Generic name: levaquin
Availability: Prescription only
Pregnancy & Lactation: Risk data available
Brand names: Levaquin, Levaquin (injection), Levofloxacin, Levofloxacin (injection)
What is Levofloxacin (systemic) (monograph)?
Warning
- Serious Adverse Effects
-
Fluoroquinolones, including levofloxacin, have been associated with disabling and potentially irreversible serious adverse reactions (e.g., tendinitis and tendon rupture, peripheral neuropathy, CNS effects) that have occurred together. Discontinue immediately and avoid use of fluoroquinolones, including levofloxacin, in patients who have experienced any of these serious adverse reactions. (See Warnings under Cautions.)
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Fluoroquinolones, including levofloxacin, may exacerbate muscle weakness in patients with myasthenia gravis. Avoid in patients with known history of myasthenia gravis.
-
Because of risk of serious adverse reactions, use levofloxacin for treatment of acute bacterial sinusitis, acute bacterial exacerbations of chronic bronchitis, or uncomplicated urinary tract infections (UTIs) only when no other treatment options available.
Introduction
Antibacterial; fluoroquinolone.
Uses for levoFLOXacin (Systemic)
Respiratory Tract Infections
Treatment of acute bacterial sinusitis caused by susceptible Streptococcus pneumoniae, Haemophilus influenzae, or Moraxella catarrhalis.
Treatment of acute bacterial exacerbations of chronic bronchitis caused by susceptible Staphylococcus aureus, S. pneumoniae, H. influenzae, H. parainfluenzae, or M. catarrhalis.
Use for treatment of acute bacterial sinusitis or acute bacterial exacerbations of chronic bronchitis only when no other treatment options available. Because systemic fluoroquinolones, including levofloxacin, have been associated with disabling and potentially irreversible serious adverse reactions (e.g., tendinitis and tendon rupture, peripheral neuropathy, CNS effects) that can occur together in the same patient (see Cautions) and because acute bacterial sinusitis and acute bacterial exacerbations of chronic bronchitis may be self-limiting in some patients, risks of serious adverse reactions outweigh benefits of fluoroquinolones for patients with these infections.
Treatment of community-acquired pneumonia (CAP) caused by susceptible S. aureus, S. pneumoniae (including multidrug-resistant S. pneumoniae [MDRSP]), H. influenzae, H. parainfluenzae, Klebsiella pneumoniae, Legionella pneumoniae, M. catarrhalis, Chlamydophila pneumoniae (formerly Chlamydia pneumoniae), or Mycoplasma pneumoniae. Select regimen for empiric treatment of CAP based on most likely pathogens and local susceptibility patterns; after pathogen is identified, modify to provide more specific therapy (pathogen-directed therapy).
Treatment of nosocomial pneumonia caused by susceptible S. aureus (oxacillin-susceptible [methicillin-susceptible] strains only), S. pneumoniae, H. influenzae, Escherichia coli, K. pneumoniae, Pseudomonas aeruginosa, or Serratia marcescens. Use adjunctive therapy as clinically indicated; if Ps. aeruginosa known or suspected to be involved, concomitant use of an antipseudomonal β-lactam recommended. Select regimen for empiric treatment of hospital-acquired pneumonia (HAP) not associated with mechanical ventilation or ventilator-associated pneumonia (VAP) based on local susceptibility data. If a fluoroquinolone used for initial empiric treatment of HAP or VAP, IDSA and ATS recommend ciprofloxacin or levofloxacin.
Consult current IDSA clinical practice guidelines available at [Web] for additional information on management of respiratory tract infections.
Skin and Skin Structure Infections
Treatment of mild to moderate uncomplicated skin and skin structure infections (including abscesses, cellulitis, furuncles, impetigo, pyoderma, wound infections) caused by susceptible S. aureus or S. pyogenes (group A β-hemolytic streptococci.
Treatment of complicated skin and skin structure infections caused by susceptible S. aureus (oxacillin-susceptible [methicillin-susceptible] strains only), Enterococcus faecalis, S. pyogenes, or Proteus mirabilis.
Consult current IDSA clinical practice guidelines available at [Web] for additional information on management of skin and skin structure infections.
Urinary Tract Infections (UTIs) and Prostatitis
Treatment of mild to moderate uncomplicated UTIs caused by susceptible E. coli, K. pneumoniae, or S. saprophyticus.
Use for treatment of uncomplicated UTIs only when no other treatment options available. Because systemic fluoroquinolones, including levofloxacin, have been associated with disabling and potentially irreversible serious adverse reactions (e.g., tendinitis and tendon rupture, peripheral neuropathy, CNS effects) that can occur together in the same patient(see Cautions) and because uncomplicated UTIs may be self-limiting in some patients, risks of serious adverse reactions outweigh benefits of fluoroquinolones for patients with uncomplicated UTIs.
Treatment of mild to moderate complicated UTIs caused by susceptible E. faecalis, Enterobacter cloacae, E. coli, K. pneumoniae, P. mirabilis, or P. aeruginosa.
Treatment of acute pyelonephritis caused by susceptible E. coli, including cases with concurrent bacteremia.
Treatment of chronic prostatitis caused by susceptible E. coli, E. faecalis, or S. epidermidis.
Endocarditis
Alternative for treatment of endocarditis† [off-label] (native or prosthetic valve or other prosthetic material) caused by fastidious gram-negative bacilli known as the HACEK group (Haemophilus, Aggregatibacter, Cardiobacterium hominis, Eikenella corrodens, Kingella). AHA and IDSA recommend ceftriaxone (or other third or fourth generation cephalosporin), but state that a fluoroquinolone (ciprofloxacin, levofloxacin, moxifloxacin) may be considered in patients who cannot tolerate cephalosporins. Consultation with an infectious disease specialist recommended.
GI Infections
Alternative for treatment of campylobacteriosis† [off-label] caused by susceptible Campylobacter. Optimal treatment of campylobacteriosis in HIV-infected patients not identified. Some clinicians withhold anti-infective treatment in those with CD4+ T-cells >200 cells/mm3 and only mild campylobacteriosis and initiate treatment if symptoms persist for more than several days. In those with mild to moderate campylobacteriosis, treatment with a fluoroquinolone (preferably ciprofloxacin or, alternatively, levofloxacin or moxifloxacin) or azithromycin is reasonable. Modify anti-infective therapy based on results of in vitro susceptibility testing; resistance to fluoroquinolones reported in 22% of C. jejuni and 35% of C. coli isolates tested in US.
Treatment of Salmonella gastroenteritis† [off-label]. CDC, NIH, and HIV Medicine Association of IDSA recommend ciprofloxacin as initial drug of choice for treatment of Salmonella gastroenteritis (with or without bacteremia) in HIV-infected adults; other fluoroquinolones (levofloxacin, moxifloxacin) also likely to be effective, but data limited. Depending on in vitro susceptibility, alternatives are co-trimoxazole and third generation cephalosporins (ceftriaxone, cefotaxime). Role of long-term anti-infective treatment (secondary prophylaxis) against Salmonella in HIV-infected individuals with recurrent bacteremia not well established; weigh benefits of such prophylaxis against risks of long-term anti-infective therapy.
Treatment of shigellosis† [off-label] caused by susceptible Shigella. Anti-infectives may not be required for mild infections, but generally indicated in addition to fluid and electrolyte replacement for treatment of patients with severe shigellosis, dysentery, or underlying immunosuppression. Empiric treatment regimen can be used initially, but in vitro susceptibility testing indicated since resistance is common. Fluoroquinolones (preferably ciprofloxacin or, alternatively, levofloxacin or moxifloxacin) have been recommended for treatment of shigellosis in HIV-infected adults, but consider that fluoroquinolone-resistant Shigella reported in the US, especially in international travelers, the homeless, and men who have sex with men (MSM). Depending on in vitro susceptibility, other drugs recommended for treatment of shigellosis include co-trimoxazole, ceftriaxone, azithromycin (not recommended in those with bacteremia), or ampicillin.
