To reduce the development of drug-resistant bacteria and maintain the effectiveness of ZYVOX formulations and other antibacterial drugs, ZYVOX should be used only to treat or prevent infections that are proven or strongly suspected to be caused by bacteria.
DESCRIPTION
ZYVOX I.V. Injection, ZYVOX Tablets, and ZYVOX for Oral Suspension contain linezolid, which is a synthetic antibacterial agent of the oxazolidinone class. The chemical name for linezolid is (S)-N-[[3-[3-Fluoro-4-(4-morpholinyl)phenyl]-2-oxo-5-oxazolidinyl]methyl]-acetamide.
The empirical formula is C 16 H 20 FN 3 O 4 . Its molecular weight is 337.35, and its chemical structure is represented below:
ZYVOX I.V. Injection is supplied as a ready-to-use sterile isotonic solution for intravenous infusion. Each mL contains 2 mg of linezolid. Inactive ingredients are sodium citrate, citric acid, and dextrose in an aqueous vehicle for intravenous administration. The sodium (Na + ) content is 0.38 mg/mL (5 mEq per 300-mL bag; 3.3 mEq per 200-mL bag; and 1.7 mEq per 100-mL bag).
ZYVOX Tablets for oral administration contain 400 mg or 600 mg linezolid as film-coated compressed tablets. Inactive ingredients are corn starch, microcrystalline cellulose, hydroxypropylcellulose, sodium starch glycolate, magnesium stearate, hypromellose, polyethylene glycol, titanium dioxide, and carnauba wax. The sodium (Na + ) content is 1.95 mg per 400-mg tablet and 2.92 mg per 600-mg tablet (0.1 mEq per tablet, regardless of strength).
ZYVOX for Oral Suspension is supplied as an orange-flavored granule/powder for constitution into a suspension for oral administration. Following constitution, each 5 mL contains 100 mg of linezolid. Inactive ingredients are sucrose, citric acid, sodium citrate, microcrystalline cellulose and carboxymethylcellulose sodium, aspartame, xanthan gum, mannitol, sodium benzoate, colloidal silicon dioxide, sodium chloride, and flavors (see PRECAUTIONS , Information for Patients ). The sodium (Na + ) content is 8.52 mg per 5 mL (0.4 mEq per 5 mL).
CLINICAL PHARMACOLOGY
Pharmacokinetics
The mean pharmacokinetic parameters of linezolid in adults after single and multiple oral and intravenous (IV) doses are summarized in Table 1. Plasma concentrations of linezolid at steady-state after oral doses of 600 mg given every 12 hours (q12h) are shown in Figure 1.
Table 1. Mean (Standard Deviation) Pharmacokinetic Parameters of Linezolid in Adults
|
Dose of Linezolid
|
C max
µg/mL |
C min
µg/mL |
T max
hrs |
AUC *
µg · h/mL |
t 1/2
hrs |
CL
mL/min |
|
400 mg tablet
|
|
single dose **/*
|
8.10
(1.83) |
-- |
1.52
(1.01) |
55.10
(25.00) |
5.20
(1.50) |
146
(67) |
|
every 12 hours
|
11.00
(4.37) |
3.08
(2.25) |
1.12
(0.47) |
73.40
(33.50) |
4.69
(1.70) |
110
(49) |
|
600 mg tablet
|
|
single dose
|
12.70
(3.96) |
-- |
1.28
(0.66) |
91.40
(39.30) |
4.26
(1.65) |
127
(48) |
|
every 12 hours
|
21.20
(5.78) |
6.15
(2.94) |
1.03
(0.62) |
138.00
(42.10) |
5.40
(2.06) |
80
(29) |
|
600 mg IV injection &
|
|
single dose
|
12.90
(1.60) |
-- |
0.50
(0.10) |
80.20
(33.30) |
4.40
(2.40) |
138
(39) |
|
every 12 hours
|
15.10
(2.52) |
3.68
(2.36) |
0.51
(0.03) |
89.70
(31.00) |
4.80
(1.70) |
123
(40) |
|
600 mg oral suspension
|
|
single dose
|
11.00
(2.76) |
-- |
0.97
(0.88) |
80.80
(35.10) |
4.60
(1.71) |
141
(45) |
|
*AUC for single dose = AUC 0-(infinity) ; for multiple-dose = AUC 0-[tgr ]
|
|
**/* Data dose-normalized from 375 mg
|
|
& Data dose-normalized from 625 mg, IV dose was given as 0.5-hour infusion.
