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Systemic Antifungal Drugs for Systemic Infections
Amphotericin B
Amphotericin A and B are
antifungal antibiotics produced by Streptomyces nodosus.
Amphotericin A is not in clinical use.
Chemistry
Amphotericin B is an amphoteric
polyene macrolide (polyene = containing many double bonds; macrolide =
containing a large lactone ring of 12 or more atoms). It is nearly
insoluble in water and is therefore prepared as a colloidal suspension of
amphotericin B and sodium desoxycholate for intravenous injection.
Several new formulations have been developed in which amphotericin B is
packaged in a lipid-associated delivery system (Table 48–1 and Liposomal
Amphotericin B).
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Table 48–1 Properties of
Conventional Amphotericin B and Some Lipid Formulations.1
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Drug
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Physical
Form
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Dosing
(mg/kg/d)
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Cmax
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Clearance
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Nephrotoxicity
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Infusional
Toxicity
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Daily Cost
($)
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Conventional
formulation
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Fungizone
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Micelles
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1
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. . .
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. . .
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. . .
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. . .
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24
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Lipid
formulations
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AmBisome
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Spheres
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3–5
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1300
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Amphotec
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Disks
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5
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(?)
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660
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Abelcet
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Ribbons
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5
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(?)
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570
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1Changes in Cmax (peak plasma
concentration), clearance, nephrotoxicity, and infusional toxicity are
relative to conventional amphotericin B.
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Liposomal Amphotericin B
Therapy with amphotericin B is
often limited by toxicity, especially drug-induced renal impairment.
This has led to the development of lipid drug formulations on the
assumption that lipid-packaged drug binds to the mammalian membrane
less readily, permitting the use of effective doses of the drug with
lower toxicity. Liposomal amphotericin preparations package the active
drug in lipid delivery vehicles, in contrast to the colloidal
suspensions, which were previously the only available forms.
Amphotericin binds to the lipids in these vehicles with an affinity
between that for fungal ergosterol and that for human cholesterol. The
lipid vehicle then serves as an amphotericin reservoir, reducing
nonspecific binding to human cell membranes. This preferential binding
allows for a reduction of toxicity without sacrificing efficacy and
permits use of larger doses. Furthermore, some fungi contain lipases
that may liberate free amphotericin B directly at the site of
infection.
Three such formulations are
now available and have differing pharmacologic properties as summarized
in Table 48–1. Although clinical trials have demonstrated different
renal and infusion-related toxicities for these preparations compared
with regular amphotericin B, there are no trials comparing the
different formulations with each other. Limited studies have suggested
at best a moderate improvement in the clinical efficacy of the lipid
formulations compared with conventional amphotericin B. Because the
lipid preparations are much more expensive, their use is usually
restricted to patients intolerant to, or not responding to,
conventional amphotericin treatment.
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Pharmacokinetics
Amphotericin B is poorly
absorbed from the gastrointestinal tract. Oral amphotericin B is thus
effective only on fungi within the lumen of the tract and cannot be used
for treatment of systemic disease. The intravenous injection of 0.6
mg/kg/d of amphotericin B results in average blood levels of 0.3–1
mcg/mL; the drug is more than 90% bound by serum proteins. Although it is
mostly metabolized, some amphotericin B is excreted slowly in the urine
over a period of several days. The serum t1/2 is
approximately 15 days. Hepatic impairment, renal impairment, and dialysis
have little impact on drug concentrations, and therefore no dose
adjustment is required. The drug is widely distributed in most tissues,
but only 2–3% of the blood level is reached in cerebrospinal fluid, thus
occasionally necessitating intrathecal therapy for certain types of
fungal meningitis.
Mechanism of Action
Amphotericin B is selective in
its fungicidal effect because it exploits the difference in lipid
composition of fungal and mammalian cell membranes. Ergosterol, a
cell membrane sterol, is found in the cell membrane of fungi, whereas the
predominant sterol of bacteria and human cells is cholesterol.
Amphotericin B binds to ergosterol and alters the permeability of the
cell by forming amphotericin B-associated pores in the cell membrane
(Figure 48–1). As suggested by its chemistry, amphotericin B combines
avidly with lipids (ergosterol) along the double bond-rich side of its
structure and associates with water molecules along the hydroxyl-rich
side. This amphipathic characteristic facilitates pore formation by
multiple amphotericin molecules, with the lipophilic portions around the
outside of the pore and the hydrophilic regions lining the inside. The
pore allows the leakage of intracellular ions and macromolecules,
eventually leading to cell death. Some binding to human membrane sterols
does occur, probably accounting for the drug's prominent toxicity.
