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A-Textbook-of-Clinical-Pharmacology-and-Therapeutics-5th-edition

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OTHER ANTIHYPERTENSIVE DRUGS 193<br />

Key points<br />

Drugs used in essential hypertension<br />

• Diuretics: thiazides (in low dose) are preferred to loop<br />

diuretics unless there is renal impairment. They may<br />

precipitate gout <strong>and</strong> worsen glucose tolerance or<br />

dyslipidaemia, but they reduce the risk <strong>of</strong> stroke <strong>and</strong><br />

other vascular events. Adverse effects include<br />

hypokalaemia, which is seldom problematic, <strong>and</strong><br />

impotence. They are suitable first-line drugs, especially<br />

in black patients, who <strong>of</strong>ten have low circulating renin<br />

levels <strong>and</strong> respond well to salt restriction <strong>and</strong> diuretics.<br />

• Beta-blockers reduce the risk <strong>of</strong> vascular events, but are<br />

contraindicated in patients with obstructive pulmonary<br />

disease. Adverse events (dose-related) include fatigue<br />

<strong>and</strong> cold extremities. Heart failure, heart block or<br />

claudication can be exacerbated in predisposed<br />

patients. They are particularly useful in patients with<br />

another indication for them (e.g. angina, postmyocardial<br />

infarction). Patients <strong>of</strong> African descent tend<br />

to respond poorly to them as single agents.<br />

• ACE inhibitors are particularly useful as an addition to a<br />

thiazide in moderately severe disease. The main<br />

adverse effect on chronic use is cough; losartan, an<br />

angiotensin-II receptor antagonist, lacks this effect but<br />

is otherwise similar to ACE inhibitors.<br />

• Calcium-channel antagonists are useful, especially in<br />

moderately severe disease. Long-acting<br />

drugs/preparations are preferred. The main adverse<br />

effect in chronic use is ankle swelling.<br />

• α 1 -Blockers are useful additional agents in patients who<br />

are poorly controlled on one or two drugs. Long-acting<br />

drugs (e.g. doxazosin) are preferred. Effects on vascular<br />

event rates are unknown. Unlike other<br />

antihypertensives, they improve the lipid pr<strong>of</strong>ile.<br />

• α-Methyldopa is useful in patients with hypertension<br />

during pregnancy.<br />

• Other drugs that are useful in occasional patients with<br />

severe disease include minoxidil, hydralazine <strong>and</strong><br />

nitroprusside.<br />

(BHS) guidelines. The main adverse effects are hyperkalaemia<br />

(especially in patients with renal impairment) <strong>and</strong>, with<br />

spironolactone, oestrogen-like effects <strong>of</strong> gynaecomastia, breast<br />

tenderness <strong>and</strong> menstrual disturbance.<br />

OTHER VASODILATORS<br />

α-ADRENOCEPTOR ANTAGONISTS<br />

There are two main types <strong>of</strong> α-adrenoceptor, α 1 - <strong>and</strong> α 2 . α 1 -<br />

Adrenoceptor antagonists lower blood pressure.<br />

Use<br />

Phenoxybenzamine irreversibly alkylates α-receptors. It is<br />

uniquely valuable in preparing patients with phaeochromocytoma<br />

for surgery, but has no place in the management <strong>of</strong><br />

essential hypertension. Prazosin is a selective α 1 -blocker, but<br />

its use is limited by severe postural hypotension, especially<br />

following the first dose. It has a short elimination half-life.<br />

Doxazosin is closely related to prazosin, but is longer lasting,<br />

permitting once daily use <strong>and</strong> causing fewer problems with<br />

first-dose hypotension. It did not compare well with diuretic,<br />

Ca 2 antagonist or ACEI as first-line agent in ALLHAT, but is<br />

useful as add-on treatment in patients with resistant hypertension.<br />

It is given last thing at night.<br />

Doxazosin improves symptoms <strong>of</strong> bladder outflow tract<br />

obstruction (Chapter 36), <strong>and</strong> is useful in men with mild<br />

symptoms from benign prostatic hypertrophy.<br />

Mechanism <strong>of</strong> action<br />

Noradrenaline activates α 1 -receptors on vascular smooth<br />

muscle, causing tonic vasoconstriction. α 1 -Antagonists cause<br />

vasodilatation by blocking this tonic action <strong>of</strong> noradrenaline.<br />

OTHER ANTIHYPERTENSIVE DRUGS<br />

Other important drugs (aldosterone antagonists, other<br />

vasodilators <strong>and</strong> centrally acting drugs) are summarized in<br />

Table 28.3.<br />

ALDOSTERONE ANTAGONISTS<br />

Neither spironolactone nor the more selective (<strong>and</strong> much more<br />

expensive) eplerenone is licensed for treating essential hypertension.<br />

They are used to treat Conn’s syndrome, but are also<br />

effective in essential hypertension (especially low renin essential<br />

hypertension) <strong>and</strong> are recommended as add-on treatment<br />

for resistant hypertension by the British Hypertension Society<br />

Adverse effects<br />

• First-dose hypotension <strong>and</strong> postural hypotension are<br />

adverse effects.<br />

• Nasal stuffiness, headache, dry mouth <strong>and</strong> pruritus have<br />

been reported, but are relatively infrequent.<br />

• α-Blockers can cause urinary incontinence, especially in<br />

women with pre-existing pelvic pathology.<br />

Metabolic effects<br />

α 1 -Adrenoceptor antagonists have a mild favourable effect on<br />

plasma lipids, with an increase in HDL <strong>and</strong> a reduction in<br />

LDL cholesterol.<br />

Pharmacokinetics<br />

Doxazosin has an elimination half-life <strong>of</strong> approximately 10–12<br />

hours <strong>and</strong> provides acceptably smooth 24-hour control if used<br />

once daily.

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