|
|
C max = Maximum plasma concentration; C min = Minimum plasma concentration; T max = Time to C max ;
AUC = Area under concentration-time curve; t 1/2 = Elimination half-life; CL = Systemic clearance
|
|
Absorption: Linezolid is rapidly and extensively absorbed after oral dosing. Maximum plasma concentrations are reached approximately 1 to 2 hours after dosing, and the absolute bioavailability is approximately 100%. Therefore, linezolid may be given orally or intravenously without dose adjustment.
Linezolid may be administered without regard to the timing of meals. The time to reach the maximum concentration is delayed from 1.5 hours to 2.2 hours and C max is decreased by about 17% when high fat food is given with linezolid. However, the total exposure measured as AUC 0-(infinity) values is similar under both conditions.
Distribution: Animal and human pharmacokinetic studies have demonstrated that linezolid readily distributes to well-perfused tissues. The plasma protein binding of linezolid is approximately 31% and is concentration-independent. The volume of distribution of linezolid at steady-state averaged 40 to 50 liters in healthy adult volunteers.
Linezolid concentrations have been determined in various fluids from a limited number of subjects in Phase 1 volunteer studies following multiple dosing of linezolid. The ratio of linezolid in saliva relative to plasma was 1.2 to 1 and for sweat relative to plasma was 0.55 to 1.
Metabolism: Linezolid is primarily metabolized by oxidation of the morpholine ring, which results in two inactive ring-opened carboxylic acid metabolites: the aminoethoxyacetic acid metabolite (A), and the hydroxyethyl glycine metabolite (B). Formation of metabolite B is mediated by a non-enzymatic chemical oxidation mechanism in vitro. Linezolid is not an inducer of cytochrome P450 (CYP) in rats, and it has been demonstrated from in vitro studies that linezolid is not detectably metabolized by human cytochrome P450 and it does not inhibit the activities of clinically significant human CYP isoforms (1A2, 2C9, 2C19, 2D6, 2E1, 3A4).
Excretion: Nonrenal clearance accounts for approximately 65% of the total clearance of linezolid. Under steady-state conditions, approximately 30% of the dose appears in the urine as linezolid, 40% as metabolite B, and 10% as metabolite A. The renal clearance of linezolid is low (average 40 mL/min) and suggests net tubular reabsorption. Virtually no linezolid appears in the feces, while approximately 6% of the dose appears in the feces as metabolite B, and 3% as metabolite A.
A small degree of nonlinearity in clearance was observed with increasing doses of linezolid, which appears to be due to lower renal and nonrenal clearance of linezolid at higher concentrations. However, the difference in clearance was small and was not reflected in the apparent elimination half-life.
Special Populations
Geriatric: The pharmacokinetics of linezolid are not significantly altered in elderly patients (65 years or older). Therefore, dose adjustment for geriatric patients is not necessary.
Pediatric: The pharmacokinetics of linezolid following a single IV dose were investigated in pediatric patients ranging in age from birth through 17 years (including premature and full-term neonates), in healthy adolescent subjects ranging in age from 12 through 17 years, and in pediatric patients ranging in age from 1 week through 12 years. The pharmacokinetic parameters of linezolid are summarized in Table 2 for the pediatric populations studied and healthy adult subjects after administration of single IV doses.
The C max and the volume of distribution (V ss ) of linezolid are similar regardless of age in pediatric patients. However, clearance of linezolid varies as a function of age. With the exclusion of pre-term neonates less than one week of age, clearance is most rapid in the youngest age groups ranging from >1 week old to 11 years, resulting in lower single-dose systemic exposure (AUC) and shorter half-life as compared with adults. As age of pediatric patients increases, the clearance of linezolid gradually decreases, and by adolescence mean clearance values approach those observed for the adult population. There is wider inter-subject variability in linezolid clearance and systemic drug exposure (AUC) across all pediatric age groups as compared with adults.
Similar mean daily AUC values were observed in pediatric patients from birth to 11 years of age dosed every 8 hours (q8h) relative to adolescents or adults dosed every 12 hours (q12h). Therefore, the dosage for pediatric patients up to 11 years of age should be 10 mg/kg q8h. Pediatric patients 12 years and older should receive 600 mg q12h (see DOSAGE AND ADMINISTRATION ).