Treatment of travelers’ diarrhea† [off-label]. If caused by bacteria, may be self-limited and often resolves within 3–7 days without anti-infective treatment. CDC states anti-infective treatment not recommended for mild travelers' diarrhea; CDC and others state empiric short-term anti-infective treatment (single dose or up to 3 days) may be used if diarrhea is moderate or severe, associated with fever or bloody stools, or extremely disruptive to travel plans. Fluoroquinolones (ciprofloxacin, levofloxacin) generally have been considered drugs of choice for empiric treatment, including self-treatment; alternatives include azithromycin and rifaximin. Consider that increasing incidence of enteric bacteria resistant to fluoroquinolones and other anti-infectives may limit usefulness of empiric treatment in individuals traveling in certain geographic areas; also consider possible adverse effects of the anti-infective and adverse consequences of such treatment (e.g., development of resistance, effect on normal gut microflora).
Prevention of travelers’ diarrhea† in individuals traveling for relatively short periods to areas of risk. CDC and others do not recommend anti-infective prophylaxis in most travelers. May consider prophylaxis in short-term travelers who are high-risk individuals (e.g., HIV-infected or other immunocompromised individuals, travelers with poorly controlled diabetes mellitus or chronic renal failure) and those taking critical trips during which even a short episode of diarrhea could adversely affect purpose of trip. If anti-infective prophylaxis used, fluoroquinolones (ciprofloxacin, levofloxacin) usually have been recommended; alternatives include azithromycin and rifaximin. Weigh use of anti-infective prophylaxis against use of prompt, early self-treatment with an empiric anti-infective if moderate to severe travelers' diarrhea occurs. Also consider increasing incidence of fluoroquinolone resistance in pathogens that cause travelers’ diarrhea (e.g., Campylobacter, Salmonella, Shigella).
Has been used as a component of various multiple-drug regimens for treatment of infections caused by Helicobacter pylori†. Data are limited regarding prevalence of fluoroquinolone-resistant H. pylori in the US; possible impact of such resistance on efficacy of fluoroquinolone-containing regimens used for treatment of H. pylori infections not known.
Anthrax
Inhalational anthrax (postexposure) to reduce incidence or progression of disease following suspected or confirmed exposure to aerosolized Bacillus anthracis spores. CDC, AAP, US Working Group on Civilian Biodefense, and US Army Medical Research Institute of Infectious Diseases (USAMRIID) recommend oral ciprofloxacin and oral doxycycline as initial drugs of choice for prophylaxis following such exposures, including exposures that occur in the context of biologic warfare or bioterrorism. Other oral fluoroquinolones (levofloxacin, moxifloxacin, ofloxacin) are alternatives for postexposure prophylaxis when ciprofloxacin or doxycycline cannot be used.
Treatment of uncomplicated cutaneous anthrax† (without systemic involvement) that occurs in the context of biologic warfare or bioterrorism. CDC states that preferred drugs for such infections include oral ciprofloxacin, doxycycline, levofloxacin, or moxifloxacin.
Alternative to ciprofloxacin for use in multiple-drug parenteral regimens for initial treatment of systemic anthrax† (inhalational, GI, meningitis, or cutaneous with systemic involvement, head or neck lesions, or extensive edema) that occurs in the context of biologic warfare or bioterrorism. For initial treatment of systemic anthrax with possible or confirmed meningitis, CDC and AAP recommend a regimen of IV ciprofloxacin in conjunction with another IV bactericidal anti-infective (preferably meropenem) and an IV protein synthesis inhibitor (preferably linezolid). If meningitis excluded, these experts recommend an initial regimen of IV ciprofloxacin in conjunction with an IV protein synthesis inhibitor (preferably clindamycin or linezolid).
Has been suggested as possible alternative to ciprofloxacin for treatment of inhalational anthrax† when a parenteral regimen not available (e.g., supply or logistic problems because large numbers of individuals require treatment in a mass-casualty setting).
Chlamydial Infections
Alternative for treatment of urogenital infections caused by Chlamydia trachomatis†. CDC recommends azithromycin or doxycycline; alternatives are erythromycin, levofloxacin, or ofloxacin.
Gonorrhea and Associated Infections
Was used in the past for treatment of uncomplicated gonorrhea† caused by susceptible Neisseria gonorrhoeae.
Because quinolone-resistant N. gonorrhoeae (QRNG) widely disseminated worldwide, including in the US, CDC states fluoroquinolones no longer recommended for treatment of gonorrhea and should not be used routinely for any associated infections that may involve N. gonorrhoeae (e.g., pelvic inflammatory disease [PID], epididymitis).
Alternative for treatment of PID†. (See Pelvic Inflammatory Disease under Uses.)
Alternative for treatment of acute epididymitis†. CDC recommends a single IM dose of ceftriaxone in conjunction with oral doxycycline for acute epididymitis most likely caused by sexually transmitted chlamydia and gonorrhea or a single IM dose of ceftriaxone in conjunction with oral levofloxacin or ofloxacin for treatment of acute epididymitis most likely caused by sexually transmitted chlamydia and gonorrhea and enteric bacteria (e.g., in men who practice insertive anal sex). Levofloxacin or ofloxacin can be used alone if acute epididymitis most likely caused by enteric bacteria (e.g., in men who have undergone prostate biopsy, vasectomy, or other urinary tract instrumentation procedure) and gonorrhea ruled out (e.g., by gram, methylene blue, or gentian violet stain).
Tuberculosis
Alternative (second-line) agent for use in multiple-drug regimens for treatment of active tuberculosis† caused by Mycobacterium tuberculosis.
Although potential role of fluoroquinolones and optimal length of therapy not fully defined, ATS, CDC, IDSA, and others state that use of fluoroquinolones as alternative (second-line) agents can be considered for treatment of active tuberculosis in patients intolerant to certain first-line agents and in those with relapse, treatment failure, or M. tuberculosis resistant to certain first-line agents. If a fluoroquinolone used in multiple-drug regimens for treatment of active tuberculosis, ATS, CDC, IDSA, and others recommend levofloxacin or moxifloxacin.
Consider that fluoroquinolone-resistant M. tuberculosis reported and there are increasing reports of extensively drug-resistant tuberculosis (XDR tuberculosis). XDR tuberculosis is caused by M. tuberculosis resistant to rifampin and isoniazid (multiple-drug resistant strains) that also are resistant to a fluoroquinolone and at least one parenteral second-line antimycobacterial (capreomycin, kanamycin, amikacin).
Consult most recent ATS, CDC, and IDSA recommendations for treatment of tuberculosis for more specific information.
Other Mycobacterial Infections
Has been used in multiple-drug regimens for treatment of disseminated infections caused by M. avium complex† (MAC).
ATS and IDSA state that role of fluoroquinolones in treatment of MAC infections not established. If a fluoroquinolone is included in multiple-drug treatment regimen (e.g., for macrolide-resistant MAC infections), moxifloxacin or levofloxacin may be preferred, although many strains are resistant in vitro.
Consult most recent ATS, CDC, and IDSA recommendations for treatment of other mycobacterial infections for more specific information.
Nongonococcal Urethritis
Alternative for treatment of nongonococcal urethritis† (NGU). CDC recommends azithromycin or doxycycline; alternatives are erythromycin, levofloxacin, or ofloxacin.
Pelvic Inflammatory Disease
Alternative for treatment of acute PID†. Do not use in any infections that may involve N. gonorrhoeae.
When combined IM and oral regimen used for treatment of mild to moderately severe acute PID, CDC recommends a single IM dose of ceftriaxone, cefoxitin (with oral probenecid), or cefotaxime given in conjunction with oral doxycycline (with or without oral metronidazole). If a parenteral cephalosporin not feasible (e.g., because of cephalosporin allergy), CDC states regimen of oral levofloxacin, ofloxacin, or moxifloxacin given in conjunction with oral metronidazole can be considered if community prevalence and individual risk of gonorrhea is low and diagnostic testing for gonorrhea performed. If QRNG are identified or if in vitro susceptibility cannot be determined (e.g., only nucleic acid amplification test [NAAT] for gonorrhea available), consultation with infectious disease specialist recommended.
