pyrimidine analogues were synthesized by microwave irradiation technique. Unlike the conventional methods where more reaction time is required, with yields of 26-75%, microwave- assisted reactions resulted in higher yields (65-83%) of products. These synthesized compounds were also screened for antibacterial and antifungal activities. Present findings revealed that analogues containing p-hydroxy, p-methoxy substituted phenyl moiety at 6 position have been found to be more potent against gram-positive microorganisms, while analogues lacking these substituents on phenyl moiety possessed gram-negative activity. The compounds having p-dimethylamino substituent on phenyl moiety at 6 positions have shown moderate activity. Further, only fluorine containing analogue at N1 position was found to possess appreciable antifungal activity. The compound P7 has shown least activity among all the synthesized compounds indicating that meta methyl group in phenyl moiety at N1 position is not well tolerated. Further, as the bulkiness on phenyl moiety at N1 increases, antimicrobial activity decreases. This suggests that electron donating substituent on aryl moiety as well as electron withdrawing substituent at N1 plays important role in determining potency of the compounds. The compounds P1, P5 and P6 have shown good antibacterial activities against S.aureus and E.coli whereas compound P8 has shown excellent antifungal activity against C.albicans. It is concluded that N1 and C-6 position are important determinants for the activity. Also electron-withdrawing substituent at C-5 position in pyrimidine increases the acidic dissociation constant of nucleus and enhances the receptor binding. Further studies are needed to explore the differences in the efficacy and safety of synthesized compounds.

 

EXPERIMENTAL

Materials

The melting points were determined in open capillary tubes and are uncorrected. The purity of compounds was checked by TLC on silica gel G plates using acetonitrile: chloroform (60:40) as mobile phase. IR spectra were recorded on Digilab FT-IR spectrophotometer. 1HNMR and 13CNMR spectra were recorded in DMSO (d6) and CDCI3 on Varian Mercury YH-300 NMR spectrophotometer. Microwave assisted reactions were carried out in a Catalysts Microwave synthesizer.

Methods

Synthesis of aryl-substituted thioureas

These were obtained by reacting the various substituted aromatic amines with ammonium thiocyanate in presence of conc. HCL. The compounds were recrystallized from hot water or ethanol and used for synthesis of pyrimidine derivatives. 14

Synthesis of N1- substituted, 5-cyano, 6-arylsubstituted thiouracil derivatives (P1-P10)

The titled compounds were synthesized using onepot reaction of aryl-substituted thiourea (0.01 mol), aldehyde (0.01 mol), ethylcyanoacetate (0.01 mol) and potassium carbonate in small amount of ethanol to obtain various N1 substituted pyrimidines. Six different aryl substituted thioureas like phenyl thiourea, p-tolyl thiourea, m-tolyl thiourea, p-anisidine thiourea, 2,4-xylidyl thiourea, p-fluoro phenyl thiourea and four aldehydes like benzaldehyde, 4-hydroxy benzaldehyde, p-methoxybenzaldehyde and p-dimethylaminobenzaldehyde were used to obtain ten different 2-thio, 4-one derivatives. The desired compounds were synthesized by the tertiary condensation of ethylcyanoacetate, aryl substituted thiourea and suitable aldehyde in presence of potassium carbonate and ethanol using MORE (Microwave organic reaction enhancement) technique. The reaction mixture was subjected to microwave pulse for 120 s (240 w), 60 s (350 w) and 60 s (450 w). Between each irradiation an interval of 3-10 minutes was kept. After the completion of reaction, the precipitate obtained was dried, which was potassium salt of nucleobase. The salt was dissolved in warm water and the solution was acidified by acetic acid to precipitate pure nucleobase. The crude product was recrystallised from acetic acid. All the compounds were obtained in good yield.

P1: 5-Cyano-1-phenyl-6-(4-hydroxyphenyl)-2-thiouracil

I.R.: ν cm-1 3363 (N-H), 2210 (C≡N), 1622 (C=O), 1305 (C=S), 3150 (O-H), 1HNMR: δ (ppm): 8.17 (s, 1H, NH), 7.24-7.95 (m, 9H, ArH), 4.33-4.40 (s, 1H, OH), 13CNMR: 72.67 (C=C), 115.81-134.02 (11C), 158.10 (phenyl C5), 115.85 (C≡N), 167.09 (-CONH-), 171.79 (C=C), 174.03 (-CSNH-), Anal: Found: C, 63.52; H, 3.39; N, 13.05; S, 9.93. Calcd for C17H11N3SO2: C, 63.54; H, 3.45; N, 13.08; O, 9.96; S, 9.98%.