Resistance to amphotericin B
occurs if ergosterol binding is impaired, either by decreasing the
membrane concentration of ergosterol or by modifying the sterol target
molecule to reduce its affinity for the drug.
Antifungal Activity
Amphotericin B remains the
antifungal agent with the broadest spectrum of action. It has activity
against the clinically significant yeasts, including Candida albicans and
Cryptococcus neoformans; the organisms causing endemic mycoses,
including Histoplasma capsulatum, Blastomyces dermatitidis, and Coccidioides
immitis; and the pathogenic molds, such as Aspergillus fumigatus
and mucor. Some fungal organisms such as Candida lusitaniae and Pseudallescheria
boydii display intrinsic amphotericin B resistance.
Clinical Use
Owing to its broad spectrum of
activity and fungicidal action, amphotericin B remains a useful agent for
nearly all life-threatening mycotic infections, although newer less toxic
agents have largely replaced amphotericin B for most conditions. It is
often used as the initial induction regimen in order to rapidly reduce
fungal burden and is then replaced by one of the newer azole drugs
(described below) for chronic therapy or prevention of relapse. Such
induction therapy is especially important for immunosuppressed patients
and those with severe fungal pneumonia, severe cryptococcal meningitis,
or disseminated infections with one of the endemic mycoses such as
histoplasmosis or coccidioidomycosis. Once a clinical response has been
elicited, these patients then often continue maintenance therapy with an
azole; therapy may be lifelong in patients at high risk for disease
relapse. For treatment of systemic fungal disease, amphotericin B is given
by slow intravenous infusion at a dosage of 0.5–1 mg/kg/d. It is usually
continued to a defined total dose (eg, 1–2 g), rather than a defined time
span, as used with other antimicrobial drugs.
Intrathecal therapy for fungal
meningitis is poorly tolerated and fraught with difficulties related to
maintaining cerebrospinal fluid access. Thus, intrathecal therapy with
amphotericin B is being increasingly supplanted by other therapies but
remains an option in cases of fungal central nervous system infections that
have not responded to other agents.
Local or topical administration
of amphotericin B has been used with success. Mycotic corneal ulcers and
keratitis can be cured with topical drops as well as by direct
subconjunctival injection. Fungal arthritis has been treated with
adjunctive local injection directly into the joint. Candiduria responds
to bladder irrigation with amphotericin B, and this route has been shown
to produce no significant systemic toxicity.
Adverse Effects
The toxicity of amphotericin B can
be divided into two broad categories: immediate reactions, related to the
infusion of the drug, and those occurring more slowly.
Infusion-Related Toxicity
Infusion-related reactions are
nearly universal and consist of fever, chills, muscle spasms, vomiting,
headache, and hypotension. They can be ameliorated by slowing the
infusion rate or decreasing the daily dose. Premedication with
antipyretics, antihistamines, meperidine, or corticosteroids can be
helpful. When starting therapy, many clinicians administer a test dose of
1 mg intravenously to gauge the severity of the reaction. This can serve
as a guide to an initial dosing regimen and premedication strategy.
Cumulative Toxicity
Renal damage is the most
significant toxic reaction. Renal impairment occurs in nearly all
patients treated with clinically significant doses of amphotericin. The
degree of azotemia is variable and often stabilizes during therapy, but
it can be serious enough to necessitate dialysis. A reversible component
is associated with decreased renal perfusion and represents a form of
prerenal renal failure. An irreversible component results from renal
tubular injury and subsequent dysfunction. The irreversible form of
amphotericin nephrotoxicity usually occurs in the setting of prolonged administration
(> 4 g cumulative dose). Renal toxicity commonly manifests as renal
tubular acidosis and severe potassium and magnesium wasting. There is
some evidence that the prerenal component can be attenuated with sodium
loading, and it is common practice to administer normal saline infusions
with the daily doses of amphotericin B.
Abnormalities of liver function
tests are occasionally seen, as is a varying degree of anemia due to
reduced erythropoietin production by damaged renal tubular cells. After intrathecal
therapy with amphotericin, seizures and a chemical arachnoiditis may
develop, often with serious neurologic sequelae.
Flucytosine
Flucytosine (5-FC) was
discovered in 1957 during a search for novel antineoplastic agents.
