Posterior Pituitary Hormones

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Presentation transcript:

Posterior Pituitary Hormones Prof. Suheil Zmeili Faculty of Medicine Department of Pharmacology University of Jordan

Posterior Pituitary Hormones ADH (Vasopressin) & Oxytocin - Nonapeptides (9 a.a) - Known as neurohormones - Synthesized in the hypothalamus - Stored in the posterior pituitary → release ? Role as neurotransmitters (V1R’s in CNS) - Role of Oxytocin in man is unknown

ADH (Vasopressin) ADH ( Vasopressin) Physiological and pharmacological actions: - Vasoconstriction (V1 receptors) - ↑ reabsorption of H2O from collecting ducts (V2 receptors) - ↑ synthesis of certain clotting factors (VIII, Von Willebrand) (V2 receptors) - ↑ ACTH release (V3 receptors) - Oxytocin-like activity

ADH (Vasopressin) Factors/Drugs ↑ ADH release: - Hypovolemia, hyperosmolarity, pain, stress, nausea, fever, hypoxia - Angiotensin II - Certain prostaglandins - Nicotine, cholinergic agonists, β-adrenergics - Tricyclic antidepressants - Insulin, morphine, vincristine…

ADH (Vasopressin) Factors/Drugs ↓ ADH release: - Hypervolemia - Hypoosmlarity - Alcohol - Atrial natriuretic peptide - Phenytoin - Cortisol - Anticholinergics, α-adrenergics, GABA...

ADH (Vasopressin) Disorders affecting ADH release: A. Excess production (inappropriate ADH secretion) → Dilutional hyponatremia Causes: - Head trauma, encephalitis - Meningitis, oat cell carcinoma Rx: - Water restriction (Rx of choice) - Hypertonic saline solution - Fludrocortisone → ↑ Na+ blood level - ? ADH antagonists

ADH (Vasopressin) ADH antagonists - Conivaptan, V1 & V2 R antagonist given IV - Tolvaptan; Lixivaptan & Satavaptan, orally effective selective V2R antagonists Clinical uses: - Inappropriate ADH secretion - CHF

ADH (Vasopressin) B. Deficiency of ADH → Diabetes insipidus (DI)→ polyuria Causes: - Idiopathic DI - Congenital, Familial DI - Hypothalamic surgery, head trauma, malignancies - Gestational DI, overproduction or decreased clearance of vasopressinase Rx: ADH preparations (HRT)

ADH (Vasopressin) ADH preparations: - Natural human ADH (Pitressin) Given I.M, S.C, has short half-life (15 min) - Lypressin (synthetic, porcine source) Given intranasally, I.V, I.M, has short DOA (4hrs) - Desmopressin (synthetic ADH-like drug) Given intranasally, S.C Most widely used preparation, has long DOA (12 hrs)

ADH (Vasopressin) - Felypressin (synthetic ADH-like drug) Has strong vasoconstrictor activity Mainly used in dentistry Clinical uses to ADH: - DI - Nocturnal enuresis - Hemophilia - Bleeding esophageal varices

ADH (Vasopressin) Side effects to ADH preparations: - Allergy - Pallor - Headache, nausea, abdominal pain in ♀’s (oxytocin-like activity) - Anginal pain (coronary artery vasospasm) - H2O intoxication (massive doses) - Gangrene (rare particularly with desmopressin= has great affinity to V2 receptors)

Drugs acting on the uterus

Uterine Stimulants I. Uterine stimulants 1. Oxytocin: (nonapeptide= 9 a.a peptide) - Contracts the myoepithelial cells of the breast → milk letdown; milk ejection Major stimuli, baby cry and suckling - Contracts the uterus → delivery The uterus is insensitive to oxytocin in early pregnancy but its sensitivity increases with advanced pregnancy reaching maximum at time of delivery - Has slight ADH-like activity

Oxytocin Oxytocin MOA: - Surface receptors → stimulation of voltage-sensitive Ca++ channels → depolarization of uterine muscles → contractions - ↑ intracellular Ca++ - ↑ prostaglandin release

Oxytocin Clinical uses to oxytocin: - Induction of labor Drug of choice given in units in an I.V infusion - Postpartum hemorrhage, I.M. Ergot alkaloids are better (ergonovine, methylergonovine, syntometrine= oxytocin + ergometrine) - Breast engorgement, intranasally - Abortifacient, I.V infusion. ≥ 20 weeks of gestation, ineffective in early pregnancy

Oxytocin Side effects to oxytocin: - Rupture of the uterus Major and most serious side effect - H2O intoxication and hypertension Due to its ADH-like activity Specific oxytocin antagonist Atosiban (inhibitor to uterine contraction=tocolytic), effective in the management of premature delivery, given IV

Prostaglandins 2. Prostaglandins: * Dinoprostone (PGE2) Vaginal pessaries, inserts and gel, tab Abortifacient, induction of labor * Dinoprost (PGF2α) I.V infusion and intramniotic Same uses as dinoprostone

Prostaglandins & Ergot Alkaloids * Carboprost (PGF2α) I.M and intramniotic Abortifacient and postpartum hemorrhage * Gemeprost (PGE1) Vaginal pessaries Used to prime the cervix 3. Ergot alkaloids: Ergonovine, Methylergonovine I.M, oral

Ergot Alkaloids Ergot alkaloids remain the drugs of choice to manage postpartum hemorrhage As compared to oxytocin, ergot alkaloids are more potent, they produce more prolonged and sustained contractions of the uterus and they are less toxic Ergot alkaloids are contraindicated to be used as inducers to delivery (associated with high incidence of fetal distress and mortality)

Uterine Relaxants II. Uterine relaxants (Tocolytics) Major clinical use: premature delivery (weeks 20-36) → improve the survival of the newborn 1. β-adrenergic agonists: ↑ cAMP → ↓ cytoplasmic Ca++ * Ritodrine I.V infusion Most widely used * Terbutaline, Oral, S.C, I.V

Uterine Relaxants Side Effects to β-adrenergics: Sweating, tachycardia, chest pain… 2. Magnesium sulfate I.V infusion Activates adenylate cyclase and stimulates Ca++ dependent ATPase Uses: premature delivery and convulsions of pre- eclampsia

Uterine Relaxants 3. Progesterone Oral, I.M Dydrogesterone 4. Oxytocin competitive antagonists Atosiban

Uterine Relaxants 5. Prostaglandin synthesis inhibitors Indomethacin, Meloxicam 6. Nifedipine ** Major contraindication to tocolytics: fetal distress