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Basic Pharmacology of Antihypertensive Agents
All antihypertensive agents act
at one or more of the four anatomic control sites depicted in Figure 11–1
and produce their effects by interfering with normal mechanisms of blood
pressure regulation. A useful classification of these agents categorizes
them according to the principal regulatory site or mechanism on which
they act (Figure 11–3). Because of their common mechanisms of action,
drugs within each category tend to produce a similar spectrum of toxicities.
The categories include the following:
1.
Diuretics, which lower blood pressure by depleting the body
of sodium and reducing blood volume and perhaps by other mechanisms.
2.
Sympathoplegic
agents, which lower blood pressure
by reducing peripheral vascular resistance, inhibiting cardiac function,
and increasing venous pooling in capacitance vessels. (The latter two
effects reduce cardiac output.) These agents are further subdivided
according to their putative sites of action in the sympathetic reflex arc
(see below).
3.
Direct
vasodilators, which reduce
pressure by relaxing vascular smooth muscle, thus dilating resistance
vessels and—to varying degrees—increasing capacitance as well.
4.
Agents
that block production or action of angiotensin and thereby reduce peripheral vascular resistance
and (potentially) blood volume.
The fact that these drug groups
act by different mechanisms permits the combination of drugs from two or
more groups with increased efficacy and, in some cases, decreased
toxicity. (See Resistant Hypertension & Polypharmacy.)
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Resistant Hypertension & Polypharmacy
Monotherapy of hypertension
(treatment with a single drug) is desirable because compliance is
likely to be better and cost is lower, and because in some cases
adverse effects are fewer. However, most patients with hypertension
require two or more drugs, preferably acting by different mechanisms
(polypharmacy). According to some estimates, up to 40% of patients may
respond inadequately even to two agents and are considered to have
"resistant hypertension." Some of these patients have
treatable secondary hypertension that has been missed but most do not
and three or more drugs are required.
One rationale for polypharmacy
in hypertension is that most drugs evoke compensatory regulatory
mechanisms for maintaining blood pressure (see Figures 6–7 and 11–1),
which may markedly limit their effect. For example, vasodilators such
as hydralazine cause a significant decrease in peripheral vascular
resistance, but evoke a strong compensatory tachycardia and salt and
water retention (Figure 11–4) that is capable of almost completely
reversing their effect. The addition of a  blocker prevents the tachycardia;
addition of a diuretic (eg, hydrochlorothiazide) prevents the salt and
water retention. In effect, all three drugs increase the sensitivity of
the cardiovascular system to each other's actions.
A second reason is that some
drugs have only modest maximum efficacy but reduction of long-term
morbidity mandates their use. Many studies of angiotensin-converting
enzyme (ACE) inhibitors report a maximal lowering of blood pressure of
less than 10 mm Hg. In patients with stage 2 hypertension (pressure
> 160/100 mm Hg), this is inadequate to prevent all the sequelae of
hypertension, but ACE inhibitors have important long-term benefits in
preventing or reducing renal disease in diabetic persons, and reduction
of heart failure.
Finally, the toxicity of some
effective drugs prevents their use at maximally effective dosage. The
widespread indiscriminate use of blockers has been criticized because
several large clinical trials indicate that some members of the group,
eg, metoprolol and carvedilol, have a greater benefit than others, eg,
atenolol. However, all blockers appear to have similar
benefits in reducing mortality after myocardial infarction, so these
drugs are particularly indicated in patients with an infarct and
hypertension.
In practice, when hypertension
does not respond adequately to a regimen of one drug, a second drug
from a different class with a different mechanism of action and
different pattern of toxicity is added. If the response is still
inadequate and compliance is known to be good, a third drug should be
added. If three drugs (usually including a diuretic) are inadequate,
dietary sodium restriction and an additional drug may be necessary.
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Drugs that Alter Sodium &
Water Balance
Dietary sodium restriction has
been known for many years to decrease blood pressure in hypertensive patients.
With the advent of diuretics, sodium restriction was thought to be less
important. However, there is now general agreement that dietary control
of blood pressure is a relatively nontoxic therapeutic measure and may
even be preventive. Even modest dietary sodium restriction lowers blood
pressure (though to varying extents) in many hypertensive persons.
Mechanisms of Action &
Hemodynamic Effects of Diuretics
Diuretics lower blood pressure
primarily by depleting body sodium stores. Initially, diuretics reduce
blood pressure by reducing blood volume and cardiac output; peripheral
vascular resistance may increase. After 6–8 weeks, cardiac output returns
toward normal while peripheral vascular resistance declines. Sodium is
believed to contribute to vascular resistance by increasing vessel
stiffness and neural reactivity, possibly related to altered
sodium-calcium exchange with a resultant increase in intracellular
calcium. These effects are reversed by diuretics or sodium restriction.
Diuretics are effective in
lowering blood pressure by 10–15 mm Hg in most patients, and diuretics
alone often provide adequate treatment for mild or moderate essential
hypertension. In more severe hypertension, diuretics are used in
combination with sympathoplegic and vasodilator drugs to control the
tendency toward sodium retention caused by these agents. Vascular
responsiveness—ie, the ability to either constrict or dilate—is
diminished by sympathoplegic and vasodilator drugs, so that the
vasculature behaves like an inflexible tube. As a consequence, blood
pressure becomes exquisitely sensitive to blood volume. Thus, in severe
hypertension, when multiple drugs are used, blood pressure may be well
controlled when blood volume is 95% of normal but much too high when
blood volume is 105% of normal.
Use of Diuretics
The sites of action within the
kidney and the pharmacokinetics of various diuretic drugs are discussed
in Chapter 15. Thiazide diuretics are appropriate for most patients with
mild or moderate hypertension and normal renal and cardiac function. More
powerful diuretics (eg, those acting on the loop of Henle) such as
furosemide are necessary in severe hypertension, when multiple drugs with
sodium-retaining properties are used; in renal insufficiency, when
glomerular filtration rate is less than 30 or 40 mL/min; and in cardiac
failure or cirrhosis, in which sodium retention is marked.
Potassium-sparing diuretics are
useful both to avoid excessive potassium depletion and to enhance the
natriuretic effects of other diuretics. Aldosterone receptor antagonists
in particular also have a favorable effect on cardiac function in people
with heart failure.