Though devoid of anticancer properties, it became apparent that it was a
potent antifungal agent. Flucytosine is a water-soluble pyrimidine analog
related to the chemotherapeutic agent fluorouracil (5-FU). Its spectrum
of action is much narrower than that of amphotericin B.
Pharmacokinetics
Flucytosine is currently
available in North America only in an oral formulation. The dosage is 100–150
mg/kg/d in patients with normal renal function. It is well absorbed (>
90%), with serum concentrations peaking 1–2 hours after an oral dose. It
is poorly protein-bound and penetrates well into all body fluid
compartments, including the cerebrospinal fluid. It is eliminated by
glomerular filtration with a half-life of 3–4 hours and is removed by
hemodialysis. Levels rise rapidly with renal impairment and can lead to
toxicity. Toxicity is more likely to occur in AIDS patients and those
with renal insufficiency. Peak serum concentrations should be measured
periodically in patients with renal insufficiency and maintained between
50 and 100 mcg/mL.
Mechanism of Action
Flucytosine is taken up by
fungal cells via the enzyme cytosine permease. It is converted
intracellularly first to 5-FU and then to 5-fluorodeoxyuridine
monophosphate (FdUMP) and fluorouridine triphosphate (FUTP), which
inhibit DNA and RNA synthesis, respectively (Figure 48–1). Human cells
are unable to convert the parent drug to its active metabolites,
resulting in selective toxicity.
Synergy with amphotericin B has
been demonstrated in vitro and in vivo. It may be related to enhanced
penetration of the flucytosine through amphotericin-damaged fungal cell
membranes. In vitro synergy with azole drugs has also been seen, although
the mechanism is unclear.
Resistance is thought to be
mediated through altered metabolism of flucytosine, and, though uncommon
in primary isolates, it develops rapidly in the course of flucytosine
monotherapy.
Clinical Use
The spectrum of activity of
flucytosine is restricted to C neoformans, some candida species,
and the dematiaceous molds that cause chromoblastomycosis. Flucytosine is
not used as a single agent because of its demonstrated synergy with other
agents and to avoid the development of secondary resistance. Clinical use
at present is confined to combination therapy, either with amphotericin B
for cryptococcal meningitis or with itraconazole for chromoblastomycosis.
Adverse Effects
The adverse effects of flucytosine
result from metabolism (possibly by intestinal flora) to the toxic
antineoplastic compound fluorouracil. Bone marrow toxicity with anemia,
leukopenia, and thrombocytopenia are the most common adverse effects,
with derangement of liver enzymes occurring less frequently. A form of
toxic enterocolitis can occur. There seems to be a narrow therapeutic
window, with an increased risk of toxicity at higher drug levels and
resistance developing rapidly at subtherapeutic concentrations. The use
of drug concentration measurements may be helpful in reducing the
incidence of toxic reactions, especially when flucytosine is combined
with nephrotoxic agents such as amphotericin B.
Azoles
Azoles are synthetic compounds
that can be classified as either imidazoles or triazoles according to the
number of nitrogen atoms in the five-membered azole ring, as indicated
below. The imidazoles consist of ketoconazole, miconazole, and
clotrimazole (Figure 48–2). The latter two drugs are now used only in
topical therapy. The triazoles include itraconazole, fluconazole,
voriconazole, and posaconazole.
Pharmacokinetics
The pharmacology of each of the
azoles is unique and accounts for some of the variations in clinical use.
Table 48–2 summarizes the differences among five of the azoles.
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Table 48–2 Pharmacologic
properties of five systemic azole drugs
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Water Solubility
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Absorption
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CSF: Serum
Concentration Ratio
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t 1/2 (Hours)
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Elimination
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Formulations
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Ketoconazole
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Low
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Variable
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< 0.1
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7–10
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Hepatic
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Oral
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Itraconazole
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Low
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Variable
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< 0.01
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24–42
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Hepatic
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Oral, IV
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Fluconazole
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High
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High
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> 0.7
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22–31
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Renal
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Oral, IV
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Voriconazole
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High
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High
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. . .
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6
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Hepatic
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Oral, IV
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Posaconazole
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Low
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High
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. . .
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25
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Hepatic
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Oral
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Mechanism of Action
The antifungal activity of azole
drugs results from the reduction of ergosterol synthesis by inhibition of
fungal cytochrome P450 enzymes (Figure 48–1). The selective toxicity of
azole drugs results from their greater affinity for fungal than for human
cytochrome P450 enzymes. Imidazoles exhibit a lesser degree of
selectivity than the triazoles, accounting for their higher incidence of
drug interactions and side effects.