P2: 5-Cyano-1-(4-methyl-phenyl)-6-(4-hydroxyphenyl)-2-thiouracil

I.R.: ν cm-1 3010 (C-H), 3288(N-H), 2260 (C≡N), 1610 (C=O), 1320 (C=S), 1HNMR: δ (ppm): 8.19 (s, 1H, NH), 7.38-7.90 (m, 8H, ArH), 4.31-4.37 (s, 1H, OH), 2.354 (s, 3H, CH3), 13CNMR: 24.35 (CH3), 72.67 (C=C), 115.82-128.31 (10C), 133.81 (N-phenyl C4), 157.55 (phenyl C4), 115.75 (C≡N), 167.21 (-CONH-), 172.10 (C=C), 174.12 (-CSNH-), Anal: Found: C, 64.41; H, 3.84; N, 12.51; S, 9.52. Calcd for C18H13N3SO2: C, 64.46; H, 3.91; N, 12.53; O, 9.54; S, 9.56%.

P3: 5-Cyano-1,6 bis-(4-methoxy-phenyl)-2-thiouracil

I.R.: ν cm-1 3005 (C-H), 3102 (N-H), 2250 (C≡N), 1590 (C=O), 1280 (C=S), 3175 (O-H), 1275 (O-CH3), 1HNMR: δ (ppm): 8.12 (s, 1H, NH), 7.31-7.97 (m, 8H, ArH), 3.78-3.91 (s, 6H, OCH3), 13CNMR: 55.85 (OCH3), 72.61 (C=C), 114.11-127.41 (10C), 159.80 (phenyl C4), 156.64 (N-phenyl C4), 115.75 (C≡N), 167.21 (-CONH-), 171.68 (C=C), 173.93 (-CSNH-), Anal: Found: C, 62.43; H, 4.08; N, 11.46; S, 8.73. Calcd for C19H15N3SO3: C, 62.45; H, 4.14; N, 11.50; O, 13.14; S, 8.78%.

P4: 5-Cyano-1-(4-methyl-phenyl)-6-phenyl-2-thiouracil

I.R.: ν cm-1 2995 (C-H), 3270 (N-H), 2240 (C≡N), 1620 (C=O), 1200 (C=S), 1HNMR: δ (ppm): 8.00-8.84 (s, 1H, NH), 7.18-7.98 (m, 9H, ArH), 2.35-2.60 (d, 3H, CH3), 13CNMR: 24.25 (CH3), 72.81 (C=C), 126.51-134.35 (11C), 134.42 (N-phenyl C4), 115.72 (C≡N), 167.15 (-CONH-), 171.95 (C=C), 173.98 (-CSNH-), Anal: Found: C, 67.69; H, 4.05; N, 13.13; S, 10.01. Calcd for C18H13N3SO: C, 67.69; H, 4.10; N, 13.16; O, 5.01; S, 10.04%.

P5: 5-Cyano-1,6-diphenyl-2-thiouracil

I.R.: ν cm-1 3005 (C-H), 3280 (N-H), 2270 (C≡N), 1610 (C=O), 1265 (C=S), 1HNMR: d (ppm): δ 9.28(s, 1H, NH), δ 7.17-7.40 (m, 10H, ArH), 13CNMR: 72.68 (C=C), 126.33-133.90 (12C), 115.95 (C≡N), 167.12 (-CONH-), 171.67 (C=C), 174.23 (-CSNH-), Anal: Found: C, 66.85; H, 3.55; N, 13.75; S, 10.47. Calcd for C17H11N3SO: C, 66.87; H, 3.63; N, 13.76; O, 5.24; S, 10.50%.

P6: 5-Cyano-1-(2,4-dimethyl-phenyl)-6-(4-methoxyphenyl)-2-thiouracil

I.R.: ν cm-1 3010 (C-H), 3261 (N-H), 2245 (C≡N), 1605 (C=O), 1275 (C=S), 1175 (O-CH3), 1HNMR: δ (ppm): 8.13-8.15 (d, 1H, NH), 7.32-7.98 (m, 7H, ArH), 2.16-2.17 (s, 6H, CH3), 3.88 (s, 3H, OCH3), 13CNMR: 16.45 (CH3), 24.55 (CH3), 55.81 (OCH3), 72.69 (C=C), 114.29-133.68 (9C), 134.23 (N-phenyl C4), 139.21 (N-phenyl C2), 160.10 (phenyl C4), 115.78 (C≡N), 167.59 (-CONH-), 171.99 (C=C), 174.33 (-CSNH-), Anal: Found: C, 66.09; H, 4.65; N, 11.53; S, 8.79. Calcd for C20H17N3SO2: C, 66.10; H, 4.71; N, 11.56; O, 8.80; S, 8.82 %.