Some pharmacokinetic
characteristics and the initial and usual maintenance dosages of
hydrochlorothiazide are listed in Table 11–2. Although thiazide diuretics
are more natriuretic at higher doses (up to 100–200 mg of
hydrochlorothiazide), when used as a single agent, lower doses (25–50 mg)
exert as much antihypertensive effect as do higher doses. In contrast to
thiazides, the blood pressure response to loop diuretics continues to
increase at doses many times greater than the usual therapeutic dose.
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Table 11–2 Pharmacokinetic
Characteristics and Dosage of Selected Oral Antihypertensive Drugs.
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Drug
|
Half-life
(h)
|
Bioavailability
(percent)
|
Suggested
Initial Dose
|
Usual
Maintenance Dose Range
|
Reduction of
Dosage Required in Moderate Renal Insufficiency1
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Amlodipine
|
35
|
65
|
2.5 mg/d
|
5–10 mg/d
|
No
|
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Atenolol
|
6
|
60
|
50 mg/d
|
50–100 mg/d
|
Yes
|
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Benazepril
|
0.62
|
35
|
5–10 mg/d
|
20–40 mg/d
|
Yes
|
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Captopril
|
2.2
|
65
|
50–75 mg/d
|
75–150 mg/d
|
Yes
|
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Clonidine
|
8–12
|
95
|
0.2 mg/d
|
0.2–1.2
mg/d
|
Yes
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Diltiazem
|
3.5
|
40
|
120–140
mg/d
|
240–360
mg/d
|
No
|
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Guanethidine
|
120
|
3–50
|
10 mg/d
|
25–50 mg/d
|
Possible
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Hydralazine
|
1.5–3
|
25
|
40 mg/d
|
40–200 mg/d
|
No
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Hydrochlorothiazide
|
12
|
70
|
25 mg/d
|
25–50 mg/d
|
No
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Lisinopril
|
12
|
25
|
10 mg/d
|
10–80 mg/d
|
Yes
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Losartan
|
1–23
|
36
|
50 mg/d
|
25–100 mg/d
|
No
|
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Methyldopa
|
2
|
25
|
1 g/d
|
1–2 g/d
|
No
|
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Metoprolol
|
3–7
|
40
|
50–100 mg/d
|
200–400
mg/d
|
No
|
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Minoxidil
|
4
|
90
|
5–10 mg/d
|
40 mg/d
|
No
|
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Nebivolol
|
12
|
Nd4
|
5 mg/d
|
10–40 mg/d
|
No
|
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Nifedipine
|
2
|
50
|
30 mg/d
|
30–60 mg/d
|
No
|
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Prazosin
|
3–4
|
70
|
3 mg/d
|
10–30 mg/d
|
No
|
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Propranolol
|
3–5
|
25
|
80 mg/d
|
80–480 mg/d
|
No
|
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Reserpine
|
24–48
|
50
|
0.25 mg/d
|
0.25 mg/d
|
No
|
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Verapamil
|
4–6
|
22
|
180 mg/d
|
240–480
mg/d
|
No
|
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1Creatinine clearance ≥ 30 mL/min. Many of these
drugs do require dosage adjustment if creatinine clearance falls below
30 mL/min.
2The active metabolite of benazepril has a
half-life of 10 hours.
3The active metabolite of losartan has a half-life
of 3–4 hours.
4Nd, not determined.
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Toxicity of Diuretics
In the treatment of
hypertension, the most common adverse effect of diuretics (except for
potassium-sparing diuretics) is potassium depletion. Although mild
degrees of hypokalemia are tolerated well by many patients, hypokalemia
may be hazardous in persons taking digitalis, those who have chronic
arrhythmias, or those with acute myocardial infarction or left
ventricular dysfunction. Potassium loss is coupled to reabsorption of
sodium, and restriction of dietary sodium intake therefore minimizes
potassium loss. Diuretics may also cause magnesium depletion, impair
glucose tolerance, and increase serum lipid concentrations. Diuretics
increase uric acid concentrations and may precipitate gout. The use of
low doses minimizes these adverse metabolic effects without impairing the
antihypertensive action. Potassium-sparing diuretics may produce
hyperkalemia, particularly in patients with renal insufficiency and those
taking ACE inhibitors or angiotensin receptor blockers; spironolactone (a
steroid) is associated with gynecomastia.
Drugs that Alter Sympathetic
Nervous System Function
In patients with moderate to
severe hypertension, most effective drug regimens include an agent that
inhibits function of the sympathetic nervous system. Drugs in this group
are classified according to the site at which they impair the sympathetic
reflex arc (Figure 11–2). This neuroanatomic classification explains
prominent differences in cardiovascular effects of drugs and allows the
clinician to predict interactions of these drugs with one another and
with other drugs.
The subclasses of sympathoplegic
drugs exhibit different patterns of potential toxicity. Drugs that lower
blood pressure by actions on the central nervous system tend to cause
sedation and mental depression and may produce disturbances of sleep,
including nightmares. Drugs that act by inhibiting transmission through
autonomic ganglia (ganglion blockers) produce toxicity from inhibition of
parasympathetic regulation, in addition to profound sympathetic blockade
and are no longer used. Drugs that act chiefly by reducing release of
norepinephrine from sympathetic nerve endings cause effects that are
similar to those of surgical sympathectomy, including inhibition of
ejaculation, and hypotension that is increased by upright posture and
after exercise. Drugs that block postsynaptic adrenoceptors produce a
more selective spectrum of effects depending on the class of receptor to which
they bind.
Finally, one should note that all
of the agents that lower blood pressure by altering sympathetic function
can elicit compensatory effects through mechanisms that are not dependent
on adrenergic nerves. Thus, the antihypertensive effect of any of these
agents used alone may be limited by retention of sodium by the kidney and
expansion of blood volume. For this reason, sympathoplegic
antihypertensive drugs are most effective when used concomitantly with a
diuretic.
Centrally Acting Sympathoplegic
Drugs
Centrally acting sympathoplegic
drugs were once widely used in the treatment of hypertension. With the
exception of clonidine, these drugs are rarely used today.
Mechanisms & Sites of
Action
These agents reduce sympathetic
outflow from vasomotor centers in the brain stem but allow these centers
to retain or even increase their sensitivity to baroreceptor control.
Accordingly, the antihypertensive and toxic actions of these drugs are
generally less dependent on posture than are the effects of drugs that
act directly on peripheral sympathetic neurons.