Table 2. Pharmacokinetic Parameters of Linezolid in Pediatrics and Adults Following a Single
Intravenous Infusion of 10 mg/kg or 600 mg Linezolid (Mean: (%CV); [Min, Max Values])
|
Age Group
|
C max
µg/mL |
V ss
L/kg |
AUC *
µg·h/mL |
t 1/2
hrs |
CL
mL/min/kg |
|
Neonatal Patients
Pre-term **
< 1 week (N=9) **/*
|
12.7 (30%)
[9.6, 22.2] |
0.81 (24%)
[0.43, 1.05] |
108 (47%)
[41, 191] |
5.6 (46%)
[2.4, 9.8] |
2.0 (52%)
[0.9, 4.0] |
|
Full-term ***
< 1 week (N=10) **/*
|
11.5 (24%)
[8.0, 18.3] |
0.78 (20%)
[0.45, 0.96] |
55 (47%)
[19, 103] |
3.0 (55%)
[1.3, 6.1] |
3.8 (55%)
[1.5, 8.8] |
|
Full-term ***
>/= 1 week to </= 28 days
(N=10) **/*
|
12.9 (28%)
[7.7, 21.6] |
0.66 (29%)
[0.35, 1.06] |
34 (21%)
[23, 50] |
1.5 (17%)
[1.2, 1.9] |
5.1 (22%)
[3.3, 7.2] |
|
Infant Patients
> 28 days to < 3 Months
(N=12) **/*
|
11.0 (27%)
[7.2, 18.0] |
0.79 (26%)
[0.42, 1.08] |
33 (26%)
[17, 48] |
1.8 (28%)
[1.2, 2.8] |
5.4 (32%)
[3.5, 9.9] |
|
Pediatric Patients
3 months through 11 years **/*
(N=59)
|
15.1 (30%)
[6.8, 36.7] |
0.69 (28%)
[0.31, 1.50] |
58 (54%)
[19, 153] |
2.9 (53%)
[0.9, 8.0] |
3.8 (53%)
[1.0, 8.5] |
|
Adolescent Subjects and Patients
12 through 17 years &
(N=36)
|
16.7 (24%)
[9.9, 28.9] |
0.61 (15%)
[0.44, 0.79] |
95 (44%)
[32, 178] |
4.1 (46%)
[1.3, 8.1] |
2.1 (53%)
[0.9, 5.2] |
|
Adult Subjects §
(N=29)
|
12.5 (21%)
[8.2, 19.3] |
0.65 (16%)
[0.45, 0.84] |
91 (33%)
[53, 155] |
4.9 (35%)
[1.8, 8.3] |
1.7 (34%)
[0.9, 3.3] |
|
*AUC = Single dose AUC 0-(infinity)
|
|
**In this data set, "pre-term" is defined as <34 weeks gestational age (Note: Only 1 patient enrolled was pre-term with a postnatal age between 1 week and 28 days)
|
|
***In this data set, "full-term" is defined as >/=34 weeks gestational age
|
|
**/* Dose of 10 mg/kg
|
|
& Dose of 600 mg or 10 mg/kg up to a maximum of 600 mg
|
|
§ Dose normalized to 600 mg
|
|
C max = Maximum plasma concentration; V ss =Volume of distribution; AUC = Area under concentration-time curve; t 1/2 = Apparent elimination half-life; CL = Systemic clearance normalized for body weight
|
|
Gender: Females have a slightly lower volume of distribution of linezolid than males. Plasma concentrations are higher in females than in males, which is partly due to body weight differences. After a 600-mg dose, mean oral clearance is approximately 38% lower in females than in males. However, there are no significant gender differences in mean apparent elimination-rate constant or half-life. Thus, drug exposure in females is not expected to substantially increase beyond levels known to be well tolerated. Therefore, dose adjustment by gender does not appear to be necessary.