Plague
Treatment of plague, including pneumonic and septicemic plague, caused by Yersinia pestis. Streptomycin (or gentamicin) historically has been considered regimen of choice for treatment of plague; alternatives are doxycycline (or tetracycline), chloramphenicol (a drug of choice for plague meningitis), fluoroquinolones (ciprofloxacin [a drug of choice for plague meningitis], levofloxacin, moxifloxacin), or co-trimoxazole (may be less effective than other alternatives). Regimens recommended for treatment of naturally occurring or endemic bubonic, septicemic, or pneumonic plague also recommended for plague that occurs following exposure to Y. pestis in the context of biologic warfare or bioterrorism.
Postexposure prophylaxis following high-risk exposure to Y. pestis (e.g., household, hospital, or other close contact with an individual who has pneumonic plague; laboratory exposure to viable Y. pestis; confirmed exposure in the context of biologic warfare or bioterrorism). Drugs of choice for such prophylaxis are doxycycline (or tetracycline) or a fluoroquinolone (ciprofloxacin, levofloxacin, moxifloxacin, ofloxacin).
levoFLOXacin (Systemic) Dosage and Administration
Administration
Administer orally or by slow IV infusion. Do not give IM, sub-Q, intrathecally, or intraperitoneally.
IV route indicated in patients who do not tolerate or are unable to take the drug orally and in other patients when the IV route offers a clinical advantage. Oral and IV routes considered interchangeable because pharmacokinetics are similar.
Patients receiving oral or IV levofloxacin should be well hydrated and instructed to drink fluids liberally to prevent highly concentrated urine and formation of crystals in urine.
Oral Administration
Tablets: Administer without regard to meals. Do not use tablets in pediatric patients weighing <30 kg.
Oral solution: Administer 1 hour before or 2 hours after meals. (See Food under Pharmacokinetics.)
Tablets or oral solution: Administer orally at least 2 hours before or 2 hours after antacids containing magnesium or aluminum, metal cations (e.g., iron), sucralfate, multivitamins or dietary supplements containing iron or zinc, or buffered didanosine (pediatric oral solution admixed with antacid). (See Interactions.)
IV Infusion
Premixed injection for IV infusion containing 5 mg/mL in 5% dextrose (single-use flexible container): Use without further dilution.
Concentrate for injection containing 25 mg/mL (single-use vials): Must be diluted prior to IV infusion.
Do not admix with other drugs or infuse simultaneously through same tubing with other drugs. Do not infuse through same tubing with any solution containing multivalent cations (e.g., magnesium). If same administration set is used for sequential infusion of several different drugs, flush tubing before and after administration using an IV solution compatible with levofloxacin and the other drug(s).
Premixed injection for IV infusion and concentrate for injection for IV infusion contain no preservatives; discard any unused portions.
For solution and drug compatibility information, see Compatibility under Stability.
Dilution
Concentrate for injection containing 25 mg/mL (single-use vials): Dilute with a compatible IV solution prior to IV infusion to provide a solution containing 5 mg/mL.
Rate of Administration
Administer doses of 250 or 500 mg by IV infusion over 60 minutes; administer doses of 750 mg by IV infusion over 90 minutes.
Rapid IV infusion or injection associated with hypotension and must be avoided.
Dosage
Dosage of oral and IV levofloxacin is identical.
Dosage adjustments not needed when switching from IV to oral administration.
Because safety of levofloxacin given for >28 days in adults and >14 days in pediatric patients not studied, manufacturers state use prolonged therapy only when potential benefits outweigh risks.
Pediatric Patients
Anthrax
Postexposure Prophylaxis Following Exposure in the Context of Biologic Warfare or Bioterrorism
Oral or IVPediatric patients as young as 1 month of age†: AAP suggests 8 mg/kg (up to 250 mg) every 12 hours in those weighing <50 kg or 500 mg once daily in those weighing >50 kg.
Children ≥6 months of age weighing <50 kg: Manufacturer recommends 8 mg/kg (up to 250 mg) every 12 hours.
Children ≥6 months of age weighing >50 kg: Manufacturer recommends 500 mg once daily.
Initiate prophylaxis as soon as possible following suspected or confirmed exposure to aerosolized B. anthracis.
Because of possible persistence of B. anthracis spores in lung tissue following an aerosol exposure, CDC, AAP, and others recommend that anti-infective postexposure prophylaxis be continued for 60 days following a confirmed exposure.
Treatment of Uncomplicated Cutaneous Anthrax (Biologic Warfare or Bioterrorism Exposure)†
OralPediatric patients ≥1 month of age†: AAP recommends 8 mg/kg (up to 250 mg) every 12 hours in those weighing <50 kg and 500 mg once daily in those weighing >50 kg.
Recommended duration is 60 days after illness onset if cutaneous anthrax occurred after exposure to aerosolized B. anthracis spores in the context of biologic warfare or bioterrorism.
Treatment of Systemic Anthrax (Biologic Warfare or Bioterrorism Exposure)†
IVPediatric patients ≥1 month of age† with systemic anthrax: 8 mg/kg (up to 250 mg) every 12 hours in those weighing <50 kg or 500 mg once daily in those weighing >50 kg.
Pediatric patients ≥1 month of age† with systemic anthrax if meningitis excluded: 10 mg/kg (up to 250 mg) every 12 hours in those weighing <50 kg or 500 mg once daily in those weighing >50 kg.
Used in multiple-drug parenteral regimen for initial treatment of systemic anthrax (inhalational, GI, meningitis, or cutaneous anthrax with systemic involvement, lesions on the head or neck, or extensive edema). Continue parenteral regimen for ≥2–3 weeks until patient is clinically stable and can be switched to appropriate oral anti-infective.
If systemic anthrax occurred after exposure to aerosolized B. anthracis spores in the context of biologic warfare or bioterrorism, continue oral follow-up regimen until 60 days after illness onset.
OralPediatric patients ≥1 month of age† (follow-up after initial multiple-drug parenteral regimen): 8 mg/kg (up to 250 mg) every 12 hours in those weighing <50 kg or 500 mg once daily in those weighing ≥50 kg.
If systemic anthrax occurred after exposure to aerosolized B. anthracis spores in the context of biologic warfare or bioterrorism, continue oral follow-up regimen until 60 days after illness onset.
Plague
Treatment or Prophylaxis of Plague
Oral or IVChildren ≥6 months of age weighing <50 kg: 8 mg/kg (up to 250 mg) every 12 hours for 10–14 days.
Children ≥6 months of age weighing >50 kg: 500 mg once daily for 10–14 days. Higher dosage (i.e., 750 mg once daily) may be used if clinically indicated.
Initiate as soon as possible after suspected or known exposure to Y. pestis.
Adults
Respiratory Tract Infections
Acute Bacterial Sinusitis
Oral or IV500 mg once every 24 hours for 10–14 days. (See Respiratory Tract Infections under Uses.)
Alternatively, 750 mg once every 24 hours for 5 days.
Acute Bacterial Exacerbations of Chronic Bronchitis
Oral or IV500 mg once every 24 hours for 7 days. (See Respiratory Tract Infections under Uses.)
Community-acquired Pneumonia (CAP)
Oral or IVS. aureus, S. pneumoniae (including MDRSP), K. pneumoniae, L. pneumophila, M. catarrhalis: 500 mg once every 24 hours for 7–14 days.
S. pneumoniae (except MDRSP), H. influenzae, H. parainfluenzae, M. pneumoniae, or C. pneumoniae: 500 mg once every 24 hours for 7–14 days or, alternatively, 750 mg once every 24 hours for 5 days.
If used for empiric treatment of CAP or treatment of CAP caused by Ps. aeruginosa, IDSA and ATS recommend 750 mg once daily.
IDSA and ATS state that CAP should be treated for a minimum of 5 days and patients should be afebrile for 48–72 hours before discontinuing anti-infective therapy.
Nosocomial Pneumonia
Oral or IV750 mg once every 24 hours for 7–14 days.
Skin and Skin Structure Infections
Uncomplicated Infections
Oral or IV500 mg once every 24 hours for 7–10 days.
Complicated Infections
Oral or IV750 mg once every 24 hours for 7–14 days.