Methyldopa (L - -methyl-3,4-dihydroxyphenylalanine) is
an analog of L -dopa and is
converted to -methyldopamine and -methylnorepinephrine; this pathway
directly parallels the synthesis of norepinephrine from dopa illustrated
in Figure 6–5. Alpha-methylnorepinephrine is stored in adrenergic nerve
vesicles, where it stoichiometrically replaces norepinephrine, and is
released by nerve stimulation to interact with postsynaptic
adrenoceptors. However, this replacement of norepinephrine by a false
transmitter in peripheral neurons is not responsible for
methyldopa's antihypertensive effect, because the -methylnorepinephrine released is an
effective agonist at the adrenoceptors that mediate peripheral
sympathetic constriction of arterioles and venules. In fact, methyldopa's
antihypertensive action appears to be due to stimulation of central
adrenoceptors by -methylnorepinephrine or -methyldopamine.
The antihypertensive action of clonidine,
a 2-imidazoline derivative, was discovered in the course of testing the
drug for use as a nasal decongestant.
After intravenous injection,
clonidine produces a brief rise in blood pressure followed by more
prolonged hypotension. The pressor response is due to direct stimulation
of adrenoceptors in arterioles. The drug
is classified as a partial agonist at receptors because it also inhibits
pressor effects of other agonists.
Considerable evidence indicates
that the hypotensive effect of clonidine is exerted at adrenoceptors in the medulla of the
brain. In animals, the hypotensive effect of clonidine is prevented by
central administration of antagonists. Clonidine reduces
sympathetic and increases parasympathetic tone, resulting in blood
pressure lowering and bradycardia. The reduction in pressure is
accompanied by a decrease in circulating catecholamine levels. These
observations suggest that clonidine sensitizes brain stem vasomotor
centers to inhibition by baroreflexes.
Thus, studies of clonidine and
methyldopa suggest that normal regulation of blood pressure involves
central adrenergic neurons that modulate baroreceptor reflexes. Clonidine
and -methylnorepinephrine bind more tightly
to 2 than to 1 adrenoceptors. As noted in
Chapter 6, 2 receptors are located on
presynaptic adrenergic neurons as well as some postsynaptic sites. It is
possible that clonidine and -methylnorepinephrine act in the brain
to reduce norepinephrine release onto relevant receptor sites.
Alternatively, these drugs may act on postsynaptic 2 adrenoceptors to inhibit
activity of appropriate neurons. Finally, clonidine also binds to a
nonadrenoceptor site, the imidazoline receptor, which may also
mediate antihypertensive effects.
Methyldopa and clonidine produce
slightly different hemodynamic effects: clonidine lowers heart rate and
cardiac output more than does methyldopa. This difference suggests that
these two drugs do not have identical sites of action. They may act
primarily on different populations of neurons in the vasomotor centers of
the brain stem.
Guanabenz and guanfacine
are centrally active antihypertensive drugs that share the central -adrenoceptor-stimulating effects of
clonidine. They do not appear to offer any advantages over clonidine and
are rarely used.
Methyldopa
Methyldopa was widely used in
the past but is now used primarily for hypertension during pregnancy. It
lowers blood pressure chiefly by reducing peripheral vascular resistance,
with a variable reduction in heart rate and cardiac output.
Most cardiovascular reflexes
remain intact after administration of methyldopa, and blood pressure
reduction is not markedly dependent on posture. Postural (orthostatic)
hypotension sometimes occurs, particularly in volume-depleted patients.
One potential advantage of methyldopa is that it causes reduction in
renal vascular resistance.
Pharmacokinetics & Dosage
Pharmacokinetic characteristics
of methyldopa are listed in Table 11–2. Methyldopa enters the brain via
an aromatic amino acid transporter. The usual oral dose of methyldopa
produces its maximal antihypertensive effect in 4–6 hours, and the effect
can persist for up to 24 hours. Because the effect depends on
accumulation and storage of a metabolite (-methylnorepinephrine) in the vesicles
of nerve endings, the action persists after the parent drug has
disappeared from the circulation.
Toxicity
The most common undesirable
effect of methyldopa is sedation, particularly at the onset of treatment.
With long-term therapy, patients may complain of persistent mental
lassitude and impaired mental concentration. Nightmares, mental
depression, vertigo, and extrapyramidal signs may occur but are
relatively infrequent. Lactation, associated with increased prolactin
secretion, can occur both in men and in women treated with methyldopa.
This toxicity is probably mediated by inhibition of dopaminergic
mechanisms in the hypothalamus.
Other important adverse effects
of methyldopa are development of a positive Coombs test (occurring in
10–20% of patients undergoing therapy for longer than 12 months), which
sometimes makes cross-matching blood for transfusion difficult and rarely
is associated with hemolytic anemia, as well as hepatitis and drug fever.
Discontinuation of the drug usually results in prompt reversal of these
abnormalities.
Clonidine
Blood pressure lowering by
clonidine results from reduction of cardiac output due to decreased heart
rate and relaxation of capacitance vessels, with a reduction in
peripheral vascular resistance.
Reduction in arterial blood
pressure by clonidine is accompanied by decreased renal vascular
resistance and maintenance of renal blood flow. As with methyldopa,
clonidine reduces blood pressure in the supine position and only rarely
causes postural hypotension. Pressor effects of clonidine are not
observed after ingestion of therapeutic doses of clonidine, but severe
hypertension can complicate a massive overdose.
Pharmacokinetics & Dosage
Typical pharmacokinetic
characteristics are listed in Table 11–2.
Clonidine is lipid-soluble and
rapidly enters the brain from the circulation. Because of its relatively
short half-life and the fact that its antihypertensive effect is directly
related to blood concentration, oral clonidine must be given twice a day
(or as a patch, below) to maintain smooth blood pressure control.
However, as is not the case with methyldopa, the dose-response curve of
clonidine is such that increasing doses are more effective (but also more
toxic).
A transdermal preparation of
clonidine that reduces blood pressure for 7 days after a single
application is also available. This preparation appears to produce less
sedation than clonidine tablets but is often associated with local skin
reactions.
Toxicity
Dry mouth and sedation are
common. Both effects are centrally mediated and dose-dependent and
coincide temporally with the drug's antihypertensive effect.