Resistance to azoles occurs via
multiple mechanisms. Once rare, increasing numbers of resistant strains
are being reported, suggesting that increasing use of these agents for
prophylaxis and therapy may be selecting for clinical drug resistance in
certain settings.
Clinical Use
The spectrum of action of azole
medications is broad, including many candida species, C neoformans,
the endemic mycoses (blastomycosis, coccidioidomycosis, histoplasmosis),
the dermatophytes, and, in the case of itraconazole and voriconazole,
even aspergillus infections. They are also useful in the treatment of
intrinsically amphotericin-resistant organisms such as P boydii.
Adverse Effects
As a group, the azoles are
relatively nontoxic. The most common adverse reaction is relatively minor
gastrointestinal upset. All azoles have been reported to cause
abnormalities in liver enzymes and, very rarely, clinical hepatitis.
Adverse effects specific to individual agents are discussed below.
Drug Interactions
All azole drugs affect the
mammalian cytochrome P450 system of enzymes to some extent, and
consequently they are prone to drug interactions. The most significant
reactions are indicated below.
Ketoconazole
Ketoconazole was the first oral
azole introduced into clinical use. It is distinguished from triazoles by
its greater propensity to inhibit mammalian cytochrome P450 enzymes; that
is, it is less selective for fungal P450 than are the newer azoles. As a
result, systemic ketoconazole has fallen out of clinical use in the USA
and is not discussed in any detail here. Its dermatologic use is
discussed in Chapter 61.
Itraconazole
Itraconazole is available in
oral and intravenous formulations and is used at a dosage of 100–400
mg/d. Drug absorption is increased by food and by low gastric pH. Like
other lipid-soluble azoles, it interacts with hepatic microsomal enzymes,
though to a lesser degree than ketoconazole. An important drug
interaction is reduced bioavailability of itraconazole when taken with
rifamycins (rifampin, rifabutin, rifapentine). It does not affect
mammalian steroid synthesis, and its effects on the metabolism of other
hepatically cleared medications are much less than those of ketoconazole.
While itraconazole displays potent antifungal activity, effectiveness can
be limited by reduced bioavailability. Newer formulations, including an
oral liquid and an intravenous preparation, have utilized cyclodextran as
a carrier molecule to enhance solubility and bioavailability. Like
ketoconazole, it penetrates poorly into the cerebrospinal fluid.
Itraconazole is the azole of choice for treatment of disease due to the
dimorphic fungi histoplasma, Blastomyces, and sporothrix.
Itraconazole has activity against Aspergillus sp, but it has been
replaced by voriconazole as the azole of choice for aspergillosis.
Itraconazole is used extensively in the treatment of dermatophytoses and
onychomycosis.
Fluconazole
Fluconazole displays a high
degree of water solubility and good cerebrospinal fluid penetration.
Unlike ketoconazole and itraconazole, its oral bioavailability is high.
Drug interactions are also less common because fluconazole has the least
effect of all the azoles on hepatic microsomal enzymes. Because of fewer
hepatic enzyme interactions and better gastrointestinal tolerance,
fluconazole has the widest therapeutic index of the azoles, permitting
more aggressive dosing in a variety of fungal infections. The drug is available
in oral and intravenous formulations and is used at a dosage of 100–800
mg/d.
Fluconazole is the azole of
choice in the treatment and secondary prophylaxis of cryptococcal
meningitis. Intravenous fluconazole has been shown to be equivalent to
amphotericin B in treatment of candidemia in ICU patients with normal
white blood cell counts. Fluconazole is the agent most commonly used for
the treatment of mucocutaneous candidiasis. Activity against the
dimorphic fungi is limited to coccidioidal disease, and in particular for
meningitis, where high doses of fluconazole often obviate the need for
intrathecal amphotericin B. Fluconazole displays no activity against
aspergillus or other filamentous fungi.
Prophylactic use of fluconazole
has been demonstrated to reduce fungal disease in bone marrow transplant
recipients and AIDS patients, but the emergence of fluconazole-resistant
fungi has raised concerns about this indication.
Voriconazole
Voriconazole is available in
intravenous and oral formulations. The recommended dosage is 400 mg/d.
