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Transcript
Nonsteroidal Antiinflammatory Drugs • 1. Non selective drugs • Salicylates e.g. Aspirin is the prototype drug • Mechanisms of action • 1- Antiinflammatory • A) Inhibit prostaglandines synthesis through irreversible inhibition of cyclo-oxygenase enzymes ( Cox-1 & Cox-2). • B) Interferes with the chemical mediators of the kallikrein system. Mechanisms of action (cont.) • B) Inhibits the migration of polymorphonuclear leukocytes to the site of inflammation. • C) Anti-oxidant activity. • D) Stabilizing lysosomes 2- Analgesics • 1- For mild & moderate dull aching pain as antiinflammatory • 2- Inhibits pain stimuli at subcortical site 3- Antipyretic • 1- COX inhibition in the C.N.S. • 2- Inhibition of IL-1 4- Antiplatelet • Irreversible inhibition of platelet COX • Aspirin effect lasts 8-10 days ( life of platelets ) Pharmacological actions • • • • • A) Analgesic B) Antipyretic C) Antithrombotic D)Anti-inflammatory E) Uricosuric ( large dos) Clinical uses • • • • • • A) Analgesic B) Antipyretic C) Anti-inflammatory D) Antithrombotic( cardioprotective) E) Chronic gouty arthritis F)Cancer pain in combination with opioid drugs Adverse effects • • • • • • At therapeutic doses A) Gastric upset ( intolerance) & gastric or duodenal ulceration B) Gouty arthritis C) Asthma, rashes D) Hepatotoxicity & renal toxicity are less frequent. • E) Reye syndrome High doses or Prolonged use of aspirin • A) Salicylism( tinnitus,vertigo, decreased hearing). • B) Hyperapnea • C)Respiratory alkalosis • D) Metabolic acidoses • E) Hyperthermia • F) Gastric & doudenal ulcer & bleeding • H) Glucose intolerance Contraindications • A) Pregnancy • B) Haemophilic patients • C) Hypersensitivity reaction to aspirin • D) Viral infections mainly in children • E) Peptic ulcers Drug-Drug interactions • Potentiates the gastric irritant effect of alcohol • Potentiates the hypoglycaemic effects of oral hypoglycaemic drugs PARACETAMOL • Is effective only as analgesic & antipyretic. • Has no antiinflammatory effect. • Has no platelet effect. • Can be used in patients with haemophilia or peptic ulcer or allergic to aspirin. PARACETAMOL (cont.) • Can be used during pregnancy. • In children with viral infections. ADVERSE EFFECTS • Mainly on liver due to its active metabolite ( N-acetyl-pbenzoquinone). • At therapeutic doses increases hepatic enzymes. • At high doses causes hepatic necrosis & renal necrosis. • Treatment of paracetamol toxicity with N-acetylcystine (SH donor ) as life saving 2-Propionic acid derivatives • 1. Ibuprofen • Pharmacokinetics • Rapidly absorbed after oral ingestion. • Half-life 1-2 hours • Highly bound to plasma proteins • Excreted through kidney as metabolites. Ibuprofen • The same mechanism & pharmacological actions of aspirin Except that it is reversible inhibitor for COX enzymes • More potent as antiinflammatory than aspirin Clinical uses • • • • • A) Analgesic B) Antipyretic C) Anti-inflammatory D)Acute gouty arthritis E) Patent ductus arteriosus Preparations of Ibuprofen • Oral preparations. • Topical cream for osteoarthritis. • A liquid gel for rapid relief of postsurgical dental pain. • Intravenous route as In patent ductus arteriosus Adverse effects • 1. Gastric upset ( less frequent than aspirin ). • 2. Fluid retention • 3.Hypersensetivity reactions • 4. Ocular disturbances • 5. Rare hematologic effects(agranulocytosis & aplastic anaemia ). Contraindications • • • • • • • 1. Peptic ulcer 2. Allergic patients to aspirin 3. Kidney impairment 4.Liver diseases 5.Pregnancy 6.Haemophilic