Clonidine should not be given to
patients who are at risk for mental depression and should be withdrawn if
depression occurs during therapy. Concomitant treatment with tricyclic
antidepressants may block the antihypertensive effect of clonidine. The
interaction is believed to be due to -adrenoceptor-blocking actions of the
tricyclics.
Withdrawal of clonidine after
protracted use, particularly with high dosages (more than 1 mg/d), can
result in life-threatening hypertensive crisis mediated by increased
sympathetic nervous activity. Patients exhibit nervousness, tachycardia,
headache, and sweating after omitting one or two doses of the drug.
Because of the risk of severe hypertensive crisis when clonidine is
suddenly withdrawn, all patients who take clonidine should be warned of
the possibility. If the drug must be stopped, it should be done gradually
while other antihypertensive agents are being substituted. Treatment of
the hypertensive crisis consists of reinstitution of clonidine therapy or
administration of and -adrenoceptor–blocking agents.
Ganglion-Blocking Agents
Historically, drugs that block
activation of postganglionic autonomic neurons by acetylcholine were
among the first agents used in the treatment of hypertension. Most such
drugs are no longer available clinically because of intolerable
toxicities related to their primary action (see below).
Ganglion blockers competitively
block nicotinic cholinoceptors on postganglionic neurons in both
sympathetic and parasympathetic ganglia. In addition, these drugs may
directly block the nicotinic acetylcholine channel, in the same fashion
as neuromuscular nicotinic blockers (see Figure 27–6).
The adverse effects of ganglion
blockers are direct extensions of their pharmacologic effects. These
effects include both sympathoplegia (excessive orthostatic hypotension
and sexual dysfunction) and parasympathoplegia (constipation, urinary
retention, precipitation of glaucoma, blurred vision, dry mouth, etc).
These severe toxicities are the major reason for the abandonment of
ganglion blockers for the therapy of hypertension.
Adrenergic Neuron–Blocking
Agents
These drugs lower blood pressure
by preventing normal physiologic release of norepinephrine from
postganglionic sympathetic neurons.
Guanethidine
In high enough doses,
guanethidine can produce profound sympathoplegia. The resulting high
maximal efficacy of this agent made it the mainstay of outpatient therapy
of severe hypertension for many years. For the same reason, guanethidine
can produce all of the toxicities expected from "pharmacologic sympathectomy,"
including marked postural hypotension, diarrhea, and impaired
ejaculation. Because of these adverse effects, guanethidine is now rarely
used.
Guanethidine is too polar to
enter the central nervous system. As a result, this drug has none of the
central effects seen with many of the other antihypertensive agents
described in this chapter.
Guanadrel is a
guanethidine-like drug that is available in the USA. Bethanidine
and debrisoquin, antihypertensive agents not available for
clinical use in the USA, are similar.
Mechanism & Sites of Action
Guanethidine inhibits the
release of norepinephrine from sympathetic nerve endings (see Figure
6–4). This effect is probably responsible for most of the sympathoplegia
that occurs in patients. Guanethidine is transported across the
sympathetic nerve membrane by the same mechanism that transports
norepinephrine itself (NET, uptake 1), and uptake is essential for the
drug's action. Once guanethidine has entered the nerve, it is
concentrated in transmitter vesicles, where it replaces norepinephrine.
Because it replaces norepinephrine, the drug causes a gradual depletion
of norepinephrine stores in the nerve ending.
Because neuronal uptake is
necessary for the hypotensive activity of guanethidine, drugs that block
the catecholamine uptake process or displace amines from the nerve
terminal (see Chapter 6) block its effects. These include cocaine,
amphetamine, tricyclic antidepressants, phenothiazines, and
phenoxybenzamine.
Pharmacokinetics & Dosage
Because of guanethidine's long
half-life (5 days), the onset of sympathoplegia is gradual (maximal
effect in 1–2 weeks), and sympathoplegia persists for a comparable period
after cessation of therapy. The dose should not ordinarily be increased
at intervals shorter than 2 weeks.
Toxicity
Therapeutic use of guanethidine
is often associated with symptomatic postural hypotension and hypotension
following exercise, particularly when the drug is given in high doses.
Guanethidine-induced sympathoplegia in men may be associated with delayed
or retrograde ejaculation (into the bladder). Guanethidine commonly
causes diarrhea, which results from increased gastrointestinal motility
due to parasympathetic predominance in controlling the activity of
intestinal smooth muscle.
Interactions with other drugs
may complicate guanethidine therapy. Sympathomimetic agents, at doses
available in over-the-counter cold preparations, can produce hypertension
in patients taking guanethidine. Similarly, guanethidine can produce
hypertensive crisis by releasing catecholamines in patients with
pheochromocytoma. When tricyclic antidepressants are administered to
patients taking guanethidine, the drug's antihypertensive effect is
attenuated, and severe hypertension may follow.
Reserpine
Reserpine, an alkaloid extracted
from the roots of an Indian plant, Rauwolfia serpentina, was one
of the first effective drugs used on a large scale in the treatment of
hypertension. At present, it is rarely used owing to its adverse effects.
Mechanism & Sites of Action
Reserpine blocks the ability of
aminergic transmitter vesicles to take up and store biogenic amines,
probably by interfering with the vesicular membrane-associated
transporter (VMAT, see Figure 6–4). This effect occurs throughout the
body, resulting in depletion of norepinephrine, dopamine, and serotonin
in both central and peripheral neurons. Chromaffin granules of the
adrenal medulla are also depleted of catecholamines, although to a lesser
extent than are the vesicles of neurons. Reserpine's effects on
adrenergic vesicles appear irreversible; trace amounts of the drug remain
bound to vesicular membranes for many days.
Depletion of peripheral amines
probably accounts for much of the beneficial antihypertensive effect of
reserpine, but a central component cannot be ruled out. Reserpine readily
enters the brain, and depletion of cerebral amine stores causes sedation,
mental depression, and parkinsonism symptoms.
At lower doses used for
treatment of mild hypertension, reserpine lowers blood pressure by a
combination of decreased cardiac output and decreased peripheral vascular
resistance.
Pharmacokinetics & Dosage
See Table 11–2.
Toxicity
At the low doses usually
administered, reserpine produces little postural hypotension. Most of the
unwanted effects of reserpine result from actions on the brain or
gastrointestinal tract.
