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Chemotherapeutic Agents / Antibiotics, chapter 34-39 •Antibacterial compounds (procaryotes) •Antiparasitic agents (eucarytotes) - Chapt 35 •Antifungal compounds (eucarytotes) •Antiviral compounds •Anticancer compounds Protozoa Helmints Insects (Scabies lice etc.) (Fungi chapt. 36) Protozoa Eucaryotes, unicellular (may exist in colonies) Protozoa and algae (protocista) Complex replication (sexual and asexual) Patogenic P. most common tropical area 3. world diseases Many diseases can be prevented by clean drinking water Certain protozal diseases spread by insects Ex. patogenic protozoa Trichomonas vaginalis: Gelital infections Giardia lamblia: Diarea Toxoplasma gondii: Toksoplasmosis Trypanozomas sp: Sleeping sickness Entamoeba histolytica: Dysen tery Plasmodium sp: Malaria Pneumocystis carinii: Oportunistic, AIDS Treatment of diseases caused by amebia, giardia, trichomonas Related comp. treatment of African sleeping sickness Metronidazol Flagyl®, Metronidazol® N O2N CH 3 N OH N O2N N CH3 Also effective against anaerobic bacteria Probably pro-drug -reductive activation (mech. not fully understood) Anaerobe org. e- O2N N O SO2 N O2N N N CH3 O2N OH N N Metabol O2N CH3 N OH N O2N OH OH Active metabol. HO-OH 2 HO OH N O OH OH O O N O2 Phase II conjugation Formation of toxic reactive oxygen species O OH O NH OH H2N O CH3 Anti - Malaria drugs Plasmodium sp. Vektor: Anopheles moskito. Complex life cyclus. Mal aria = bad air 40% of world population at risk 300 mil acute illnessess pr year ca 1 mill deaths pr year Malaria kills a child every 30 sec. 90% in incidents sub-sahara Africa De fleste l.m. aktive her Historic drugs -Azodyes and salvarsan (1. synthetic effective drug) -Quinine fra Cinchona (Kinabark) HO N MeO Azo dyes Bayer etc Late 1800-century, ex. HO3S Salvarsan 1. antisyphilis drug 1912 N N HO HO Quinine Quinoline As As Pararødt N H2N N Metylorange O2N N N OH MOdern antimalarials NH2 N Cinchona pubescens (Kinatre) from South America Screening of dyes as antibacterials 1932: Prontocil active against Streptoccocces infection no activity on bacterial cultures O H2N S O H2N N N NH2 1935: Prontocil metabilized (azoreductase) to Sulfanilamid in vivo O H2N S O NH2 Modern sulfa drugsr O H R N S O NH2 R: Aryl or hetroaryl (rel. toxisk) Quinolines Mechanism (DNA Intercalation) Ferriprotoporphyrin IX: Binds to FPIX (metabolite from hemoglobine); tox. form of FPIX, proteinbound FPIX less tox.) Weak base Hypothesis: Increase pH in parasite Quinine Kinin® Hydroksyklorokin Plaquenil® Klorokin Klorokinfosfat® HO N HO N NH NH N MeO Cl Cl N N Meflokin Lariam® N More active, less tox (comp Quinine) Resistance! HO N H N Dye Quinine N H3CO NH N Pamakin, 1926 N NH Cl klorokin N CF 3 CF 3 Also klorokin resistant P. palsifarum Biguanides Pro-drug Proguanil (= Chloroguanide) Inhib. protozoan folate reduktase Paludrine® (c.f. Trimetoprim) Malarone® + atovakvon taut. NH Cl NH NH 5 1 3 N 2 N 4 N H H H Liver 6 Cl NH NH - H2 Imine 3 H2N 2 N 4 NH2 1N O N H2N N O H2N N N Folinsyre OH OH N OH N H Fra folinsyre i kosten hos mennesker N H Dehydropteridinsyre PABA N H2N N H N NH N H N H CO2H NH2 OCH 3 N N N H N H Dehydrofolinsyre Trimetoprim H2N N N H2N N NH OH Folatreduktase CO2H Tetrahydrofolinsyre Essensielle prossesser hos bakterier og dyr Inkl tymidinsyntese Other biguanides Klorhexidine O O OH N5 CO2H O R S NH O O H2N enol N Antibakt sulfonamid H2N keto Cycloguanil CO2H N H OH 6 Cl NH N taut. O Proguanil (chloroguanide) OH enamine N N H N H NH2 OCH 3 OCH 3 CO2H Cl NH CO2H N H N H NH N H H N H N NH H N NH Cl Others O Cl OH H3CO 8 O H3CO CH3 O O ox Malarone® + proguanil. Also other parasites (P. carinii) Ubiquinone antimetabolite? H O O O O O H H Artemisin from Artemisia annua Chinesee trad. med. H O MeO O O O H Mech. involves radicals H Artemeter Semisynth. analog Improved solubil. Artemeter og Lumefandrin Riamet® R H3CO Ubiquinone, Q10, Cenzyme Q electron carrier cellular respiration OH Atovakvon Red H3CO No cross resist. Synth. analogs, active field CH3 OH Drugs for Helmint infections Eukaryotes – Invertebrates. Tropical diseases! Animal parasites; ex Trichinella spiralis (trikiner). Benzimidazoles Many active analogs known Binds to tubulin - prevents formation of microtubules inhib. mitosis (c.f. certain anticancer drugs) May also inhib. fumarate reductase Mebendazol Vermox® O N NH N H OMe O Drugs against Ectoparasites (insects) Lice, scabies etc Pyretrines Insecticides from Crysantemum sp O R' R Cl O O O Chlorinated pesticides: Lindane Block GABA CNS neurtransmittor (Also neurotox. effects on humans) Cl Cl Cl Cl Cl Cl Cl O Synth. analog, more stabile Mixt. of 4 stereoisomers Permetrin Nix® Irreversible Inhibitors Acetylcholine esterase Not drugs, nerve gasses, insecticides etc. Malation Prioderm® lice Gen structur mustard gasses L R2 P R1 N O N L: Leaving group R1: alkoksy R2: alkyl, alkoksy, amino P F O P O O O O O O Sarin Tabun O OH O Aging OH R2 Pralidoxim P O R1 OR L P O OR O P R1 O OH HO OH N L R1 N Me Pralidoxim motgift OH OR O P R1 O N N Me O O S P O S P OR O only insects O P O O S O O O Malation Malaoxon not tox. Act as mustard gasses Chemotherapeutic Agents / Antibiotics, chapter 34-39 •Antibacterial compounds (procaryotes) •Antiparasitic agents (eucarytotes) •Antifungal compounds (eucarytotes) - Chapt 36 •Antiviral compounds •Anticancer compounds Fungicides / Fungistatika / Antimykotika Chemotherapeutics / Antibiotics Synthetic Antifungals N Azoles N N H Azol / Pyrrol N H 1,2-Diazol 1,3-Diazol / Imidazol Squalen epoksidsyklase Squalen epoksidase HO O Squalen N H Antimycotic allylic amines H Lanosterol Lanosterol 14a-demetylase Antimycotic azoles Component of fungus cell walls HO HO Ergosterol H H HO H Kolesterol H N N N H 1,2,4-Triazol Lanosterol CH2OH CH3 HO HO H O N N Fe N N H C(OH)3 HO H HCO2H 14a-demethylase heme (CYP450 fungi) N R N N N Fe N N Antimyc. azole HO H Klotrimazol: Canesten®, Klotrimazol® utvortes Canesten®, vaginal behandlig Ekonazol: Pevaryl®, utvortes Pevaryl®, vaginal behandlig Miconazol: Daktar®, utvortes Daktar®, vaginal behandlig Cl N N Cl Cl N N Cl O X=H: Ekonazol X=Cl: Mikonazol X Ketokonazol: Cl O N N Cl SAR: O O N N O -Weakly basic azole ring, imidazol / 1,2,4-triazol "cis", [±] F N Vorikonazol F OH N (R) N (less tox. humans), pKa 6.5-6.8 Flukonazol N -2 or 3 other aromatic rings (Racemate) -Cl (or F) on at least one aromatic ring N (s) F (F i flukonazol) Cl Itrakonazol: O N N N O Cl O N N N O N N -Lipophilic structures (as lanosterol) Squalen epoksidsyklase Squalen epoksidase Allylic amines Terbinafin Lamicil® HO O Squalen Antimycotic allylic amines H Lanosterol Lanosterol 14a-demetylase Antimycotic azoles N HO Prevents formation of cell wall comp. Accumulation of toxic squalene HO H Ergosterol H H Kolesterol H HO Enzyme-Nu Enz--Nu Squalene epoxide cyclase B Squalene epoxidase H H H HO O H HO H H Lanosterol (Animals Fungi) Antimycotic Antibiotics OH n n Polyenes O O O Aminosukker Proad spectrum. Some effect on certain protozoa. Isolated, Streptomyces sp. Binds to sterols in fungal cell membrane; cell leaks K+, small org. molecules SAR: •Macrolaktone [26 eor 38-ring, Larger than macrolides ( erytromycin etc)] •Polyene (Macrolides not polyenes) •Several OH-groups •amino sugar, mykosamin •Bad water sol. OH O HO O HO HO HO HO OH O O OH N CO2H HO HO HO Nystatin A O OH NH2 OH O O