HuBio 543 September 27, 2007 Neil M. Nathanson K-536A, HSB 3-9457 nathanso@u.washington.edu Adrenergic Antagonists
Alpha- Adrenergic Antagonists I. Non-selective alpha adrenergic receptor antagonists A. Covalent (haloalkylamines) Dibenamine Phenoxybenzamine* B. Noncovalent Phentolamine* Tolazoline II. a1-selective Doxazosin Prazosin* Terazosin III. a2-selective Yohimbine* (* = Drug List)
Covalent inactivation of a-receptor by phenoxybenzamine CH2 N O CH3 C�H CH2Cl Phenoxybenzamine CH2 N O CH3 C�H + CH2 CH2 N O CH2 C�H CH2 CH3 Ethylene iminium ion Alkylated a-receptor
Phenoxybenzamine Administration causes: Postural hypotension Reflex tachycardia Miosis Impaired ejaculation Can act on the CNS (nausea and sedation)
EPINEPHRINE REVERSAL AFTER PHENOXYBENZAMINE 220 BP (mm. Hg) 180 140 EPINEPHRINE PRETREAT WITH POB: 120 100 BP (mm. Hg) 80 60 EPINEPHRINE
Effect of phenoxybenzamine on responses to EPI and NE HR BP EPI NE EPI POB NE
Phenoxybenzamine Indications: Treatment of pheochromocytoma Prior to surgery to remove pheochromocytoma
Alpha- Adrenergic Antagonists I. Non-selective alpha adrenergic receptor antagonists A. Covalent (haloalkylamines) Dibenamine Phenoxybenzamine* B. Noncovalent Phentolamine* Tolazoline II. a1-selective Doxazosin Prazosin* Terazosin III. a2-selective Yohimbine* (* = Drug List)
Epinephrine reversal by phentolamine 15 µg/kg Blood Pressure + Epi 5 µg/kg + Epi 5 µg/kg
Contraction of arterial strips Comparison of Competitive vs. “Non-equilibrium” Blockade Pretreat with Phentolamine No Pretreatment Contraction of arterial strips (a1- receptor) Pretreat with Phenoxybenzamine Concentration of Norepinephrine
Alpha- Adrenergic Antagonists I. Non-selective alpha adrenergic receptor antagonists A. Covalent (haloalkylamines) Dibenamine Phenoxybenzamine* B. Noncovalent Phentolamine* Tolazoline II. a1-selective Doxazosin Prazosin* Terazosin III. a2-selective Yohimbine* (* = Drug List)
Prazosin causes epinephrine reversal Pretreat with prazosin Blood Pressure Epinephrine Epinephrine
X X Presynaptic Receptors Inhibit NE Release NE NE NE NE ß1- AdR a2-
X X XX Block Presynaptic Receptors: Increase NE Release NE NE Increased HR NE NE ß1- AdR NE NE NE XX a2- AdR NE POB Presynaptic Receptors Active: Less NE Release NE NE ß1- AdR Less Tachycardia X X NE NE a2- AdR NE
Months Long-lasting anti-hypertensive effect of prazosin therapy 150 130 Supine 110 Mean Blood ressureP (mm. Hg) Standing 90 70 50 6 12 18 24 Months
Yohimbine blocks a2 - receptors and thus increases NE release
Beta-Adrenergic Antagonists I. Non-selective ß-blockers Nadolol* Propranolol* Timolol* Pindolol Sotalol II. ß1-Selective Antagonists III. ß2-Selective Antagonists Atenolol* Esmolol* Metoprolol* Acebutolol Betaxolol Practolol Butoxamine* (* = Drug List)
Propranolol blocks responses to isoproterenol 0.5 mg/kg Propranolol 0.2 µg/kg ISO 0.2 µg/kg ISO 1 µg/kg ISO Cardiac Force Arterial Pressure Heart Rate 1 min.
EFFECT OF ANTAGONISTS ON RESPONSES TO ISO + phentolamine + propranolol BP + ISO + ISO + ISO
Effect of antagonists on pressor response to NE + Propranolol 2 mg/kg + Phentolamine 15 mg/kg 240 160 BP (mm. Hg) 80 NE, 2.5 µg/kg NE, 2.5 µg/kg NE, 2.5 µg/kg
Both a and ß receptors contribute to epinephrine action + phentolamine + propranolol Blood Pressure + Epi + Epi + Epi
Effect of antagonists on responses to adrenergic agonists PRO NE + PHEN Contraction of VSM ISO ISO + PHEN ISO + PROP Relaxation of airway SM NE Contraction of heart NE + PRO NE + PHEN CONCENTRATION OF AGONIST
Therapeutic Uses of Beta Blockers Endocrine �Hyperthyroidism Pheochromocytoma Other Glaucoma Certain types of tremor Cardiovascular Angina Pectoris Arrhythmias Hypertension Recurrence of heart attack CNS Prophylaxis of migraine Alleviation of anxiety
Why do ß blockers have anti-hypertensive action? Possible reasons: Block ß-receptors in heart decrease cardiac output Decrease renin secretion from kidney Resets baroreceptor sensitivity Acts in CNS to “decrease” sympathetic activity
Propranolol decreases mortality after heart attack 10 8 Placebo 6 Cumulative mortality Rate (%) 4 Propranolol 2 6 12 18 24 30 MONTHS
Therapeutic Uses of Beta Blockers Endocrine �Hyperthyroidism Pheochromocytoma Other Glaucoma Certain types of tremor Cardiovascular Angina Pectoris Arrhythmias Hypertension Recurrence of heart attack CNS Prophylaxis of migraine Alleviation of anxiety
ADVERSE EFFECTS OF ß-BLOCKERS MAJOR EFFECTS OTHER SIDE EFFECTS Heart Failure Fatigue Bronchospasm Constipation Heart Block Diarrhea Bradycardia Nightmares Hypotension Depression Hypoglycemia Paresthesias Claudication Skin Rash
Chronic propranolol increases density of ß-AdR in heart 60 40 Cardiac ß-AdR Number 20 Control Propranolol-treated
% Change in FEV1 From Control Effects of opthalmic administration of timolol Control Patients % Change in FEV1 From Control -20 Asthma Patients -40 1 2 3 Time (hours)
Beta-Adrenergic Antagonists I. Non-selective ß-blockers Nadolol* Propranolol* Timolol* Pindolol Sotalol II. ß1-Selective Antagonists III. ß2-Selective Antagonists Atenolol* Esmolol* Metoprolol* Acebutolol Betaxolol Practolol Butoxamine* (* = Drug List)
Comparison of propranolol vs. practolol Block of sympa- thetic nerve-stimulated HR increase PRO PRACT PRO Block of ISO-mediated vasodilation PRACT Block of ISO-mediated bronchodilation PRO PRACT .01 .1 1 10 Dose antagonist, mg/kg
Beta-Adrenergic Antagonists I. Non-selective ß-blockers Nadolol* Propranolol* Timolol* Pindolol Sotalol II. ß1-Selective Antagonists III. ß2-Selective Antagonists Atenolol* Esmolol* Metoprolol* Acebutolol Betaxolol Practolol Butoxamine* (* = Drug List)
Labetalol UGLY- 4 optical isomers, with different selectivities Non-selective ß-blocker PLUS a1-selective antagonist Used for treatment of: Hypertension Pheochromocytoma-associated hypertension Hypertension following abrupt withdrawl of clonidine Carvedilol is another non-selective ß PLUS a1 blocker