Urinary Tract Infections (UTIs) and Prostatitis
Uncomplicated UTIs
Oral or IV250 mg once every 24 hours for 3 days. (See Urinary Tract Infections [UTIs] and Prostatitis under Uses.)
Complicated UTIs
Oral or IVE. faecalis, E. cloacae, or Ps. aeruginosa: 250 mg once every 24 hours for 10 days.
E. coli, K. pneumoniae, or P. mirabilis: 250 mg once every 24 hours for 10 days or, alternatively, 750 mg once every 24 hours for 5 days.
Acute Pyelonephritis
Oral or IVE. coli: 250 mg once every 24 hours or 10 days or, alternatively, 750 mg once every 24 hours for 5 days.
Chronic Prostatitis
Oral or IV500 mg once every 24 hours for 28 days.
GI Infections†
Campylobacter Infections†
Oral or IVHIV-infected: 750 mg once daily.
Recommended treatment duration is 7–10 days for gastroenteritis or ≥14 days for bacteremic infections. Duration of 2–6 weeks recommended for recurrent infections.
Salmonella Gastroenteritis†
Oral or IVHIV-infected: 750 mg once daily.
Recommended treatment duration is 7–14 days if CD4+ T-cells ≥200 cells/mm3 (≥14 days if bacteremic or infection is complicated) or 2–6 weeks if CD4+ T-cells <200 cells/mm3.
Consider secondary prophylaxis in those with recurrent bacteremia; also may consider in those with recurrent gastroenteritis (with or without bacteremia) or with CD4+ T-cells <200 cells/mm3 and severe diarrhea. Discontinue secondary prophylaxis if Salmonella infection resolves and there has been a sustained response to antiretroviral therapy with CD4+ T-cells >200 cells/mm3.
Shigella Infections†
Oral or IVHIV-infected: 750 mg once daily.
Recommended treatment duration is 7–10 days for gastroenteritis or ≥14 days for bacteremic infections. Up to 6 weeks may be required for recurrent infections, especially if CD4+ T-cells <200 cells/mm3.
Treatment of Travelers’ Diarrhea†
Oral500 mg once daily for 1–3 days.
Prevention of Travelers’ Diarrhea†
Oral500 mg once daily.
Anti-infective prophylaxis generally discouraged (see GI Infections under Uses); if such prophylaxis used, give during period of risk (not exceeding 2–3 weeks) beginning day of travel and continuing for 1 or 2 days after leaving area of risk.
Helicobacter pylori Infection
Oral500 mg once daily usually used; 250 mg once daily also has been used.
Used as a component of multiple-drug regimen (see GI Infections under Uses).
Anthrax
Postexposure Prophylaxis of Anthrax (Biologic Warfare or Bioterrorism Exposure)
Oral or IV500 mg once daily recommended by manufacturers.
750 mg once daily recommended by CDC.
Initiate prophylaxis as soon as possible following suspected or confirmed exposure to aerosolized B. anthracis.
Because of possible persistence of B. anthracis spores in lung tissue following an aerosol exposure, CDC and others recommend that anti-infective postexposure prophylaxis be continued for 60 days following a confirmed exposure.
Treatment of Uncomplicated Cutaneous Anthrax (Biologic Warfare or Bioterrorism Exposure)†
Oral750 mg once daily.
Recommended duration is 60 days if cutaneous anthrax occurred after exposure to aerosolized B. anthracis spores in the context of biologic warfare or bioterrorism.
Treatment of Systemic Anthrax (Biologic Warfare or Bioterrorism Exposure)†
IV750 mg once daily.
Used in multiple-drug parenteral regimen for initial treatment of systemic anthrax (inhalational, GI, meningitis, or cutaneous with systemic involvement, lesions on the head or neck, or extensive edema). Continue parenteral regimen for ≥2–3 weeks until patient is clinically stable and can be switched to appropriate oral anti-infective.
If anthrax occurred after exposure to aerosolized B. anthracis spores in the context of biologic warfare or bioterrorism, continue oral follow-up regimen until 60 days after illness onset.
Chlamydial Infections†
Urogenital Infections†
Oral500 mg once daily for 7 days recommended by CDC for infections caused by C. trachomatis.
Gonorrhea and Associated Infections†
Epididymitis†
Oral500 mg once daily for 10 days recommended by CDC.
Use only when epididymitis† most likely caused by sexually transmitted enteric bacteria (e.g., E. coli) and N. gonorrhoeae ruled out. (See Gonorrhea and Associated Infections under Uses.)
Mycobacterial Infections†
Active Tuberculosis†
Oral or IV0.5–1 g once daily. Must be used in conjunction with other antituberculosis agents.
ATS, CDC, and IDSA state data insufficient to date to support intermittent levofloxacin regimens for treatment of tuberculosis.
Disseminated MAC Infections
OralHIV-infected: 500 mg once daily.
Nongonococcal Urethritis†
Oral
500 mg once daily for 7 days recommended by CDC.
Pelvic Inflammatory Disease†
Oral
500 mg once daily for 14 days given in conjunction with oral metronidazole (500 mg twice daily for 14 days).
Use only when cephalosporins not feasible, community prevalence and individual risk of gonorrhea low, and in vitro susceptibility confirmed. (See Pelvic Inflammatory Disease under Uses.)
IV
500 mg once daily; used with or without IV metronidazole (500 mg every 8 hours).
Use only when cephalosporins not feasible, community prevalence and individual risk of gonorrhea are low, and in vitro susceptibility confirmed. (See Pelvic Inflammatory Disease under Uses.)
Plague
Treatment or Prophylaxis of Plague
Oral or IV500 mg once daily for 10–14 days. Higher dosage (i.e., 750 mg once daily) may be used if clinically indicated.
Initiate as soon as possible after suspected or known exposure to Y. pestis.
Special Populations
Hepatic Impairment
Dosage adjustments not required.
Renal Impairment
Adjust dosage in adults with Clcr <50 mL/minute. (See Table 1.) Adjustments not needed when used for treatment of uncomplicated UTIs in patients with renal impairment.
Dosage recommendations not provided by manufacturer for pediatric patients with renal impairment.
Usual Daily Dosage for Normal Renal Function (Clcr ≥ 50 mL/min) |
Clcr (mL/min) |
Dosage for Renal Impairment |
---|---|---|
250 mg |
20–49 |
Dosage adjustment not required |
250 mg |
10–19 |
Uncomplicated UTIs: Dosage adjustment not required. Other infections: 250 mg once every 48 hours |
250 mg |
Hemodialysis or CAPD patients |
Information not available |
500 mg |
20–49 |
Initial 500-mg dose, then 250 mg once every 24 hours |
500 mg |
10–19 |
Initial 500-mg dose, then 250 mg once every 48 hours |
500 mg |
Hemodialysis or CAPD patients |
Initial 500-mg dose, then 250 mg once every 48 hours; supplemental doses not required after dialysis |
750 mg |
20–49 |
750 mg once every 48 hours |
750 mg |
10–19 |
Initial 750-mg dose, then 500 mg once every 48 hours |
750 mg |
Hemodialysis or CAPD patients |
Initial 750-mg dose, then 500 mg once every 48 hours; supplemental doses not required after dialysis |
Geriatric Patients
No dosage adjustments except those related to renal impairment. (See Renal Impairment under Dosage and Administration.)
Warnings
Contraindications
-
Known hypersensitivity to levofloxacin or other quinolones.
Warnings/Precautions
Warnings
Disabling and Potentially Irreversible Serious Adverse Reactions
Systemic fluoroquinolones, including levofloxacin, associated with disabling and potentially irreversible serious adverse reactions (e.g., tendinitis and tendon rupture, peripheral neuropathy, CNS effects) that can occur together in the same patient. May occur within hours to weeks after a systemic fluoroquinolone is initiated; have occurred in all age groups and in patients without preexisting risk factors for such adverse reactions.
Immediately discontinue levofloxacin at first signs or symptoms of any serious adverse reactions.
Avoid systemic fluoroquinolones, including levofloxacin, in patients who have experienced any of the serious adverse reactions associated with fluoroquinolones.