High doses of reserpine
characteristically produce sedation, lassitude, nightmares, and severe
mental depression; occasionally, these occur even in patients receiving
low doses (0.25 mg/d). Much less frequently, ordinary low doses of
reserpine produce extrapyramidal effects resembling Parkinson's disease,
probably as a result of dopamine depletion in the corpus striatum.
Although these central effects are uncommon, it should be stressed that
they may occur at any time, even after months of uneventful treatment.
Patients with a history of mental depression should not receive
reserpine, and the drug should be stopped if depression appears.
Reserpine rather often produces mild
diarrhea and gastrointestinal cramps and increases gastric acid
secretion. The drug should not be given to patients with a history of
peptic ulcer.
Adrenoceptor Antagonists
The detailed pharmacology of - and -adrenoceptor blockers is presented in
Chapter 10.
Beta-Adrenoceptor–Blocking
Agents
Of the large number of blockers tested, most have been shown
to be effective in lowering blood pressure. The pharmacologic properties
of several of these agents differ in ways that may confer therapeutic
benefits in certain clinical situations.
Propranolol
Propranolol was the first blocker shown to be effective in
hypertension and ischemic heart disease. Propranolol has now been largely
replaced by cardioselective blockers such as metoprolol and
atenolol. All -adrenoceptor–blocking agents are
useful for lowering blood pressure in mild to moderate hypertension. In
severe hypertension, blockers are especially useful in
preventing the reflex tachycardia that often results from treatment with
direct vasodilators. Beta blockers have been shown to reduce mortality
after a myocardial infarction and some also reduce mortality in patients
with heart failure; they are particularly advantageous for treating
hypertension in patients with these conditions (see Chapter 13).
Mechanism & Sites of Action
Propranolol's efficacy in
treating hypertension as well as most of its toxic effects result from
nonselective blockade. Propranolol decreases blood
pressure primarily as a result of a decrease in cardiac output. Other blockers may decrease cardiac output or
decrease peripheral vascular resistance to various degrees, depending on cardioselectivity
and partial agonist activities.
Propranolol inhibits the
stimulation of renin production by catecholamines (mediated by 1 receptors). It is likely
that propranolol's effect is due in part to depression of the
renin-angiotensin-aldosterone system. Although most effective in patients
with high plasma renin activity, propranolol also reduces blood pressure
in hypertensive patients with normal or even low renin activity. Beta
blockers might also act on peripheral presynaptic adrenoceptors to reduce sympathetic
vasoconstrictor nerve activity.
In mild to moderate
hypertension, propranolol produces a significant reduction in blood
pressure without prominent postural hypotension.
Pharmacokinetics & Dosage
See Table 11–2. Resting
bradycardia and a reduction in the heart rate during exercise are
indicators of propranolol's -blocking effect, and changes in these
parameters may be used as guides for regulating dosage. Propranolol can
be administered twice daily, and slow-release preparations are available.
Toxicity
The principal toxicities of
propranolol result from blockade of cardiac, vascular, or bronchial receptors and are described in more
detail in Chapter 10. The most important of these predictable extensions
of the -blocking action occur in patients with
bradycardia or cardiac conduction disease, asthma, peripheral vascular
insufficiency, and diabetes.
When propranolol is discontinued
after prolonged regular use, some patients experience a withdrawal
syndrome, manifested by nervousness, tachycardia, increased intensity of
angina, and increase of blood pressure. Myocardial infarction has been
reported in a few patients. Although the incidence of these complications
is probably low, propranolol should not be discontinued abruptly. The
withdrawal syndrome may involve up-regulation or supersensitivity of adrenoceptors.
Metoprolol & Atenolol
Metoprolol and atenolol, which
are cardioselective, are the most widely used blockers in the treatment of
hypertension. Metoprolol is approximately equipotent to propranolol in
inhibiting stimulation of 1 adrenoceptors such as
those in the heart but 50- to 100-fold less potent than propranolol in
blocking 2 receptors. Relative
cardioselectivity may be advantageous in treating hypertensive patients
who also suffer from asthma, diabetes, or peripheral vascular disease.
Although cardioselectivity is not complete, metoprolol causes less
bronchial constriction than propranolol at doses that produce equal
inhibition of 1 adrenoceptor responses.
Metoprolol is extensively metabolized by CYP2D6 with high first-pass
metabolism. The drug has a relatively short half-life of 4–6 hours, but
the extended-release preparation can be dosed twice daily (Table 11–2).
Sustained-release metoprolol is effective in reducing mortality from
heart failure and is particularly useful in patients with hypertension
and heart failure.
Atenolol is not extensively
metabolized and is excreted primarily in the urine with a half-life of 6
hours; it is usually dosed once daily. Recent studies have found atenolol
less effective than metoprolol in preventing the complications of
hypertension. A possible reason for this difference is that once-daily
dosing does not maintain adequate blood levels of atenolol. The usual
dosage is 50–100 mg/d. Patients with reduced renal function should
receive lower doses.
Nadolol, Carteolol, Betaxolol,
& Bisoprolol
Nadolol and carteolol,
nonselective -receptor antagonists, are not
appreciably metabolized and are excreted to a considerable extent in the
urine. Betaxolol and bisoprolol are 1-selective blockers that
are primarily metabolized in the liver but have long half-lives. Because
of these relatively long half-lives, these drugs can be administered once
daily. Nadolol is usually begun at a dosage of 40 mg/d, carteolol at 2.5
mg/d, betaxolol at 10 mg/d, and bisoprolol at 5 mg/d. Increases in dosage
to obtain a satisfactory therapeutic effect should take place no more
often than every 4 or 5 days. Patients with reduced renal function should
receive correspondingly reduced doses of nadolol and carteolol.
Pindolol, Acebutolol, &
Penbutolol
Pindolol, acebutolol, and
penbutolol are partial agonists, ie, blockers with some intrinsic
sympathomimetic activity. They lower blood pressure by decreasing
vascular resistance and appear to depress cardiac output or heart rate
less than other blockers, perhaps because of significantly
greater agonist than antagonist effects at 2 receptors. This may be
particularly beneficial for patients with bradyarrhythmias or peripheral
vascular disease. Daily doses of pindolol start at 10 mg; of acebutolol,
at 400 mg; and of penbutolol, at 20 mg.
Labetalol, Carvedilol, &
Nebivolol
These drugs have both blocking and vasodilating effects.
