SYMPATHOTROPIC DRUGS SYMPATHOLYTICS Indications: •hypertension (mild and moderate) •antimigraine drugs •disorders of peripheral vascularity •benign prostatic hyperplasia •urinary obstruction – postoperative atonia •pheochromocytoma Sympatholycs (direct and indirect) Direct sympatholytics α α-lytics – reversible – irreversible α1 lytics α2-lytics non-selective α-lytics drugs with combined effect •ergot alkaloids (ergotamine, ergometrine, ergotoxine, methylergometrine, dihydroergotamine, dihydroergotoxine, dihydroergocristine) Direct sympatholytics α non-selective •in Secale cornutum, product of Claviceps purpurea, fungus that infects cereal crops •derivatives of lysergic acid •effects: - CNS (halucinations, ↓ prolactine secretion) - smooth muscle of blood vessel (effects mimetic or lytic) - uterine muscle → contractions Ergot alkaloids and their derivatives ➙ reversible α-lytics Direct sympatholytics α non-selective INDICATIONS AND USE (today rare use, in gynekology, sometimes in individually prepared prescription): •uterotonics •antimigraine drugs •(vasodilators) •(hypertension) Direct sympatholytics α non-selective Ergot alkaloids •ergotamine, ergometrine - parcial α-agonistic effects - uterotonic effect, amplified by methylation of derivatives (methylergometrine) •ergotoxine - mixture of alkaloids, mainly ergocristine, ergocriptine and ergocornine - especially α-lytic effects • α-lytic effects are increased in dihydro-derivatives (dihydroergotamine, dihydroergotoxine, dihydroergocristine) ! Direct sympatholytics α non-selective Ergot alkaloids • methylergometrine uterotonic effect (amplified by methylation of derivatives derivátů) • therapy and prevention of uterine bleeding after childbirth (in hypotony and atony of myometrium) • therapy and prevention of uterine bleeding after evacuation or revision of the uterus after a miscarriage • subinvolution of uterus in the postpartum period • gynecological operations – for the ↑ uterine tone • III. time of birth after birth limbs Direct sympatholytics α non-selective Ergot alkaloids INDICATIONS AND USE • pheochromocytoma • mild and moderate hypertension • peripheral vasospastic diseases: (Raynaud phenomena) • urinary obstruction • • today almost not used Direct sympatholytics α non-selective Synthetic drugs •phentolamine (in Czech Rep. non registered) •blocks α1 and α2 receptors – decrease of peripheral vascular resistance •cardiostimulatory effect (↑ HR,tachy or arrhytmia)➙ resulted from α2-adrenergic blockade → non-regulated noradrenaline releasing • GIT stimulation ➙ HCl hypersecretion and diarrhea • parenteral administration • obsol. • •phenoxybenzamine (in Cz. Rep. non registered) • irreversible α-receptor antagonist • covalent binding to the receptor – need of receptor synthesis de novo Use: - pheochromocytoma therapy • • Direct sympatholytics α non-selective α1sympatholytics Overview of drugs, use •terazosin, doxazosin, alfuzosin, tamsulosin… •prazosin (in Czech Rep. non registered) •Use: - hypertension (relaxation of arterial and venous smooth muscle) - benign prostatic hyperplasia - urinary obstruction Direct sympatholytics α1 selective •urapidil • •combined central and peripheral action, blocks α1 receptors, in CNS blocks H1 receptors, activates 5-HT1A receptors •Use: - hypertension (hypertension crisis, severe, respectively, very severe forms of hypertension and hypertension resistant to standard therapy) Direct sympatholytics with combined effect α2 sympatholytics •yohimbine (in Czech Rep. non registered) •vasodilation in the pelvic area, afrodisiac effect •it is contained in some dietary supplements Direct sympatholytics α2 selective •competitive antagonists (intrinsic aktivity = 0) or partial agonists (ISA - intrinsic sympathomimetic activity) = dualists •nonselective or cardioselective (selectively block í β1 receptors) •sufficient solubility in fats → penetration across HEB Direct sympatholytics β-blockers, β-sympatholytics Organ effects cardiovascular system: negatively chronotropic and inotropic effect → ↓ BP and HR - inhibition of vasodilation by β2-receptor blockade → peripheral vascular resistence increase - renine secretion reduction bronchi: bronchoconstriction eye: intraocular pressure decrease metabolic effects: glycogenolysis reduction, lipolysis inhibition Direct sympatholytics β-blockers, β-sympatholytics NONSELECTIVE (1 + 2) propranolol, metipranolol (CARDIO)SELECTIVE (1) atenolol, metoprolol NONSELECTIVE (1 + 2) WITH ISA pindolol, bopindolol (in Czech Rep. non registered) (CARDIO)SELECTIVE (1) WITH ISA acebutolol WITH COMBINED EFFECTS  +  labetalol carvedilol Direct sympatholytics β-blockers, β-sympatholytics Use, indications: •hypertension •Ischemic heart disease, non-stabil angina pectoris, status after acute myocardial infarction •arrhytmia •glaucoma •hyperthyreosis •anxiety (moderate effect) Direct sympatholytics β-blockers, β-sympatholytics Side effects: •asthma bronchiale, dyspnoea •heart insufficiency •bradycardia, blockade of heart impuls conduction •masking of hypoglycemia symptoms •disorders of peripheral blood circulation •sleep disorders, depression (lipophilic drugs) •rash, fever and other allergic symptoms (rarely) •abrupt discontinuation of therapy – „rebound phenomena“ Direct sympatholytics β-blockers, β-sympatholytics decreases catecholamine concentratio in the synaptic cleft by: • inhibition of NT synthesis • inhibition of NT storage • inhibicí of NT release • false precursors Nondirect sympatholytics •blockators of nerve endings ➙ block catecholamine uptake to the nerve endings and cause stabilization of the membranes (representatives: guanethidine, bretylium, debrisoquine) •false precursors (α-methyldopa – see above – ranked among SM but the resulting effect is sympatholytic!) •drugs causing catecholamine depletion (reserpine) •drugs inhibiting NT synthesis (methyltyrosine = metyrosine) •today rare medical use Nondirect sympatholytics