patients The concomitant administration of ibuprofen antagonizes the irrevesible platelet inhibition of aspirin( limit cardioprotective effect of aspirin ). Oxicam derivatives • Piroxicam • Tenoxicam Piroxicam • Mechanism of actions • A) Non-selective inhibitors to Cox1 & Cox2 • B) Traps free radicals • C) Inhibits polymorphonuclear leukocytes migration • D) Inhibits lymphocyte function. Pharmacokinetics • Well absorbed orally • Half- Life 45 hours • Given once daily Adverse effects • Less frequent gastric upset (20%) . • Dizziness • Tinnitus • Headache • Allergy Acetic acid derivatives • 1. Diclofenac • Mechanism of action • A) As aspirin ,but non-selective inhibitor to cox1 & Cox2. • More potent as antiinflammatory than analgesic and antipyretics Pharmacokinetics • Accumulates in synovial Fluid Clinical uses • • • • • • A) Any inflammatory conditions B) Musculoskeletal pain C) Dysmenorrhoea D)Acute gouty arthritis E) Fever F) Locally to prevent or treat post opthalmic inflammation • G) A topical gel for solar keratoses Adverse effects • Gastric upset • Renal impairment • Elevation of serum aminotransferase • Salt & water retention Preparations of Diclofenac • Diclofenac with misoprostol decreases upper gastrointestinal ulceration ,but result in diarrhea. • Diclofenac with omeprazole to prevent recurrent bleeding. • .1% opthalmic preparation for postoperative opthalmic inflammation. • A topical gel 3% for solar keratoses. • Rectal suppository as analgesic or for postoperative nausea. Preparations of Diclofenac • Oral mouth wash. • Intramuscular preparations. Selective Cox2 inhibitors • Advantages : • 1. Highly selective inhibitors to cox2 enzyme. • 2. Potent anti-inflammatory. • 3. Have analgesic& antipyretic • 4. Highly bound to plasma proteins. Selective Cox2 inhibitors • 5. Lower incidence of gastric upset • 6. No effect on platelet aggregation (cox1 ) • 7. Renal toxicities ( they are not recommended for patients with severe renal insufficiency) • 8. High incidence of cardiovascular thrombotic events with some of them as rofecoxib. Selective Cox2 inhibitors • 9- They are recommended in postoperative patients undergoing bone repair. • 10- Also, indicated in primary familial adenomatous polyposis, dysmenorrhea, • Acute gouty arthritis, acute musculoskeletal pain , ankylosing spondylitis. Celecoxib • • • • • Absorption is decreased by food. Half-life 11hours Highly bound to plasma proteins No effect on platelet aggregation Metabolized in liver by CYP2C9 to in active metabolite. • Its clearance is decreased in liver impairment. • Given twice daily. Clinical uses • Rheumatoid arthritis • Osteoarthritis Side effects • Dyspepsia & heart burn. • edema & renal adverse effects. • Allergy (skin rash ). Drug interactions • With warfarrin potentiate its,through interfering with its metabolism. actions Meloxicam • Relatively selective Cox2 inhibitors. • Safer than piroxicam. Pharmacokinetics • Given orally ,rectally, I.M.,I.V. • Metabolized in liver to inactive metabolites. • Excreted in urine 50% and in feces 50%. • Half-life 20 hours. • Given once daily. Clinical uses • Analgesic • Rheumatoid arthritis • Osteoarthritis. Adverse effects • Gastric upset • Skin rash • Headache Drug interactions • Cholestyramine increases the clearance of the drug . Nabumetone • Well absorbed orally. • Metabolized in liver to active metabolities. • Half-life 26 hours. • Taken once daily. Clinical uses • Rheumatoid arthritis • Osteoarthritis Adverse effects • • • • • • Gastric upset Allergy (skin rash ). Headache Tinnitus Pseudoporphyria Photosensitivity