O O O HO O O O OH Erytromycin Nystatin A Amfotericin B toxic, bad oral avail; Local treatment, mouth, GI tract Systhemic infect (infusion) Somewhat less tox. OH OH O OH O HO O HO HO HO HO OH O HO OH O HO OH HO HO O CO2H O Amfotericin B Nystatin A O O OH O OH CO2H OH OH NH 2 OH NH 2 Amfotær struktur OH OH OH O CO 2H O Hemiacetal OH OH O OH CO 2 O HO O O OH NH 2 OH O O OH NH 3 CO 2H CO 2H OH O O OH NH 2 OH O O OH OH NH 2 OH Peptides Caspofungin Serious systhemic infect. Semisynth. from prod. of fermentation ( Glarea lozoyensis) Inhib. synth of b-1,3-D-glucan; cell wall comp. certain fungi Few good inhib. of fungi cell wall comp. compared to antibacterials Chemotherapeutic Agents / Antibiotics, chapter 34-39 •Antibacterial compounds (procaryotes)-Antimycobacterials •Antiparasitic agents (eucarytotes) •Antifungal compounds (eucarytotes) •Antiviral compounds •Anticancer compounds G+ G- Mycobacteria chapt. 37 Pathog enic mycoba cteria: M. tuberculosis (tuberculosis) M. Leprae (Leprosy) M. Avium (Opportunistic infection in AIDS patients) M. bovis (mainly cattle infect, infected milk USA) 30 million people will die from TB the next 10 years TUBERCULOSIS (TB) High lipid / wax content in cell wall (myco lic acid) Slow growing orga nisms Aerobe bacteria Resistant to chemicals and drying Easily killed by heat 8 million new cases each year ca. 1/3 of the world population are infected (incl. dormant infections) ca. 95% of the cases in developing countries no new drugs on the marked for the last 25 - 30 years Until ca. 1950; 50 % o f all infected died Infection by inhalation of the bacteria Pulmonary TB mo st co mmon May also attack other orga ns including CNS WHO (1993): TB a "global emergency" First effective drug: Streptomycin 1946 H2 N HN O HO HO HO O HO HO NH OH NH NH OH H2 N NHMe Inhibits protein synthesis Toxic! Treatment •Long time ≥6 mnds •Combination of drugs Different stages of bacterial growth DOT: Directly observed therapy First-line drugs Isoniazid N O Isoniazid® O HN NHNH 2 Isoniazide Antituberculosis drug NH2 Mn2+ /O N O H H O N N Active acyl radical formed in vivo H O O NH2 NH2 N N NADH co-enzyme in enzyme involved in cell wall component synth Inactive der. of co-enz Long Chain ACP-Enoyl Fatty Acid Reductase (inhA) APC: Acyl carrier protein) O OH ((CH ) CH 2 23 3 CH3(CH2)1'7 14 17 CO2H -mycolates O CH3(CH2)17 17 15 ketomycolates H3CO CH3(CH2)17 OH ((CH ) CH 2 23 3 Mycolic acid ACP R R H H O O NH2 CO2H 1,4 hydride add. N OH ((CH ) CH 2 23 3 17 15 methoxymycolates O ACP CO2H NADH co-enzyme inhA NH2 N NAD+ First-line drugs Ethambutol Pyrazinamide O OH NHNH2 O NHNH2 N H N HO N N H N Isoniazide Mechanism not fully known Synth of cell wall comp.: Inhib. arabinocyl transferase? Mechanism not known Arabinose, Arabinomannan and Lipoarabinomannan Rifampicin Rimactan® Broad spectrum antibiotic From Streptomyces sp HO MeCO 2 OH OH O MeO O Rifampicin Inhib bacterial RNA polymerase Inhib. RNA-synth. (p-p intract. naphtalene rings aromatic AA?) OH OH NH N O OH O N Induce CYP2C; increased metabol. of certain anti AIDS drugs Second-line drugs Ethionamide NH2 S Cycloserine Isolated Spreptomyces sp p-Aminosalicylic acid CO2H OH H2N O O N NH2 Mech. ≈ Isoniazide PABA antimetabolite NHNH2 O Folic acid synth (≈antibact. sulfa ) N Isoniazide Kanamycin (aminoglycoside antibiotics) NH2 O R O HO HO NH2 HO HO O O H2N OH R=OH: Kanamycin A R=NH2: Kanamycin B NH2 NH Inhib. alanine racemase and alanine ligase; Inhib. peptidoglycan synth Others Oxazolidinones Quinolones O R F O CO2H O R N R R N N F O NH O Treatment of MAC infections Clarithromycin (Macrolide) O N HO HO O HO MeO O Ethambutol O O Quinolones O O Other macrolides O OH Rifabutin (Rifamycin)