Renal Insufficiency: The pharmacokinetics of the parent drug, linezolid, are not altered in patients with any degree of renal insufficiency; however, the two primary metabolites of linezolid may accumulate in patients with renal insufficiency, with the amount of accumulation increasing with the severity of renal dysfunction (see Table 3). The clinical significance of accumulation of these two metabolites has not been determined in patients with severe renal insufficiency. Because similar plasma concentrations of linezolid are achieved regardless of renal function, no dose adjustment is recommended for patients with renal insufficiency. However, given the absence of information on the clinical significance of accumulation of the primary metabolites, use of linezolid in patients with renal insufficiency should be weighed against the potential risks of accumulation of these metabolites. Both linezolid and the two metabolites are eliminated by dialysis. No information is available on the effect of peritoneal dialysis on the pharmacokinetics of linezolid. Approximately 30% of a dose was eliminated in a 3-hour dialysis session beginning 3 hours after the dose of linezolid was administered; therefore, linezolid should be given after hemodialysis.
Table 3. Mean (Standard Deviation) AUCs and Elimination Half-lives of Linezolid and Metabolites A and B in Patients with Varying Degrees of Renal Insufficiency
After a Single 600-mg Oral Dose of Linezolid
|
Parameter
|
Healthy
Subjects
CL CR > 80
mL/min |
Moderate Renal
Impairment
30 < CL CR
< 80 mL/min |
Severe Renal
Impairment
10 < CL CR
< 30 mL/min |
Hemodialysis-Dependent |
|
Off Dialysis * |
On Dialysis |
|
Linezolid
|
|
AUC 0-(infinity) , µg h/mL
|
110 (22) |
128 (53) |
127 (66) |
141 (45) |
83 (23) |
|
t 1/2 , hours
|
6.4 (2.2) |
6.1 (1.7) |
7.1 (3.7) |
8.4 (2.7) |
7.0 (1.8) |
|
Metabolite A
|
|
AUC 0-48 , µg h/mL
|
7.6 (1.9) |
11.7 (4.3) |
56.5 (30.6) |
185 (124) |
68.8 (23.9) |
|
t 1/2 , hours
|
6.3 (2.1) |
6.6 (2.3) |
9.0 (4.6) |
NA |
NA |
|
Metabolite B
|
|
AUC 0-48 , µg h/mL
|
30.5 (6.2) |
51.1 (38.5) |
203 (92) |
467 (102) |
239 (44) |
|
t 1/2 , hours
|
6.6 (2.7) |
9.9 (7.4) |
11.0 (3.9) |
NA |
NA |
|
* between hemodialysis sessions
|
|
NA = Not applicable
|
|
Hepatic Insufficiency: The pharmacokinetics of linezolid are not altered in patients (n=7) with mild-to-moderate hepatic insufficiency (Child-Pugh class A or B). On the basis of the available information, no dose adjustment is recommended for patients with mild-to-moderate hepatic insufficiency. The pharmacokinetics of linezolid in patients with severe hepatic insufficiency have not been eva luated.
Drug-Drug Interactions
Drugs Metabolized by Cytochrome P450: Linezolid is not an inducer of cytochrome P450 (CYP) in rats. It is not detectably metabolized by human cytochrome P450 and it does not inhibit the activities of clinically significant human CYP isoforms (1A2, 2C9, 2C19, 2D6, 2E1, 3A4). Therefore, no CYP450-induced drug interactions are expected with linezolid. Concurrent administration of linezolid does not substantially alter the pharmacokinetic characteristics of (S)-warfarin, which is extensively metabolized by CYP2C9. Drugs such as warfarin and phenytoin, which are CYP2C9 substrates, may be given with linezolid without changes in dosage regimen.
Antibiotics:
Aztreonam: The pharmacokinetics of linezolid or aztreonam are not altered when administered together.
Gentamicin: The pharmacokinetics of linezolid or gentamicin are not altered when administered together.
Monoamine Oxidase Inhibition: Linezolid is a reversible, nonselective inhibitor of monoamine oxidase. Therefore, linezolid has the potential for interaction with adrenergic and serotonergic agents.
Adrenergic Agents: A significant pressor response has been observed in normal adult subjects receiving linezolid and tyramine doses of more than 100 mg. Therefore, patients receiving linezolid need to avoid consuming large amounts of foods or beverages with high tyramine content (see PRECAUTIONS , Information for Patients ).