Labetalol is formulated as a racemic mixture of four isomers (it has two
centers of asymmetry). Two of these isomers—the (S,S)- and (R,S)-isomers—are
relatively inactive, a third (S,R)- is a potent blocker, and the last (R,R)- is
a potent blocker. Labetalol has a 3:1 ratio of : antagonism after oral dosing. Blood
pressure is lowered by reduction of systemic vascular resistance (via blockade) without significant
alteration in heart rate or cardiac output. Because of its combined - and -blocking activity, labetalol is useful
in treating the hypertension of pheochromocytoma and hypertensive
emergencies. Oral daily doses of labetalol range from 200 to 2400 mg/d.
Labetalol is given as repeated intravenous bolus injections of 20–80 mg
to treat hypertensive emergencies.
Carvedilol, like labetalol, is
administered as a racemic mixture. The S(–) isomer is a
nonselective -adrenoceptor blocker, but both S(–)
and R(+) isomers have approximately equal -blocking potency. The isomers are
stereoselectively metabolized in the liver, which means that their
elimination half-lives may differ. The average half-life is 7–10 hours.
The usual starting dosage of carvedilol for ordinary hypertension is 6.25
mg twice daily. Carvedilol reduces mortality in patients with heart
failure and is therefore particularly useful in patients with both heart
failure and hypertension.
Nebivolol is a 1-selective blocker with
vasodilating properties that are not mediated by blockade. D-Nebivolol
has highly selective 1 blocking effects, while
the L-isomer causes vasodilation; it
is marketed as a racemic mixture. The vasodilating effect may be due to
an increase in endothelial release of nitric oxide via induction of
endothelial nitric oxide synthase. The hemodynamic effects of nebivolol
therefore differ from those of pure blockers in that peripheral vascular
resistance is acutely lowered (by nebivolol) as opposed to increased (by
the older agents). Nebivolol is extensively metabolized and has active
metabolites. The half-life is 10–12 hours, but the drug can be given once
daily. Dosing is generally started at 5 mg/d, with dose escalation as
high as 40 mg, if necessary. The efficacy of nebivolol is similar to that
of other antihypertensive agents, but several studies report fewer
adverse effects.
Esmolol
Esmolol is a 1-selective blocker that is
rapidly metabolized via hydrolysis by red blood cell esterases. It has a
short half-life (9–10 minutes) and is administered by constant
intravenous infusion. Esmolol is generally administered as a loading dose
(0.5–1 mg/kg), followed by a constant infusion. The infusion is typically
started at 50–150 mcg/kg/min, and the dose increased every 5 minutes, up
to 300 mcg/kg/min, as needed to achieve the desired therapeutic effect.
Esmolol is used for management of intraoperative and postoperative
hypertension, and sometimes for hypertensive emergencies, particularly
when hypertension is associated with tachycardia.
Prazosin & Other Alpha1
Blockers
Mechanism & Sites of Action
Prazosin, terazosin, and
doxazosin produce most of their antihypertensive effects by selectively
blocking 1 receptors in arterioles
and venules. These agents produce less reflex tachycardia when lowering
blood pressure than do nonselective antagonists such as phentolamine. Alpha1-receptor
selectivity allows norepinephrine to exert unopposed negative feedback
(mediated by presynaptic 2 receptors) on its own
release (see Chapter 6); in contrast, phentolamine blocks both
presynaptic and postsynaptic receptors, with the result that reflex
activation of sympathetic neurons by phentolamine's effects produces
greater release of transmitter onto receptors and correspondingly greater
cardioacceleration.
Alpha blockers reduce arterial
pressure by dilating both resistance and capacitance vessels. As
expected, blood pressure is reduced more in the upright than in the
supine position. Retention of salt and water occurs when these drugs are
administered without a diuretic. The drugs are more effective when used
in combination with other agents, such as a blocker and a diuretic, than when used
alone. Owing to their beneficial effects in men with prostatic
hyperplasia and bladder obstruction symptoms, these drugs are used
primarily in men with concurrent hypertension and benign prostatic
hyperplasia.
Pharmacokinetics & Dosage
Pharmacokinetic characteristics
of prazosin are listed in Table 11–2. Terazosin is also extensively
metabolized but undergoes very little first-pass metabolism and has a
half-life of 12 hours. Doxazosin has an intermediate bioavailability and
a half-life of 22 hours.
Terazosin can often be given
once daily, with doses of 5–20 mg/d. Doxazosin is usually given once
daily starting at 1 mg/d and progressing to 4 mg/d or more as needed.
Although long-term treatment with these blockers causes relatively little
postural hypotension, a precipitous drop in standing blood pressure
develops in some patients shortly after the first dose is absorbed. For
this reason, the first dose should be small and should be administered at
bedtime. Although the mechanism of this first-dose phenomenon is not
clear, it occurs more commonly in patients who are salt- and
volume-depleted.
Aside from the first-dose
phenomenon, the reported toxicities of the 1 blockers are relatively
infrequent and mild. These include dizziness, palpitations, headache, and
lassitude. Some patients develop a positive test for antinuclear factor
in serum while on prazosin therapy, but this has not been associated with
rheumatic symptoms. The 1 blockers do not adversely
and may even beneficially affect plasma lipid profiles, but this action
has not been shown to confer any benefit on clinical outcomes.
Other
Alpha-Adrenoceptor–Blocking Agents
The nonselective agents, phentolamine
and phenoxybenzamine, are useful in diagnosis and treatment of
pheochromocytoma and in other clinical situations associated with
exaggerated release of catecholamines (eg, phentolamine may be combined
with propranolol to treat the clonidinewithdrawal syndrome, described
previously). Their pharmacology is described in Chapter 10.
Vasodilators
Mechanism & Sites of Action
This class of drugs includes the
oral vasodilators, hydralazine and minoxidil, which are used for
long-term outpatient therapy of hypertension; the parenteral
vasodilators, nitroprusside, diazoxide, and fenoldopam, which are used to
treat hypertensive emergencies; the calcium channel blockers, which are
used in both circumstances; and the nitrates, which are used mainly in
angina (Table 11–3).
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Table 11–3 Mechanisms of Action
of Vasodilators.