The drug is well absorbed orally, with a bioavailability exceeding 90%,
and it exhibits less protein binding than itraconazole. Metabolism is
predominantly hepatic. Voriconazole is a clinically relevant inhibitor of
mammalian CYP3A4. As a result, dose reduction of a number of medications
is required when voriconazole is started, including cyclosporine,
tacrolimus, and HMG-CoA reductase inhibitors. Observed toxicities include
rash and elevated hepatic enzymes. Visual disturbances are common,
occurring in up to 30% of patients receiving intravenous voriconazole,
and include blurring and changes in color vision or brightness. These
visual changes usually occur immediately after a dose of voriconazole and
resolve within 30 minutes. Photosensitivity dermatitis is commonly
observed in patients receiving chronic oral therapy.
Voriconazole is similar to
itraconazole in its spectrum of action, having excellent activity against
Candida sp (including fluconazole-resistant species such as C krusei)
and the dimorphic fungi. Voriconazole is less toxic than amphotericin B
and is the treatment of choice for invasive aspergillosis.
Posaconazole
Posaconazole is the newest
triazole to be licensed in the USA. It is available only in a liquid oral
formulation and is used at a dosage of 800 mg/d, divided into two or
three doses. Absorption is improved when taken with meals high in fat.
Posaconazole is rapidly distributed to the tissues, resulting in high
tissue levels but relatively low blood levels. Visual changes have not
been reported, but drug interactions with increased levels of CYP3A4
substrates such as tacrolimus and cyclosporine have been documented.
Posaconazole is the broadest
spectrum member of the azole family, with activity against most species
of candida and aspergillus. It is the only azole with significant
activity against the agents of zygomycosis and mucormycosis. It is
currently licensed for salvage therapy in invasive aspergillosis, as well
as prophylaxis of fungal infections during induction chemotherapy for
leukemia, and for allogeneic bone marrow transplant patients with
graft-versus-host disease.
Echinocandins
Echinocandins are the newest
class of antifungal agents to be developed. They are large cyclic
peptides linked to a long-chain fatty acid. Caspofungin, micafungin,
and anidulafungin are the only licensed agents in this
category of antifungals, although other drugs are under active
investigation. These agents are active against candida and aspergillus,
but not C neoformans or the agents of zygomycosis and
mucormycosis.
Pharmacokinetics
Echinocandins are available only
in intravenous formulations. Caspofungin is administered as a single
loading dose of 70 mg, followed by a daily dose of 50 mg. Caspofungin is
water-soluble and highly protein-bound. The half-life is 9–11 hours, and
the metabolites are excreted by the kidneys and gastrointestinal tract.
Dosage adjustments are required only in the presence of severe hepatic
insufficiency. Micafungin displays similar properties with a half-life of
11–15 hours and is used at a dose of 150 mg/d for treatment of candida
esophagitis, 100 mg/d for treatment of candidemia, and 50 mg/d for
prophylaxis of fungal infections. Anidulafungin has a half-life of 24–48
hours. For esophageal candidiasis, it is administered intravenously at
100 mg on the first day and 50 mg/d thereafter for 14 days. For
candidemia, a loading dose of 200 mg is recommended with 100 mg/d
thereafter for at least 14 days after the last positive blood culture.
Mechanism of Action
Echinocandins act at the level
of the fungal cell wall by inhibiting the synthesis of  (1–3)-glucan
(Figure 48–1). This results in disruption of the fungal cell wall and
cell death.
Adverse Effects
Echinocandin agents are
extremely well tolerated, with minor gastrointestinal side effects and
flushing reported infrequently. Elevated liver enzymes have been noted in
several patients receiving caspofungin in combination with cyclosporine,
and this combination should be avoided. Micafungin has been shown to
increase levels of nifedipine, cyclosporine, and sirolimus. Anidulafungin
does not seem to have significant drug interactions, but histamine
release may occur during intravenous infusion.
Clinical Use
Caspofungin is currently
licensed for disseminated and mucocutaneous candida infections, as well
as for empiric antifungal therapy during febrile neutropenia and has
largely replaced amphotericin B for the latter indication. Note that
caspofungin is licensed for use in invasive aspergillosis only as salvage
therapy in patients who have failed to respond to amphotericin B, and not
as primary therapy. Micafungin is licensed for mucocutaneous candidiasis,
candidemia, and prophylaxis of candida infections in bone marrow
transplant patients. Anidulafungin is approved for use in esophageal
candidiasis and invasive candidiasis, including candidemia.
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