Tendinitis and Tendon Rupture
Systemic fluoroquinolones, including levofloxacin, are associated with an increased risk of tendinitis and tendon rupture in all age groups.
Risk of developing fluoroquinolone-associated tendinitis and tendon rupture is increased in older adults (usually those >60 years of age), individuals receiving concomitant corticosteroids, and kidney, heart, or lung transplant recipients. (See Geriatric Use under Cautions.)
Other factors that may independently increase the risk of tendon rupture include strenuous physical activity, renal failure, and previous tendon disorders such as rheumatoid arthritis. Tendinitis and tendon rupture have been reported in patients receiving fluoroquinolones who did not have any risk factors for such adverse reactions.
Fluoroquinolone-associated tendinitis and tendon rupture most frequently involve the Achilles tendon; also reported in rotator cuff (shoulder), hand, biceps, thumb, and other tendon sites.
Tendinitis and tendon rupture can occur within hours or days after levofloxacin is initiated or as long as several months after completion of therapy and can occur bilaterally.
Immediately discontinue levofloxacin if pain, swelling, inflammation, or rupture of a tendon occurs. (See Advice to Patients.)
Avoid systemic fluoroquinolones, including levofloxacin, in patients who have a history of tendon disorders or have experienced tendinitis or tendon rupture.
Peripheral Neuropathy
Systemic fluoroquinolones, including levofloxacin, are associated with an increased risk of peripheral neuropathy.
Sensory or sensorimotor axonal polyneuropathy affecting small and/or large axons resulting in paresthesias, hypoesthesias, dysesthesias, and weakness reported with systemic fluoroquinolones, including levofloxacin. Symptoms may occur soon after initiation of the drug and, in some patients, may be irreversible.
Immediately discontinue levofloxacin if symptoms of peripheral neuropathy (e.g., pain, burning, tingling, numbness, and/or weakness) occur or if there are other alterations in sensations (e.g., light touch, pain, temperature, position sense, vibratory sensation). (See Advice to Patients.)
Avoid systemic fluoroquinolones, including levofloxacin, in patients who have experienced peripheral neuropathy.
CNS Effects
Systemic fluoroquinolones, including levofloxacin, are associated with increased risk of psychiatric adverse effects, including toxic psychosis, hallucinations, paranoia, depression, suicidal thoughts or acts, anxiety, agitation, restlessness, nervousness, confusion, delirium, disorientation, disturbances in attention, insomnia, nightmares, and memory impairment. Attempted or completed suicides reported, especially in patients with a history of depression or underlying risk factor for depression. These adverse effects may occur after first dose.
Systemic fluoroquinolones, including levofloxacin, are associated with increased risk of seizures (convulsions), increased intracranial pressure (including pseudotumor cerebri), dizziness, and tremors. Use with caution in patients with known or suspected CNS disorders that predispose to seizures or lower the seizure threshold (e.g., severe cerebral arteriosclerosis, epilepsy) or with other risk factors that predispose to seizures or lower the seizure threshold (e.g., certain drugs, renal impairment).
If psychiatric or other CNS effects occur, immediately discontinue levofloxacin and institute appropriate measures. (See Advice to Patients.)
Exacerbation of Myasthenia Gravis
Fluoroquinolones, including levofloxacin, have neuromuscular blocking activity and may exacerbate muscle weakness in myasthenia gravis patients; death or need for ventilatory support reported.
Avoid use in patients with known history of myasthenia gravis. (See Advice to Patients.)
Sensitivity Reactions
Hypersensitivity Reactions
Serious and occasionally fatal hypersensitivity and/or anaphylactic reactions reported in patients receiving fluoroquinolones, including levofloxacin. These reactions often occur with first dose.
Some hypersensitivity reactions have been accompanied by cardiovascular collapse, hypotension or shock, seizures, loss of consciousness, tingling, angioedema (e.g., edema or swelling of the tongue, larynx, throat, or face), airway obstruction (e.g., bronchospasm, shortness of breath, acute respiratory distress), dyspnea, urticaria, pruritus, and other severe skin reactions.
Other serious and sometimes fatal adverse reactions reported with fluoroquinolones, including levofloxacin, that may or may not be related to hypersensitivity reactions include one or more of the following: fever, rash or other severe dermatologic reactions (e.g., toxic epidermal necrolysis, Stevens-Johnson syndrome); vasculitis, arthralgia, myalgia, serum sickness; allergic pneumonitis; interstitial nephritis, acute renal insufficiency or failure; hepatitis, jaundice, acute hepatic necrosis or failure; anemia (including hemolytic and aplastic), thrombocytopenia (including thrombotic thrombocytopenic purpura), leukopenia, agranulocytosis, pancytopenia, and/or other hematologic effects.
Immediately discontinue levofloxacin at first appearance of rash, jaundice, or any other sign of hypersensitivity. Institute appropriate therapy as indicated (e.g., epinephrine, corticosteroids, maintenance of an adequate airway and oxygen).
Photosensitivity Reactions
Moderate to severe photosensitivity/phototoxicity reactions reported with fluoroquinolones, including levofloxacin
Phototoxicity may manifest as exaggerated sunburn reactions (e.g., burning, erythema, exudation, vesicles, blistering, edema) on areas exposed to sun or artificial ultraviolet (UV) light (usually the face, neck, extensor surfaces of forearms, dorsa of hands).
Avoid unnecessary or excessive exposure to sunlight or artificial UV light (tanning beds, UVA/UVB treatment) while receiving levofloxacin. If patient needs to be outdoors, they should wear loose-fitting clothing that protects skin from sun exposure and use other sun protection measures (sunscreen).
Discontinue levofloxacin if photosensitivity or phototoxicity (sunburn-like reaction, skin eruption) occurs.
Other Warnings/Precautions
Hepatotoxicity
Severe hepatotoxicity, including acute hepatitis, has occurred in patients receiving levofloxacin and sometimes resulted in death. Most cases occurred within 6–14 days of initiation of levofloxacin therapy and were not associated with hypersensitivity reactions. The majority of fatalities were in geriatric patients ≥65 years of age. (See Geriatric Use under Cautions.)
Immediately discontinue levofloxacin in any patient who develops symptoms of hepatitis (e.g., loss of appetite, nausea, vomiting, fever, weakness, tiredness, right upper quadrant tenderness, itching, yellowing of the skin or eyes, light colored bowel movements, or dark colored urine).
Prolongation of QT Interval
Prolonged QT interval leading to ventricular arrhythmias, including torsades de pointes, reported with some fluoroquinolones, including levofloxacin.
Avoid use in patients with a history of prolonged QT interval or uncorrected electrolyte disorders (e.g., hypokalemia). Also avoid use in those receiving class IA (e.g., quinidine, procainamide) or class III (e.g., amiodarone, sotalol) antiarrhythmic agents.
Risk of prolonged QT interval may be increased in geriatric patients. (See Geriatric Use under Cautions.)
Risk of Aortic Aneurysm and Dissection
Rupture or dissection of aortic aneurysms reported in patients receiving systemic fluoroquinolones. Epidemiologic studies indicate an increased risk of aortic aneurysm and dissection within 2 months following use of systemic fluoroquinolones, particularly in geriatric patients. Cause for this increased risk not identified.
Unless there are no other treatment options, do not use systemic fluoroquinolones, including levofloxacin, in patients who have an aortic aneurysm or are at increased risk for an aortic aneurysm. This includes geriatric patients and patients with peripheral atherosclerotic vascular disease, hypertension, or certain genetic conditions (e.g., Marfan syndrome, Ehlers-Danlos syndrome).
If patient reports adverse effects suggestive of aortic aneurysm or dissection, immediately discontinue the fluoroquinolone. (See Advice to Patients.)
Hypoglycemia or Hyperglycemia
Systemic fluoroquinolones, including levofloxacin, are associated with alterations in blood glucose concentrations, including symptomatic hypoglycemia and hyperglycemia. Blood glucose disturbances during fluoroquinolone therapy usually have occurred in patients with diabetes mellitus receiving an oral antidiabetic agent (e.g., glyburide) or insulin.
