Download presentation
Presentation is loading. Please wait.
1
قالوا سبحانك لا علم لنا إلا ما علمتنا إنك أنت العليم الحكيم صدق الله العظيم صدق الله العظيم (سورة البقرة 32) (سورة البقرة 32)
2
SYNTHESIS AND BIOLOGICAL TESTING OF NEW 1-ADAMANTYL DERIVATIVES
4
Pharmacological Properties of Adamantane Derivatives Antiviral Activities Antimicrobial Activities Anti-inflammatory Activity CNS Activities 11 -HSD1 Inhibitory Activity Miscellaneous Activities
5
Antiviral Adamantane Derivatives Anti-Influenza and Anti-Herpes viruses
8
Anti-HIV Derivatives
9
Antimicrobial Adamantane Derivatives
13
Anti-inflammatory Adamantane Derivatives
15
CNS Activities Anti-Parkinsonian Activity The high lipophilicity of the adamantane derivatives enables them to pass through the blood brain barriers leading to the existence of high levels of these derivatives in the central nervous system The therapeutic efficacy of amantadine in the symptomatic treatment of Parkinson's disease was discovered in 1969 Amantadine is known to increase the synthesis, release and uptake of dopamine in the striatum Amantadine was found to act as blocker of brain monoamineoxidase A and as non-competitive N-methyl-D-aspartate (NMDA)-receptor antagonist thereby influencing the dopamine transmission
18
11 -HSD1 Inhibitory Activity
23
Pharmacological Properties of 1,2,4-Triazoles 1,2,4-Triazoles (s-triazoles) and their fused heterocyclic derivatives are known for their diverse pharmacological activities. The most interesting of these are the anti- inflammatory, analgesic, antibacterial, antifungal and other activities.
24
Anti-inflammatory 1,2,4-triazole derivatives
26
Antimicrobial 1,2,4-triazole derivatives
29
1,2,4-Triazolo[3,4-b][1,3,4]thiadiazoles
![1,2,4-Triazolo[3,4-b][1,3,4]thiadiazoles](http://images.slideplayer.com/16/5087739/slides/slide_29.jpg "1,2,4-Triazolo[3,4-b][1,3,4]thiadiazoles")
30
Pharmacological Properties of 1,3,4-Thiadiazoles 1,3,4-Thiadiazole-2-sulphonamides were early known as carbonic anhydrase inhibitors which are clinically useful in the treatment of various diseases such as glaucoma, epilepsy, congestive heart failure, mountain sickness, gastric and duodenal ulcers and other neurological disorders Antibacterial, antifungal and anti-inflammatory activities were also reported for several 1,3,4-thiadiazole derivatives
31
1,3,4-Thiadiazoles as Carbonic Anhydrase Inhibitors
32
Antimicrobial 1,3,4-Thiadiazoles
35
RESEARCH OBJECTIVES
38
NMR data of compound 145b
39
NMR data of compound 146e
41
NMR data of compound 149c
43
NMR data of compound 150j
46
NMR data of compound 151e
49
NMR data of compound 151o
52
NMR data of compound 152i
56
NMR data of compound 154c
57
NMR data of compound 155b
59
NMR data of compound 157
61
NMR data of compound 164a
62
BIOLOGICAL TESTING In vitro antimicrobial testing (all new compounds) In vivo acute anti-inflammatory testing in rats (26 compounds) Oral acute toxicity of compounds 151l and 159 in mice.
63
Antimicrobial Activity The primary screening was carried out using the agar disc-diffusion method using Müller-Hinton agar medium for measuring the growth inhibitory activity against the standard strains of the Gram-positive bacteria: Staphylococcus aureus IFO 3060, Bacillus subtilis IFO 3007, Micrococcus luteus IFO 3232, the Gram-negative bacteria Escherichia coli IFO 3301, Pseudomonas aeuroginosa IFO 3448 and the yeast-like pathogenic fungus Candida albicans IFO 0583 The minimal inhibitory concentration (MIC) for the most active compounds against the same microorganism used in the primary screening was carried out using the microdilution susceptibility method in Müller- Hinton Broth and Sabouraud Liquid Medium
64