A reversible enhancement of the pressor response of either pseudoephedrine HCl (PSE) or phenylpropanolamine HCl (PPA) is observed when linezolid is administered to healthy normotensive subjects (see PRECAUTIONS , Drug Interactions ). A similar study has not been conducted in hypertensive patients. The interaction studies conducted in normotensive subjects eva luated the blood pressure and heart rate effects of placebo, PPA or PSE alone, linezolid alone, and the combination of steady-state linezolid (600 mg q12h for 3 days) with two doses of PPA (25 mg) or PSE (60 mg) given 4 hours apart. Heart rate was not affected by any of the treatments. Blood pressure was increased with both combination treatments. Maximum blood pressure levels were seen 2 to 3 hours after the second dose of PPA or PSE, and returned to baseline 2 to 3 hours after peak. The results of the PPA study follow, showing the mean (and range) maximum systolic blood pressure in mm Hg: placebo = 121 (103 to 158); linezolid alone = 120 (107 to 135); PPA alone = 125 (106 to 139); PPA with linezolid = 147 (129 to 176). The results from the PSE study were similar to those in the PPA study. The mean maximum increase in systolic blood pressure over baseline was 32 mm Hg (range: 20-52 mm Hg) and 38 mm Hg (range: 18-79 mm Hg) during co-administration of linezolid with pseudoephedrine or phenylpropanolamine, respectively.
Serotonergic Agents: The potential drug-drug interaction with dextromethorphan was studied in healthy volunteers. Subjects were administered dextromethorphan (two 20-mg doses given 4 hours apart) with or without linezolid. No serotonin syndrome effects (confusion, delirium, restlessness, tremors, blushing, diaphoresis, hyperpyrexia) have been observed in normal subjects receiving linezolid and dextromethorphan.
MICROBIOLOGY
Linezolid is a synthetic antibacterial agent of a new class of antibiotics, the oxazolidinones, which has clinical utility in the treatment of infections caused by aerobic Gram-positive bacteria. The in vitro spectrum of activity of linezolid also includes certain Gram-negative bacteria and anaerobic bacteria. Linezolid inhibits bacterial protein synthesis through a mechanism of action different from that of other antibacterial agents; therefore, cross-resistance between linezolid and other classes of antibiotics is unlikely. Linezolid binds to a site on the bacterial 23S ribosomal RNA of the 50S subunit and prevents the formation of a functional 70S initiation complex, which is an essential component of the bacterial translation process. The results of time-kill studies have shown linezolid to be bacteriostatic against enterococci and staphylococci. For streptococci, linezolid was found to be bactericidal for the majority of strains.
In clinical trials, resistance to linezolid developed in 6 patients infected with Enterococcus faecium (4 patients received 200 mg q12h, lower than the recommended dose, and 2 patients received 600 mg q12h). In a compassionate use program, resistance to linezolid developed in 8 patients with E. faecium and in 1 patient with Enterococcus faecalis. All patients had either unremoved prosthetic devices or undrained abscesses. Resistance to linezolid occurs in vitro at a frequency of 1 × 10 -9 to 1 × 10 -11 . In vitro studies have shown that point mutations in the 23S rRNA are associated with linezolid resistance. Reports of vancomycin-resistant E. faecium becoming resistant to linezolid during its clinical use have been published. 1 In one report nosocomial spread of vancomycin- and linezolid-resistant E. faecium occurred 2 . There has been a report of Staphylococcus aureus (methicillin-resistant) developing resistance to linezolid during its clinical use. 3 The linezolid resistance in these organisms was associated with a point mutation in the 23S rRNA (substitution of thymine for guanine at position 2576) of the organism. When antibiotic-resistant organisms are encountered in the hospital, it is important to emphasize infection control policies. 4,5 Resistance to linezolid has not been reported in Streptococcus spp., including Streptococcus pneumoniae.
In vitro studies have demonstrated additivity or indifference between linezolid and vancomycin, gentamicin, rifampin, imipenem-cilastatin, aztreonam, ampicillin, or streptomycin.
Linezolid has been shown to be active against most isolates of the following microorganisms, both in vitro and in clinical infections, as described in the INDICATIONS AND USAGE section.
Aerobic and facultative Gram-positive microorganisms
Enterococcus faecium (vancomycin-resistant strains only)
Staphylococcus aureus (including methicillin-resistant strains)
Streptococcus agalactiae
Streptococcus pneumoniae (including multi-drug resistant isolates [MDRSP] * )
Streptococcus pyogenes
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