Slow acting anti-inflammatory drugs(Disease modifying drugs ). • 1.Used as a second line in treating arthritis. • 2.When the disease is progressing & causing deformties. • 3. Can not repair existing damage,but prevent further injury. Slow acting anti-inflammatory drugs(Disease modifying drugs ). • 4. Have no analgesic effects • 5. Need weeks or months to act. Hydroxychloroquine • • • • • • Mechanism of action 1. Suppress T lymphocytes 2. Decrease leukocytes action 3. Stabilize lysosomal activity 4. Inhibits DNA& RNA synthesis 5. Traps free radicals Clinical uses • Arthritis used in a large doses & long duration Adverse effects • • • • • • • 1. 2. 3. 4. 5. 6. 7. Nausea & vomiting Cinchonism ( tinnitus.vertigo ) Irreversible retinal damage Ototoxicity Corneal deposits Allergic skin reaction Hepatitis Methotrexate • Mechanism of action • 1. Dihydrofolate reductase inhibitor • 2. Immunosuppressive agent Adverse effects • 1. Nausea • 2. Mucosal ulcers • 3. Bone marrow depression which can be reversed by leucovorin. • 4. Hepatotoxicity is dose related. Anti- TNF-alpha drugs • Infliximab • 1. Is a chimeric(25%mouse &75%human). • 2. Binds with high affinity to human TNF-alpha. • 3. Given as I.V. infusion • 4. Half-life 8-12 days. • 5. Given at 0,2,6 weeks followed by intervals of rest 4-6 weeks. Infliximab • Improvement reaches up to 60% • Can be used in combination with methotrexate reduce the prevalence of human antichimeric antibodies. Clinical uses • • • • • • Rheumatoid arthritis Ulcerative colitis Psoriasis Psoriatic arthritis Giant cell arteritis Sarcoidosis Adverse effects • • • • • • • 1. 2. 3. 4. 5. 67- Upper respiratory tract infections. Cough. Nausea. Headache. Rash. Activate latent tuberculosis Infusion site reaction Leflunomide • 1. Immunosuppressive drug used in the treatment of R.A. • 2. Undergoes rapid conversion in intestinal mucosa & plasma to active metabolities. Pharmacokinetics • • • • Orally effective Half-life 15 days Highly bound to plasma proteins Cholestyramine increases its clearance Mechanism of action • 1. Inhibits dihydroorotate dehydrogenase which lead to inhibition of ribonucleotide synthesis & arrest the stimulated cells in G1 phase. • 2. Inhibits T cell proliferation & production of autoantibodies by β cells. Mechanism ( cont.) • Increase interleukin 10 receptor • mRNA. • Decrease interleukin 8 receptor type A m RNA. • Decrease TNF-α- dependent NFkB Clinical uses • Rheumatoid arthritis • Can be given with methtrxate Adverse effects • • • • • • • Diarrhea Elevated liver enzymes Mild alopecia Weight gain Increased blood pressure Leukopenia & thrombocytopenia Contraindicated in pregnancy SulfASALAZINE • MECHANISM OF ACTION • Through its active metabolite sulfapyridine &the parent drug itself. • Suppression of T cell . • Inhibition of B cell proliferation Pharmacokinetics • Only 10-20% of orally administered sulfa is absorbed. • Fraction undergoes enterohepatic circulation into the bowel. • Reduced by intestinal bacteria to liberate 5-aminosalicylic acid Pharmacokinetics • And sulfapyridine which is well absorbed while 5-aminosalicylic remains unabsorbed. • Excreted partly unchanged as sulfasalazine in urine • Sulfapyridine metabolized in liver by acetylation &hydroxylation • Half-life 6-17 hours. Clinical uses • Rheumatoid arthritis reduce the rate of appearance of new joint damage. • Juvenile chronic arthritis • Ankylosing spondylitis. Adverse effects • • • • • • • Nausea, vomiting Headache Skin rash Hemolytic anemia Methemoglobinemia Reversible infertility in men Neutropenia & thrombocytopenia (rare)