Severe cases of hypoglycemia resulting in coma or death reported with some systemic fluoroquinolones. Although most reported cases of hypoglycemic coma involved patients with risk factors for hypoglycemia (e.g., older age, diabetes mellitus, renal insufficiency, concomitant use of antidiabetic agents [especially sulfonylureas]), some involved patients receiving a fluoroquinolone who were not diabetic and not receiving an oral antidiabetic agent or insulin.
Carefully monitor blood glucose concentrations when levofloxacin used in diabetic patients.
If a hypoglycemic reaction occurs, discontinue the fluoroquinolone and initiate appropriate therapy immediately. (See Advice to Patients.)
Musculoskeletal Effects
Increased incidence of musculoskeletal disorders (arthralgia, arthritis, tendinopathy, gait abnormality) reported in pediatric patients receiving levofloxacin. Use in pediatric patients only for inhalational anthrax (postexposure) or treatment or prophylaxis of plague and only in those 6 months of age or older. (See Pediatric Use under Cautions.)
Fluoroquinolones, including levofloxacin, cause arthropathy and osteochondrosis in immature animals of various species. Persistent lesions in cartilage reported in levofloxacin studies in immature dogs.
C. difficile-associated Diarrhea and Colitis
Treatment with anti-infectives alters normal colon flora and may permit overgrowth of Clostridioides difficile (formerly known as Clostridium difficile). C. difficile infection (CDI) and C. difficile-associated diarrhea and colitis (CDAD; also known as antibiotic-associated diarrhea and colitis or pseudomembranous colitis) reported with nearly all anti-infectives, including levofloxacin, and may range in severity from mild diarrhea to fatal colitis. C. difficile produces toxins A and B which contribute to development of CDAD; hypertoxin-producing strains of C. difficile are associated with increased morbidity and mortality since they may be refractory to anti-infectives and colectomy may be required.
Consider CDAD if diarrhea develops during or after therapy and manage accordingly. Obtain careful medical history since CDAD may occur as late as 2 months or longer after anti-infective therapy is discontinued.
If CDAD is suspected or confirmed, discontinue anti-infectives not directed against C. difficile as soon as possible. Initiate appropriate anti-infective therapy directed against C. difficile (e.g., vancomycin, fidaxomicin, metronidazole), supportive therapy (e.g., fluid and electrolyte management, protein supplementation), and surgical evaluation as clinically indicated.
Selection and Use of Anti-infectives
Use for treatment of acute bacterial sinusitis, acute bacterial exacerbations of chronic bronchitis, or uncomplicated UTIs only when no other treatment options available. Because levofloxacin, like other systemic fluoroquinolones, has been associated with disabling and potentially irreversible serious adverse reactions (e.g., tendinitis and tendon rupture, peripheral neuropathy, CNS effects) that can occur together in the same patient, risks of serious adverse reactions outweigh benefits for patients with these infections.
To reduce development of drug-resistant bacteria and maintain effectiveness of levofloxacin and other antibacterials, use only for treatment or prevention of infections proven or strongly suspected to be caused by susceptible bacteria.
When selecting or modifying anti-infective therapy, use results of culture and in vitro susceptibility testing. In the absence of such data, consider local epidemiology and susceptibility patterns when selecting anti-infectives for empiric therapy.
Information on test methods and quality control standards for in vitro susceptibility testing of antibacterial agents and specific interpretive criteria for such testing recognized by FDA is available at [Web].
Specific Populations
Pregnancy
No adequate and well-controlled studies in pregnant women; animal studies (rats and rabbits) did not reveal evidence of fetal harm.
Use during pregnancy only if potential benefits justify potential risks to fetus.
Lactation
Distributed into milk following oral or IV administration.
Discontinue nursing or the drug.
Pediatric Use
Safety and efficacy not established for any indication in infants <6 months of age.
Labeled by FDA for inhalational anthrax (postexposure) or for treatment or prophylaxis of plague in adolescents and children ≥6 months of age. Safety and efficacy not established for any other indication in this age group.
Increased incidence of musculoskeletal disorders reported in pediatric patients receiving levofloxacin. Causes arthropathy and osteochondrosis in juvenile animals. (See Musculoskeletal Effects under Cautions.)
AAP states use of a systemic fluoroquinolone may be justified in children <18 years of age in certain specific circumstances when there are no safe and effective alternatives and the drug is known to be effective.
Geriatric Use
No substantial differences in safety and efficacy relative to younger adults, but increased sensitivity cannot be ruled out.
Risk of severe tendon disorders, including tendon rupture, is increased in older adults (usually those >60 years of age). This risk is further increased in those receiving concomitant corticosteroids. (See Tendinitis and Tendon Rupture under Cautions.) Use caution in geriatric adults, especially those receiving concomitant corticosteroids.
Serious and sometimes fatal hepatotoxicity reported with levofloxacin; majority of fatalities have occurred in geriatric patients ≥65 years of age. (See Hepatotoxicity under Cautions.)
Risk of prolonged QT interval leading to ventricular arrhythmias may be increased in geriatric patients, especially those receiving concurrent therapy with other drugs that can prolong QT interval (e.g., class IA or III antiarrhythmic agents) or with risk factors for torsades de pointes (e.g., known QT prolongation, uncorrected hypokalemia). (See Prolongation of QT Interval under Cautions.)
Risk of aortic aneurysm and dissection may be increased in geriatric patients. (See Risk of Aortic Aneurysm and Dissection under Cautions.)
Consider age-related decreases in renal function when selecting dosage. (See Renal Impairment under Dosage and Administration.)
Hepatic Impairment
Pharmacokinetics not studied in patients with hepatic impairment, but pharmacokinetic alterations unlikely.
Renal Impairment
Substantially decreased clearance and increased half-life. Use with caution and adjust dosage. (See Renal Impairment under Dosage and Administration.)
Perform appropriate renal function tests prior to and during therapy.
Common Adverse Effects
GI effects (nausea, diarrhea, constipation), headache, insomnia, dizziness.
How should I use Levofloxacin (systemic) (monograph)
Administration
Administer orally or by slow IV infusion. Do not give IM, sub-Q, intrathecally, or intraperitoneally.
IV route indicated in patients who do not tolerate or are unable to take the drug orally and in other patients when the IV route offers a clinical advantage. Oral and IV routes considered interchangeable because pharmacokinetics are similar.
Patients receiving oral or IV levofloxacin should be well hydrated and instructed to drink fluids liberally to prevent highly concentrated urine and formation of crystals in urine.
Oral Administration
Tablets: Administer without regard to meals. Do not use tablets in pediatric patients weighing <30 kg.
Oral solution: Administer 1 hour before or 2 hours after meals. (See Food under Pharmacokinetics.)
Tablets or oral solution: Administer orally at least 2 hours before or 2 hours after antacids containing magnesium or aluminum, metal cations (e.g., iron), sucralfate, multivitamins or dietary supplements containing iron or zinc, or buffered didanosine (pediatric oral solution admixed with antacid). (See Interactions.)
IV Infusion
Premixed injection for IV infusion containing 5 mg/mL in 5% dextrose (single-use flexible container): Use without further dilution.
Concentrate for injection containing 25 mg/mL (single-use vials): Must be diluted prior to IV infusion.
Do not admix with other drugs or infuse simultaneously through same tubing with other drugs. Do not infuse through same tubing with any solution containing multivalent cations (e.g., magnesium). If same administration set is used for sequential infusion of several different drugs, flush tubing before and after administration using an IV solution compatible with levofloxacin and the other drug(s).
Premixed injection for IV infusion and concentrate for injection for IV infusion contain no preservatives; discard any unused portions.
For solution and drug compatibility information, see Compatibility under Stability.
Dilution
Concentrate for injection containing 25 mg/mL (single-use vials): Dilute with a compatible IV solution prior to IV infusion to provide a solution containing 5 mg/mL.
Rate of Administration
Administer doses of 250 or 500 mg by IV infusion over 60 minutes; administer doses of 750 mg by IV infusion over 90 minutes.
Rapid IV infusion or injection associated with hypotension and must be avoided.
Dosage
Dosage of oral and IV levofloxacin is identical.