Diameter of Growth Inhibition Zone (mm)Ar/R Comp. No. C APAECMLBSSA ---202216C6H5C6H5 145a ---1820153-FC 6 H 4 145b ---1618134-FC 6 H 4 145c ---1318154-ClC 6 H 4 145d ---1127224-BrC 6 H 4 145e ----10-C6H5C6H5 146a ----12-3-FC 6 H 4 146b ----12-4-FC 6 H 4 146c ----11-4-ClC 6 H 4 146d ---1012-4-BrC 6 H 4 146e ---1213-NH 2 148 ----11-CH 3 NH149a ------CH 3 CH 2 NH149b ------CH 3 (CH 2 ) 3 NH149c ------CH 2 =CH-CH 2 NH149d ------C 6 H 5 CH 2 NH149e NT1920182526Gentamicin NT1617192123Ampicillin 21NT Clotrimazole
65
Diameter of Growth Inhibition Zone (mm)R Comp. No. C APAECMLBSSA ----1310 H 150a ----14 2-F 150b 17--- 16 4-F 150c ----1411 2-Cl 150d ----1614 4-Cl 150e 16--14 13 4-Br 150f -1315121614 2-OH 150g -1419132519 4-OH 150h ---151815 4-CH 3 150i ------ 2-OCH 3 150j ------ 4-OCH 3 150k ----14 2-NO 2 150l ------ 4-NO 2 150m ------ 4-(CH 3 ) 2 N 150n ----1918 2,6-F 2 150o ------ 2-Cl,6-F 150p ----1614 2,6-Cl 2 150q ----1716 2,4-Cl 2 150r 12---17 3,4-Cl 2 150s ------ 3,4-(CH 3 O) 2 150t ------ 2,4-(NO 2 ) 2 150u ------ 2-NO 2,4,5- (CH 3 O) 2 150v
66
Diameter of Growth Inhibition Zone (mm)R Comp. No. C APAECMLBSSA ----1513 CH 3 151a --15-1415 C2H5C2H5 151b ----1511 COOC 2 H 5 151c ---14-- C6H5C6H5 151d -12---- 4-FC 6 H 4 151e -1118-1112 3-CF 3 C 6 H 4 151f ------ 2-CH 3 OC 6 H 4 151g 17----- C 6 H 5 CH 2 151h ----1112 CH 3 151i ----1214 C2H5C2H5 151j ----11- COOC 2 H 5 151k ------ C6H5C6H5 151l ----1213 4-FC 6 H 4 151m -1419--- 3-CF 3 C 6 H 4 151n ------ 2-CH 3 OC 6 H 4 151o ------ C 6 H 5 CH 2 151p NT1920182526Gentamicin NT1617192123Ampicillin 21NT Clotrimazole
67
Diameter of Growth Inhibition Zone (mm)R Comp. No. C APAECMLBSSA ---161912 H 152a ------ 2-F 152b --15--- 2-Cl 152c ----1511 4-CH 3 152d 13---2217 2-OH 152e 19---2622 4-OH 152f ----1115 4-OCH 3 152g 14----- 2,6-F 2 152h ----1514 2-Cl,6-F 152i ---16 12 2,6-Cl 2 152j ----1715 2,4-Cl 2 152k ----1311 3,4-Cl 2 152l -1619172420 3,4-(CH 3 O) 2 152m ------ 2-NO 2,4,5-(CH 3 O) 2 152n NT1920182526Gentamicin NT1617192123Ampicillin 21NT Clotrimazole
68
Diameter of Growth Inhibition Zone (mm)R/X Comp. No. C APAECMLBSSA -2027-13 - 153 ------ H 154a 14----- F 154b ------ Cl 154c ------ NO 2 154d ---14 13 CH 3 155a ----1312 CH 3 CH 2 155b ----14- C6H5C6H5 155c 17--162218 - 157 ---132018 - 159 11---1311 - 161 NT1920182526Gentamicin NT1617192123Ampicillin 21NT Clotrimazole
69
Diameter of Growth Inhibition Zone (mm)X Comp. No. C APAECMLBSSA ---151413 H 164a ---111914 F 164b ---122015 Cl 164c ------ - 165 NT1920182526Gentamicin NT1617192123Ampicillin 21NT Clotrimazole
70
Minimal Inhibitory Concentration (MIC, g/ml) Comp. No. C APAECMLBSSA ND 22 145a ND 4 145b ND 12145e ND 2 12150h ND 4 150o ND 2 151n ND 4 152a ND 2 152e 8ND 12152f ND 2 12152m ND20.5ND 153 ND 2 157 ND 4 159 ND 4 164b ND 2 164c ND10.5222Gentamicin ND2220.52Ampicillin 2ND Clotrimazole
71
Anti-inflammatory Testing The acute anti-inflammatory activity of 26 representative compounds was determined in vivo following the carrageenan-induced paw oedema method in rats The selection of the representative compounds and dose levels were made after carrying out pilot experiments which showed the absence of anti-inflammatory activity in compounds 146a-e, 148 and 149a-e The compounds were tested at 20 and 40 mg/kg dose levels
72
Mean % Reduction of paw oedemaR/XComp. No. 40 mg/kg20 mg/kg 19.3721.923,4-(CH 3 O) 2 150t 39.8839.16C6H5C6H5 151d 38.3725.882-CH 3 OC 6 H 4 151g 34.7627.95C2H5C2H5 151j 50.4428.86C6H5C6H5 151l 22.9013.064-FC 6 H 4 151m 15.2723.23H152a 37.6633.022-Cl152c 31.2020.412-OH152e 35.0110.453,4-Cl 2 152l 10.6211.32C2H5C2H5 155b 32.7029.54-157 65.1950.60-159 36.837.47-161 52.79Indomethacin (5 mg/kg)
73
Oral Acute Toxicity Testing (gm/kg) LD 50 (95% Confidence limit)LD 84 LD 50 LD 16 Comp. No. 1.64 (1.23-1.89)2.881.640.82151l 2.52 (1.97-3.10)4.432.521.77159
74
Thank You
Similar presentations