P7: 5-Cyano-1-(3-methyl-phenyl)-6-(4-methoxyphenyl)-2-thiouracil

I.R.: ν cm-1 3000 (C-H), 3280 (N-H), 2205 (C≡N), 1605 (C=O), 1250 (C=S), 1170 (O-CH3), 1HNMR: δ (ppm): 8.13 (s, 1H, NH), 7.30-7.98 (m, 8H, ArH), 3.88 (s, 3H, OCH3), 2.17 (s, 3H, CH3), 13CNMR: 24.13 (CH3), 55.95 (OCH3), 72.67 (C=C), 114.29-134.08 (10C), 138.66 (N-phenyl C3), 159.79 (phenyl C4), 115.71 (C≡N), 167.12 (-CONH-), 172.01 (C=C), 173.96 (-CSNH-), Anal: Found: C, 65.29; H, 4.27; N, 12.01; S, 9.13. Calcd for C19H15N3SO2: C, 65.31; H, 4.33; N, 12.03; O, 9.16; S, 9.18%.

P8: 5-Cyano-1-(4-fluoro-phenyl)-6-(4-methoxyphenyl)-2-thiouracil

I.R.: ν cm-1 2995 (C-H), 3280 (N-H), 2240 (C≡N), 1590 (C=O), 1262 (C=S), 1280 (O-CH3), 1HNMR: δ (ppm): 8.13-8.15 (s, 1H, NH), 7.33-7.98 (m, 8H, ArH), 3.85-3.90 (s, 3H, OCH3), 13CNMR: 55.88 (OCH3), 72.55 (C=C), 114.32-129.56 (10C), 159.10 (N-phenyl C4), 159.79 (phenyl C4), 115.68 (C≡N), 167.22 (-CONH-), 171.57 (C=C), 174.13 (-CSNH-), Anal: Found: C, 61.33; H, 3.36; N, 11.90; S, 9.06. Calcd for C18H12FN3SO2: C, 61.18; H, 3.42; F, 5.38; N, 11.89; O, 9.06; S, 9.07%.

P9: 5-Cyano-1-(2,4-dimethyl-phenyl)-6-(4-dimethylamino-phenyl)-2-thiouracil

I.R.: ν cm-1 3002 (C-H), 3300 (N-H), 2245 (C≡N), 1590 (C=O), 1250 (C=S), 1HNMR: δ (ppm): 8.02 (s, 1H, NH), 7.36-7.90 (m, 7H, ArH), 2.25-2.30 (d, 12H, CH3), 13CNMR: 16.35 (CH3), 24.65 (CH3), 40.23 (-N(CH3)2), 72.78 (C=C), 114.12-133.98 (9C), 134.43(N-phenyl C4), 139.15 (N-phenyl C2), 148.78 (phenyl C4), 115.68 (C≡N), 167.12 (-CONH-), 171.57 (C=C), 174.11 (-CSNH-), Anal: Found: C, 67.01; H, 5.28; N, 14.86; S, 8.49. Calcd for C21H20N4SO: C, 67.00; H, 5.35; N, 14.88; O, 4.25; S, 8.52%.

P10: 5-Cyano-1-phenyl-6-(4-dimethylamino-phenyl)-2-thiouracil

I.R.: ν cm-1 3012 (C-H), 3275 (N-H), 2260 (C≡N), 1595 (C=O), 1270 (C=S), 1HNMR: δ (ppm): 8.03 (s, 1H, NH), 7.34-7.91 (m, 9H, ArH), 3.10-3.79 (s, 6H, CH3), 13CNMR: 40.31 (-N(CH3)2), 72.87 (C=C), 114.22-133.95 (11C), 148.78 (phenyl C4), 115.60 (C≡N), 167.02 (-CONH-), 171.79 (C=C), 174.13 (-CSNH-), Anal: Found: C, 65.48; H, 4.56; N, 16.03; S, 9.16. Calcd for C19H16N4SO: C, 65.50; H, 4.63; N, 16.08; O, 4.59; S, 9.20%.

Antimicrobial activity

All synthesized compounds were screened for antibacterial activity by cup- plate method against gram-positive species S. aureus and B. subtilis and gram-negative species E. coli and P.aeruginosa in the concentration of 25 μg. These compounds were also screened for antifungal activity against fungi C. albicans in the same concentration. The activities were compared with standard antibiotics; norfloxacin and grisievofulvin. All the synthesized compounds were dissolved in dimethyl sulphoxide, which was used as a control. The plates were incubated at 37 ℃ for 24 hours and the zone of inhibition was measured in mm.

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