Dosage adjustments not needed when switching from IV to oral administration.
Because safety of levofloxacin given for >28 days in adults and >14 days in pediatric patients not studied, manufacturers state use prolonged therapy only when potential benefits outweigh risks.
Pediatric Patients
Anthrax
Postexposure Prophylaxis Following Exposure in the Context of Biologic Warfare or Bioterrorism
Oral or IVPediatric patients as young as 1 month of age†: AAP suggests 8 mg/kg (up to 250 mg) every 12 hours in those weighing <50 kg or 500 mg once daily in those weighing >50 kg.
Children ≥6 months of age weighing <50 kg: Manufacturer recommends 8 mg/kg (up to 250 mg) every 12 hours.
Children ≥6 months of age weighing >50 kg: Manufacturer recommends 500 mg once daily.
Initiate prophylaxis as soon as possible following suspected or confirmed exposure to aerosolized B. anthracis.
Because of possible persistence of B. anthracis spores in lung tissue following an aerosol exposure, CDC, AAP, and others recommend that anti-infective postexposure prophylaxis be continued for 60 days following a confirmed exposure.
Treatment of Uncomplicated Cutaneous Anthrax (Biologic Warfare or Bioterrorism Exposure)†
OralPediatric patients ≥1 month of age†: AAP recommends 8 mg/kg (up to 250 mg) every 12 hours in those weighing <50 kg and 500 mg once daily in those weighing >50 kg.
Recommended duration is 60 days after illness onset if cutaneous anthrax occurred after exposure to aerosolized B. anthracis spores in the context of biologic warfare or bioterrorism.
Treatment of Systemic Anthrax (Biologic Warfare or Bioterrorism Exposure)†
IVPediatric patients ≥1 month of age† with systemic anthrax: 8 mg/kg (up to 250 mg) every 12 hours in those weighing <50 kg or 500 mg once daily in those weighing >50 kg.
Pediatric patients ≥1 month of age† with systemic anthrax if meningitis excluded: 10 mg/kg (up to 250 mg) every 12 hours in those weighing <50 kg or 500 mg once daily in those weighing >50 kg.
Used in multiple-drug parenteral regimen for initial treatment of systemic anthrax (inhalational, GI, meningitis, or cutaneous anthrax with systemic involvement, lesions on the head or neck, or extensive edema). Continue parenteral regimen for ≥2–3 weeks until patient is clinically stable and can be switched to appropriate oral anti-infective.
If systemic anthrax occurred after exposure to aerosolized B. anthracis spores in the context of biologic warfare or bioterrorism, continue oral follow-up regimen until 60 days after illness onset.
OralPediatric patients ≥1 month of age† (follow-up after initial multiple-drug parenteral regimen): 8 mg/kg (up to 250 mg) every 12 hours in those weighing <50 kg or 500 mg once daily in those weighing ≥50 kg.
If systemic anthrax occurred after exposure to aerosolized B. anthracis spores in the context of biologic warfare or bioterrorism, continue oral follow-up regimen until 60 days after illness onset.
Plague
Treatment or Prophylaxis of Plague
Oral or IVChildren ≥6 months of age weighing <50 kg: 8 mg/kg (up to 250 mg) every 12 hours for 10–14 days.
Children ≥6 months of age weighing >50 kg: 500 mg once daily for 10–14 days. Higher dosage (i.e., 750 mg once daily) may be used if clinically indicated.
Initiate as soon as possible after suspected or known exposure to Y. pestis.
Adults
Respiratory Tract Infections
Acute Bacterial Sinusitis
Oral or IV500 mg once every 24 hours for 10–14 days. (See Respiratory Tract Infections under Uses.)
Alternatively, 750 mg once every 24 hours for 5 days.
Acute Bacterial Exacerbations of Chronic Bronchitis
Oral or IV500 mg once every 24 hours for 7 days. (See Respiratory Tract Infections under Uses.)
Community-acquired Pneumonia (CAP)
Oral or IVS. aureus, S. pneumoniae (including MDRSP), K. pneumoniae, L. pneumophila, M. catarrhalis: 500 mg once every 24 hours for 7–14 days.
S. pneumoniae (except MDRSP), H. influenzae, H. parainfluenzae, M. pneumoniae, or C. pneumoniae: 500 mg once every 24 hours for 7–14 days or, alternatively, 750 mg once every 24 hours for 5 days.
If used for empiric treatment of CAP or treatment of CAP caused by Ps. aeruginosa, IDSA and ATS recommend 750 mg once daily.
IDSA and ATS state that CAP should be treated for a minimum of 5 days and patients should be afebrile for 48–72 hours before discontinuing anti-infective therapy.
Nosocomial Pneumonia
Oral or IV750 mg once every 24 hours for 7–14 days.
Skin and Skin Structure Infections
Uncomplicated Infections
Oral or IV500 mg once every 24 hours for 7–10 days.
Complicated Infections
Oral or IV750 mg once every 24 hours for 7–14 days.
Urinary Tract Infections (UTIs) and Prostatitis
Uncomplicated UTIs
Oral or IV250 mg once every 24 hours for 3 days. (See Urinary Tract Infections [UTIs] and Prostatitis under Uses.)
Complicated UTIs
Oral or IVE. faecalis, E. cloacae, or Ps. aeruginosa: 250 mg once every 24 hours for 10 days.
E. coli, K. pneumoniae, or P. mirabilis: 250 mg once every 24 hours for 10 days or, alternatively, 750 mg once every 24 hours for 5 days.
Acute Pyelonephritis
Oral or IVE. coli: 250 mg once every 24 hours or 10 days or, alternatively, 750 mg once every 24 hours for 5 days.
Chronic Prostatitis
Oral or IV500 mg once every 24 hours for 28 days.
GI Infections†
Campylobacter Infections†
Oral or IVHIV-infected: 750 mg once daily.
Recommended treatment duration is 7–10 days for gastroenteritis or ≥14 days for bacteremic infections. Duration of 2–6 weeks recommended for recurrent infections.
Salmonella Gastroenteritis†
Oral or IVHIV-infected: 750 mg once daily.
Recommended treatment duration is 7–14 days if CD4+ T-cells ≥200 cells/mm3 (≥14 days if bacteremic or infection is complicated) or 2–6 weeks if CD4+ T-cells <200 cells/mm3.
Consider secondary prophylaxis in those with recurrent bacteremia; also may consider in those with recurrent gastroenteritis (with or without bacteremia) or with CD4+ T-cells <200 cells/mm3 and severe diarrhea. Discontinue secondary prophylaxis if Salmonella infection resolves and there has been a sustained response to antiretroviral therapy with CD4+ T-cells >200 cells/mm3.
Shigella Infections†
Oral or IVHIV-infected: 750 mg once daily.
Recommended treatment duration is 7–10 days for gastroenteritis or ≥14 days for bacteremic infections. Up to 6 weeks may be required for recurrent infections, especially if CD4+ T-cells <200 cells/mm3.
Treatment of Travelers’ Diarrhea†
Oral500 mg once daily for 1–3 days.
Prevention of Travelers’ Diarrhea†
Oral500 mg once daily.
Anti-infective prophylaxis generally discouraged (see GI Infections under Uses); if such prophylaxis used, give during period of risk (not exceeding 2–3 weeks) beginning day of travel and continuing for 1 or 2 days after leaving area of risk.
Helicobacter pylori Infection
Oral500 mg once daily usually used; 250 mg once daily also has been used.
Used as a component of multiple-drug regimen (see GI Infections under Uses).
Anthrax
Postexposure Prophylaxis of Anthrax (Biologic Warfare or Bioterrorism Exposure)
Oral or IV500 mg once daily recommended by manufacturers.
750 mg once daily recommended by CDC.
Initiate prophylaxis as soon as possible following suspected or confirmed exposure to aerosolized B. anthracis.
Because of possible persistence of B. anthracis spores in lung tissue following an aerosol exposure, CDC and others recommend that anti-infective postexposure prophylaxis be continued for 60 days following a confirmed exposure.
Treatment of Uncomplicated Cutaneous Anthrax (Biologic Warfare or Bioterrorism Exposure)†
Oral750 mg once daily.
