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THE EICOSANOIDS: PROSTAGLANDINS, THROMBOXANES, LEUKOTRIENES, & RELATED COMPOUNDS

THE EICOSANOIDS: PROSTAGLANDINS, THROMBOXANES, LEUKOTRIENES, & RELATED COMPOUNDS. Dr. Haitham M. Al- Wali P h .D Pharmacology. PROSTAGLANDINS.

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THE EICOSANOIDS: PROSTAGLANDINS, THROMBOXANES, LEUKOTRIENES, & RELATED COMPOUNDS

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  1. THE EICOSANOIDS: PROSTAGLANDINS, THROMBOXANES, LEUKOTRIENES, & RELATED COMPOUNDS Dr. Haitham M. Al-Wali Ph.D Pharmacology

  2. PROSTAGLANDINS • The NSAIDs act by inhibiting the synthesis of prostaglandins. Thus, an understanding of NSAIDs requires comprehension of the actions and biosynthesis of prostaglandins—unsaturated fatty acid derivatives containing 20 carbons that include a cyclic ring structure. [Note: These compounds are sometimes referred to as eicosanoids; “eicosa” refers to the 20 carbon atoms.]

  3. A. Role of prostaglandins as local mediators • Prostaglandins and related compounds are produced in minute quantities by nearly all tissues. • They generally act locally on the tissues, and they are rapidly metabolized to inactive products at their sites of action. Therefore, the prostaglandins do not circulate in the blood in significant concentrations. • Thromboxanesand leukotrienes are related lipids that are synthesized from the same precursors as the prostaglandins.

  4. B. Synthesis of prostaglandins • Arachidonic acid is the primary precursor of the prostaglandins and related compounds. • Arachidonic acid is present as a component of the phospholipids of cell membranes. • Tissue phospholipids---PLA2---→arachidonic acid • There are two major pathways in the synthesis of the eicosanoids from arachidonic acid, 1)the cyclooxygenase and 2)the lipoxygenase pathways.

  5. Cyclooxygenase pathway: All eicosanoids are synthesized via the cyclooxygenase pathway. Two related isoforms of the cyclooxygenase enzymes have been described. • Cyclooxygenase-1 (COX-1) is responsible for the physiologic production of prostanoids, whereas cyclooxygenase-2 (COX-2) causes the elevated production of prostanoids that occurs in sites of chronic disease and inflammation. • COX-1is a constitutive enzyme that regulates normal cellular processes, such as gastric cytoprotection, vascular homeostasis, platelet aggregation, and reproductive and kidney functions.

  6. COX-2 is constitutively expressed in tissues such as the brain, kidney, and bone. Its expression at other sites is increased during states of chronic inflammation. • Differences in binding site shape have permitted the development of selective COX-2 inhibitors. • COX-2 expression is induced by inflammatory mediators like TNF-α and IL-1 but can also be pharmacologically inhibited by glucocorticoids.

  7. 2. Lipoxygenase pathway: • several lipoxygenases can act on arachidonic acid to form leukotrienes • Antileukotriene drugs, such as zileuton, zafirlukast, and montelukast, are treatment options for asthma.

  8. C. Actions of prostaglandins • Vascular • TXA2and PGF2 are a potent vasoconstrictor. • Vasodilator prostaglandins, especially PGI2 and PGE2, promote vasodilation by increasing cAMP and decreasing smooth muscle intracellular calcium.

  9. Gastrointestinal Tract • Most of the prostaglandins and thromboxanesactivate gastrointestinal smooth muscle. Longitudinal muscle is contracted by PGE2 and PGF2, whereas circular muscle is contracted strongly by PGF2 and weakly by PGI2, and relaxed by PGE2 . Administration of either PGE2 or PGF2 results in colicky cramps .

  10. Airways Respiratory smooth muscle is relaxed by PGE2 and PGI2 and contracted by PGD2, TXA2, and PGF2. The leukotrienesare bronchoconstrictors. • PLATELETS Both PGD2 and PGI2 inhibit aggregation. TXA2 is the major product of platelet COX-1, is a platelet aggregator, and amplifies the effects of other more potent platelet agonists such as thrombin.

  11. Female Reproductive Organs • Uterine muscle is contracted by PGF2α, TXA2, and low concentrations of PGE2; PGI2 and high concentrations of PGE2 cause relaxation. • Male Reproductive Organs • Smooth muscle–relaxing prostaglandins such as PGE1 enhance penile erection by relaxing the smooth muscle of the corpora cavernosa.

  12. D. Therapeutic uses of prostaglandins • Prostaglandins have a major role in modulating pain, inflammation, and fever. • They also control many physiological functions, such as acid secretion and mucus production in the gastrointestinal (GI) tract, uterine contractions, and renal blood flow. • Prostaglandins are also among the chemical mediators that are released in allergic and inflammatory processes.

  13. Alprostadil • Alprostadilis a PGE1 that is naturally produced in tissues such as seminal vesicles and cavernous tissues, in the placenta, and in the ductusarteriosus of the fetus. • Therapeutically, alprostadil can be used to treat erectile dysfunction • to keep the ductusarteriosus open in neonates with congenital heart conditions until surgery is possible. PGE1 maintains the patency of the ductusarteriosusduring pregnancy.

  14. Lubiprostone • Lubiprostoneis a PGE1 derivative indicated for the treatment of chronic idiopathic constipation, opioid-induced constipation, and irritable bowel syndrome with constipation. • It stimulates chloride channels in the luminal cells of the intestinal epithelium, thereby increasing intestinal fluid secretion. • Nausea and diarrhea are the most common side effects of lubiprostone

  15. Misoprostol • Misoprostol, a PGE1 analog, is used to protect the mucosal lining of the stomach during chronic NSAID treatment. • Misoprostol interacts with prostaglandin receptors on parietal cells within the stomach, reducing gastric acid secretion. Furthermore, misoprostol has a GI cytoprotective effect by stimulating mucus and bicarbonate production. • Misoprostolis also used off-label in obstetric settings for labor induction, since it increases uterine contractions by interacting with prostaglandin receptors in the uterus. Misoprostol has the potential risk to induce abortion in pregnant women.

  16. Prostaglandin F2α analogs • Bimatoprost, latanoprost, tafluprost, and travoprostare PGF2α analogs • indicated for the treatment of open-angle glaucoma. By binding to prostaglandin receptors, they increase uveoscleraloutflow, reducing intraocular pressure. They are administered as ophthalmic solutions once a day and are as effective as timolol or better in reducing intraocular pressure. • Bimatoprostincreases eyelash distinction, length, and darkness and is approved for the treatment of eyelash hypotrichosis. Ocular reactions include blurred vision, iris color change, ocular irritation, and foreign body sensation.

  17. Prostacyclin (PGI2) analogs • Epoprostenol, the pharmaceutical form of naturally occurring prostacyclin, and the synthetic analogs of prostacyclin iloprost and treprostinilare potent pulmonary vasodilators that are used for the treatment of pulmonary arterial hypertension. • Dizziness, headache, flushing, and fainting are the most common adverse effects. • Bronchospasm and cough can also occur after inhalation of iloprost.

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