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Mechanism
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Examples
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Release of
nitric oxide from drug or endothelium
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Nitroprusside,
hydralazine, nitrates,1 histamine, acetylcholine
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Reduction
of calcium influx
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Verapamil,
diltiazem, nifedipine
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Hyperpolarization
of smooth muscle membrane through opening of potassium channels
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Minoxidil,
diazoxide
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Activation
of dopamine receptors
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Fenoldopam
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1See Chapter 12.
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Chapter 12 contains additional
discussion of vasodilators. All the vasodilators that are useful in
hypertension relax smooth muscle of arterioles, thereby decreasing
systemic vascular resistance. Sodium nitroprusside and the nitrates also
relax veins. Decreased arterial resistance and decreased mean arterial
blood pressure elicit compensatory responses, mediated by baroreceptors
and the sympathetic nervous system (Figure 11–4), as well as renin,
angiotensin, and aldosterone. Because sympathetic reflexes are intact,
vasodilator therapy does not cause orthostatic hypotension or sexual
dysfunction.
Vasodilators work best in
combination with other antihypertensive drugs that oppose the
compensatory cardiovascular responses. (See Resistant Hypertension &
Polypharmacy.)
Hydralazine
Hydralazine, a hydrazine
derivative, dilates arterioles but not veins. It has been available for
many years, although it was initially thought not to be particularly
effective because tachyphylaxis to its antihypertensive effects developed
rapidly. The benefits of combination therapy are now recognized, and
hydralazine may be used more effectively, particularly in severe
hypertension. The combination of hydralazine with nitrates is effective
in heart failure and should be considered in patients with both
hypertension and heart failure, especially in African-American patients.
Pharmacokinetics & Dosage
Hydralazine is well absorbed and
rapidly metabolized by the liver during the first pass, so that
bioavailability is low (averaging 25%) and variable among individuals. It
is metabolized in part by acetylation at a rate that appears to be
bimodally distributed in the population (see Chapter 4). As a
consequence, rapid acetylators have greater first-pass metabolism, lower
blood levels, and less antihypertensive benefit from a given dose than do
slow acetylators. The half-life of hydralazine ranges from 1.5 to 3
hours, but vascular effects persist longer than do blood concentrations,
possibly due to avid binding to vascular tissue.
Usual dosage ranges from 40 mg/d
to 200 mg/d. The higher dosage was selected as the dose at which there is
a small possibility of developing the lupus erythematosus-like syndrome
described in the next section. However, higher dosages result in greater
vasodilation and may be used if necessary. Dosing two or three times
daily provides smooth control of blood pressure.
Toxicity
The most common adverse effects
of hydralazine are headache, nausea, anorexia, palpitations, sweating,
and flushing. In patients with ischemic heart disease, reflex tachycardia
and sympathetic stimulation may provoke angina or ischemic arrhythmias.
With dosages of 400 mg/d or more, there is a 10–20% incidence—chiefly in
persons who slowly acetylate the drug—of a syndrome characterized by
arthralgia, myalgia, skin rashes, and fever that resembles lupus
erythematosus. The syndrome is not associated with renal damage and is
reversed by discontinuance of hydralazine. Peripheral neuropathy and drug
fever are other serious but uncommon adverse effects.
Minoxidil
Minoxidil is a very efficacious
orally active vasodilator. The effect results from the opening of
potassium channels in smooth muscle membranes by minoxidil sulfate, the
active metabolite. Increased potassium permeability stabilizes the
membrane at its resting potential and makes contraction less likely. Like
hydralazine, minoxidil dilates arterioles but not veins. Because of its
greater potential antihypertensive effect, minoxidil should replace
hydralazine when maximal doses of the latter are not effective or in
patients with renal failure and severe hypertension, who do not respond
well to hydralazine.
Pharmacokinetics & Dosage
Pharmacokinetic parameters of
minoxidil are listed in Table 11–2. Even more than with hydralazine, the
use of minoxidil is associated with reflex sympathetic stimulation and
sodium and fluid retention. Minoxidil must be used in combination with a blocker and a loop diuretic.
Toxicity
Tachycardia, palpitations,
angina, and edema are observed when doses of blockers and diuretics are inadequate.
Headache, sweating, and hypertrichosis, which is particularly bothersome
in women, are relatively common. Minoxidil illustrates how one person's
toxicity may become another person's therapy. Topical minoxidil (as
Rogaine) is used as a stimulant to hair growth for correction of
baldness.
Sodium Nitroprusside
Sodium nitroprusside is a
powerful parenterally administered vasodilator that is used in treating
hypertensive emergencies as well as severe heart failure. Nitroprusside
dilates both arterial and venous vessels, resulting in reduced peripheral
vascular resistance and venous return. The action occurs as a result of
activation of guanylyl cyclase, either via release of nitric oxide or by
direct stimulation of the enzyme. The result is increased intracellular
cGMP, which relaxes vascular smooth muscle (Figure 12–2).
In the absence of heart failure,
blood pressure decreases, owing to decreased vascular resistance, whereas
cardiac output does not change or decreases slightly. In patients with
heart failure and low cardiac output, output often increases owing to
afterload reduction.
Pharmacokinetics & Dosage
Nitroprusside is a complex of
iron, cyanide groups, and a nitroso moiety. It is rapidly metabolized by
uptake into red blood cells with liberation of cyanide. Cyanide in turn
is metabolized by the mitochondrial enzyme rhodanase, in the presence of
a sulfur donor, to the less toxic thiocyanate. Thiocyanate is distributed
in extracellular fluid and slowly eliminated by the kidney.
Nitroprusside rapidly lowers
blood pressure, and its effects disappear within 1–10 minutes after
discontinuation. The drug is given by intravenous infusion. Sodium
nitroprusside in aqueous solution is sensitive to light and must
therefore be made up fresh before each administration and covered with
opaque foil. Infusion solutions should be changed after several hours.
Dosage typically begins at 0.5 mcg/kg/min and may be increased up to 10
mcg/kg/min as necessary to control blood pressure. Higher rates of
infusion, if continued for more than an hour, may result in toxicity.
Because of its efficacy and rapid onset of effect, nitroprusside should
be administered by infusion pump and arterial blood pressure continuously
monitored via intra-arterial recording.