Recommended duration is 60 days if cutaneous anthrax occurred after exposure to aerosolized B. anthracis spores in the context of biologic warfare or bioterrorism.
Treatment of Systemic Anthrax (Biologic Warfare or Bioterrorism Exposure)†
IV750 mg once daily.
Used in multiple-drug parenteral regimen for initial treatment of systemic anthrax (inhalational, GI, meningitis, or cutaneous with systemic involvement, lesions on the head or neck, or extensive edema). Continue parenteral regimen for ≥2–3 weeks until patient is clinically stable and can be switched to appropriate oral anti-infective.
If anthrax occurred after exposure to aerosolized B. anthracis spores in the context of biologic warfare or bioterrorism, continue oral follow-up regimen until 60 days after illness onset.
Chlamydial Infections†
Urogenital Infections†
Oral500 mg once daily for 7 days recommended by CDC for infections caused by C. trachomatis.
Gonorrhea and Associated Infections†
Epididymitis†
Oral500 mg once daily for 10 days recommended by CDC.
Use only when epididymitis† most likely caused by sexually transmitted enteric bacteria (e.g., E. coli) and N. gonorrhoeae ruled out. (See Gonorrhea and Associated Infections under Uses.)
Mycobacterial Infections†
Active Tuberculosis†
Oral or IV0.5–1 g once daily. Must be used in conjunction with other antituberculosis agents.
ATS, CDC, and IDSA state data insufficient to date to support intermittent levofloxacin regimens for treatment of tuberculosis.
Disseminated MAC Infections
OralHIV-infected: 500 mg once daily.
Nongonococcal Urethritis†
Oral
500 mg once daily for 7 days recommended by CDC.
Pelvic Inflammatory Disease†
Oral
500 mg once daily for 14 days given in conjunction with oral metronidazole (500 mg twice daily for 14 days).
Use only when cephalosporins not feasible, community prevalence and individual risk of gonorrhea low, and in vitro susceptibility confirmed. (See Pelvic Inflammatory Disease under Uses.)
IV
500 mg once daily; used with or without IV metronidazole (500 mg every 8 hours).
Use only when cephalosporins not feasible, community prevalence and individual risk of gonorrhea are low, and in vitro susceptibility confirmed. (See Pelvic Inflammatory Disease under Uses.)
Plague
Treatment or Prophylaxis of Plague
Oral or IV500 mg once daily for 10–14 days. Higher dosage (i.e., 750 mg once daily) may be used if clinically indicated.
Initiate as soon as possible after suspected or known exposure to Y. pestis.
Special Populations
Hepatic Impairment
Dosage adjustments not required.
Renal Impairment
Adjust dosage in adults with Clcr <50 mL/minute. (See Table 1.) Adjustments not needed when used for treatment of uncomplicated UTIs in patients with renal impairment.
Dosage recommendations not provided by manufacturer for pediatric patients with renal impairment.
Usual Daily Dosage for Normal Renal Function (Clcr ≥ 50 mL/min) |
Clcr (mL/min) |
Dosage for Renal Impairment |
---|---|---|
250 mg |
20–49 |
Dosage adjustment not required |
250 mg |
10–19 |
Uncomplicated UTIs: Dosage adjustment not required. Other infections: 250 mg once every 48 hours |
250 mg |
Hemodialysis or CAPD patients |
Information not available |
500 mg |
20–49 |
Initial 500-mg dose, then 250 mg once every 24 hours |
500 mg |
10–19 |
Initial 500-mg dose, then 250 mg once every 48 hours |
500 mg |
Hemodialysis or CAPD patients |
Initial 500-mg dose, then 250 mg once every 48 hours; supplemental doses not required after dialysis |
750 mg |
20–49 |
750 mg once every 48 hours |
750 mg |
10–19 |
Initial 750-mg dose, then 500 mg once every 48 hours |
750 mg |
Hemodialysis or CAPD patients |
Initial 750-mg dose, then 500 mg once every 48 hours; supplemental doses not required after dialysis |
Geriatric Patients
No dosage adjustments except those related to renal impairment. (See Renal Impairment under Dosage and Administration.)
What other drugs will affect Levofloxacin (systemic) (monograph)?
Drugs That Prolong QT Interval
Potential pharmacologic interaction (additive effect on QT interval prolongation). Avoid use in patients receiving class IA (e.g., quinidine, procainamide) or class III (e.g., amiodarone, sotalol) antiarrhythmic agents. (See Prolongation of QT Interval under Cautions.)
Specific Drugs and Laboratory Tests
Drug or Test |
Interaction |
Comments |
---|---|---|
Antacids (aluminum- or magnesium-containing) |
Decreased absorption of oral levofloxacin; data not available regarding IV levofloxacin |
Administer oral levofloxacin at least 2 hours before or 2 hours after such antacids |
Antiarrhythmic agents |
Potential additive effects on QT interval prolongation Procainamide: Increased half-life and decreased clearance of procainamide |
Avoid levofloxacin in patients receiving class IA (e.g., quinidine, procainamide) or class III (e.g., amiodarone, sotalol) antiarrhythmic agents |
Anticoagulants, oral (warfarin) |
Enhanced warfarin effects and clinical bleeding |
Monitor PT, INR, or other suitable coagulation tests and monitor for bleeding |
Antidiabetic agents (e.g., insulin, glyburide) |
Alterations in blood glucose (hyperglycemia and hypoglycemia) reported |
Closely monitor blood glucose; if hypoglycemic reaction occurs, immediately discontinue levofloxacin and initiate appropriate therapy |
Cimetidine |
Slightly increased levofloxacin AUC and half-life |
Not considered clinically important; levofloxacin dosage adjustments not warranted |
Corticosteroids |
Increased risk of tendinitis or tendon rupture, especially in patients >60 years of age |
Use concomitantly with caution |
Cyclosporine or tacrolimus |
Possible increased AUC of cyclosporine or tacrolimus |
Manufacturer of levofloxacin states dosage adjustments not needed for either drug when levofloxacin used with cyclosporine; some clinicians suggest monitoring plasma concentrations of cyclosporine or tacrolimus |
Didanosine |
Possible decreased absorption of oral levofloxacin; data not available regarding IV levofloxacin |
Administer oral levofloxacin at least 2 hours before or 2 hours after buffered didanosine (pediatric oral solution admixed with antacid) |
Digoxin |
No evidence of clinically important effect on pharmacokinetics of digoxin or levofloxacin |
Dosage adjustments not needed for either drug |
Iron preparations |
Decreased absorption of oral levofloxacin; data not available regarding IV levofloxacin |
Administer oral levofloxacin at least 2 hours before or after ferrous sulfate and dietary supplements containing iron |
Multivitamins and mineral supplements |
Decreased absorption of oral levofloxacin; data not available regarding IV levofloxacin |
Administer oral levofloxacin at least 2 hours before or 2 hours after supplements containing zinc, calcium, magnesium, or iron |
NSAIAs |
Possible increased risk of CNS stimulation, seizures; animal studies suggest risk may be less than that associated with some other fluoroquinolones |
|
Probenecid |
Slightly increased levofloxacin AUC and half-life |
Not considered clinically important; levofloxacin dosage adjustments not required |
Psychotherapeutic agents |
Fluoxetine or imipramine: Potential additive effect on QT interval prolongation |
|
Tests for opiates |
Possibility of false-positive results for opiates in patients receiving some quinolones, including levofloxacin, when commercially available urine screening immunoassay kits are used |
Positive opiate urine screening test results may need to be confirmed using more specific methods |
Sucralfate |
Decreased absorption of oral levofloxacin; data not available regarding IV levofloxacin |
Administer oral levofloxacin at least 2 hours before or 2 hours after sucralfate |
Theophylline |
No evidence of clinically important pharmacokinetic interaction with levofloxacin; increased theophylline concentrations and increased risk of theophylline-related adverse effects reported with some other quinolones |
Closely monitor theophylline concentrations and make appropriate dosage adjustments; consider that adverse theophylline effects (e.g., seizures) may occur with or without elevated theophylline concentrations |