Toxicity
Other than excessive blood
pressure lowering, the most serious toxicity is related to accumulation
of cyanide; metabolic acidosis, arrhythmias, excessive hypotension, and
death have resulted. In a few cases, toxicity after relatively low doses
of nitroprusside suggested a defect in cyanide metabolism. Administration
of sodium thiosulfate as a sulfur donor facilitates metabolism of
cyanide. Hydroxocobalamin combines with cyanide to form the nontoxic
cyanocobalamin. Both have been advocated for prophylaxis or treatment of
cyanide poisoning during nitroprusside infusion. Thiocyanate may
accumulate over the course of prolonged administration, usually several
days or more, particularly in patients with renal insufficiency who do
not excrete thiocyanate at a normal rate. Thiocyanate toxicity is
manifested as weakness, disorientation, psychosis, muscle spasms, and
convulsions, and the diagnosis is confirmed by finding serum
concentrations greater than 10 mg/dL. Rarely, delayed hypothyroidism
occurs, owing to thiocyanate inhibition of iodide uptake by the thyroid.
Methemoglobinemia during infusion of nitroprusside has also been
reported.
Diazoxide
Diazoxide is an effective and
relatively long-acting parenterally administered arteriolar dilator that
is occasionally used to treat hypertensive emergencies. Injection of
diazoxide results in a rapid fall in systemic vascular resistance and
mean arterial blood pressure associated with substantial tachycardia and
increase in cardiac output. Studies of its mechanism suggest that it prevents
vascular smooth muscle contraction by opening potassium channels and
stabilizing the membrane potential at the resting level.
Pharmacokinetics & Dosage
Diazoxide is similar chemically
to the thiazide diuretics but has no diuretic activity. It is bound
extensively to serum albumin and to vascular tissue. Diazoxide is
partially metabolized; its metabolic pathways are not well characterized.
The remainder is excreted unchanged. Its half-life is approximately 24
hours, but the relationship between blood concentration and hypotensive
action is not well established. The blood pressure-lowering effect after
a rapid injection is established within 5 minutes and lasts for 4–12
hours.
When diazoxide was first
marketed, a dose of 300 mg by rapid injection was recommended. It
appears, however, that excessive hypotension can be avoided by beginning
with smaller doses (50–150 mg). If necessary, doses of 150 mg may be
repeated every 5 minutes until blood pressure is lowered satisfactorily.
Nearly all patients respond to a maximum of three or four doses.
Alternatively, diazoxide may be administered by intravenous infusion at
rates of 15–30 mg/min. Because of reduced protein binding, hypotension
occurs after smaller doses in persons with chronic renal failure, and
smaller doses should be administered to these patients. The hypotensive
effects of diazoxide are also greater when patients are pretreated with blockers to prevent the reflex
tachycardia and associated increase in cardiac output.
Toxicity
The most significant toxicity
from diazoxide has been excessive hypotension, resulting from the
recommendation to use a fixed dose of 300 mg in all patients. Such
hypotension has resulted in stroke and myocardial infarction. The reflex
sympathetic response can provoke angina, electrocardiographic evidence of
ischemia, and cardiac failure in patients with ischemic heart disease,
and diazoxide should be avoided in this situation.
Diazoxide inhibits insulin
release from the pancreas (probably by opening potassium channels in the
beta cell membrane) and is used to treat hypoglycemia secondary to
insulinoma. Occasionally, hyperglycemia complicates diazoxide use,
particularly in persons with renal insufficiency.
In contrast to the structurally
related thiazide diuretics, diazoxide causes renal salt and water retention.
However, because the drug is used for short periods only, this is
rarely a problem.
Fenoldopam
Fenoldopam is a peripheral
arteriolar dilator used for hypertensive emergencies and postoperative
hypertension. It acts primarily as an agonist of dopamine D1
receptors, resulting in dilation of peripheral arteries and natriuresis.
The commercial product is a racemic mixture with the (R)-isomer
mediating the pharmacologic activity.
Fenoldopam is rapidly
metabolized, primarily by conjugation. Its half-life is 10 minutes. The
drug is administered by continuous intravenous infusion. Fenoldopam is
initiated at a low dosage (0.1 mcg/kg/min), and the dose is then titrated
upward every 15 or 20 minutes to a maximum dose of 1.6 mcg/kg/min or
until the desired blood pressure reduction is achieved.
As with other direct
vasodilators, the major toxicities are reflex tachycardia, headache, and
flushing. Fenoldopam also increases intraocular pressure and should be
avoided in patients with glaucoma.
Calcium Channel Blockers
In addition to their antianginal
(see Chapter 12) and antiarrhythmic effects (see Chapter 14), calcium
channel blockers also reduce peripheral resistance and blood pressure.
The mechanism of action in hypertension (and, in part, in angina) is
inhibition of calcium influx into arterial smooth muscle cells.
Verapamil, diltiazem, and
the dihydropyridine family (amlodipine, felodipine, isradipine,
nicardipine, nifedipine, and nisoldipine) are all equally
effective in lowering blood pressure, and many formulations are currently
approved for this use in the USA. Clevidipine is a newer member of
this group that is formulated for intravenous use only.
Hemodynamic differences among
calcium channel blockers may influence the choice of a particular agent.
Nifedipine and the other dihydropyridine agents are more selective as
vasodilators and have less cardiac depressant effect than verapamil and
diltiazem. Reflex sympathetic activation with slight tachycardia
maintains or increases cardiac output in most patients given
dihydropyridines. Verapamil has the greatest depressant effect on the
heart and may decrease heart rate and cardiac output. Diltiazem has
intermediate actions. The pharmacology and toxicity of these drugs is
discussed in more detail in Chapter 12. Doses of calcium channel blockers
used in treating hypertension are similar to those used in treating
angina. Some epidemiologic studies reported an increased risk of
myocardial infarction or mortality in patients receiving short-acting
nifedipine for hypertension. It is therefore recommended that
short-acting oral dihydropyridines not be used for hypertension.
Sustained-release calcium blockers or calcium blockers with long
half-lives provide smoother blood pressure control and are more
appropriate for treatment of chronic hypertension. Intravenous
nicardipine and clevidipine are available for the treatment of
hypertension when oral therapy is not feasible; parenteral verapamil and
diltiazem can also be used for the same indication. Nicardipine is
typically infused at rates of 2–15 mg/h. Clevidipine is infused starting
at 1–2 mg/h and progressing to 4–6 mg/h. It has a rapid onset of action
and has been used in acute hypertension occurring during surgery. Oral
short-acting nifedipine has been used in emergency management of severe
hypertension.
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