Teicoplanin

Not available in the US

Mechanism of Action

  • Bactericidal; binds irreversibly to D-ala-D-ala cell wall precorsor, inhibiting cell wall synthesis

General

Adult Dosing

Bacterial Meningitis

  • 15-20mg/kg IV q8-12h

Bacterial Endocarditis

  • 15mg/kg q12h

Febrile Neutropenia

  • 15mg/kg q12h

Skin / soft tissue infection

  • 15-20mg/kg q8-12h

Pneumonia

  • 15-20mg/kg q8-12h

Sepsis / Bacteremia

  • 15-20mg/kg q8-12h

CNS Infection

  • 15-20mg/kg q8-12h
    • Up to 2g q8h may be required to achieve adequate CSF penetration

Peritonitis (peritoneal dialysis associated)

  • 20-25mg/L, added to dialysate fluid


Pediatric Dosing

Pediatric Dosing

General

  • 15mg/kg q6hr
  • Do not exceed 750mg per dose in patients with normal renal function

Neonates

  • 10-15mg/kg q8-24h (depending on PMA)

Special Populations

  • Pregnancy Rating: C
  • Lactation Risk: Probably safe
  • Obesity: Dose based on total body weight; may require more frequent dosing

Renal Dosing

  • Load: 15-25mg/kg IV regardless of renal function
  • Maintenance: 7.5-15mg/kg/day in 1-3 divided doses (q8-24hr intervals) based on CrCl
    • CrCl >50: 7.5-15mg/kg q12hr
    • CrCl 10-50: 7.5-15mg/kg q24hr
    • CrCl <10: 7.5-15mg/kg q48-72hr (or redose based on levels)
  • Therapeutic trough level: 10-20 mcg/mL (15-20 mcg/mL for MRSA or severe infections)

Hepatic Dosing

  • No dose adjustment necessary

Contraindications

  • Allergy to class/drug

Adverse Reactions

Serious

Common

  • Phlebitis
  • GI upset (with PO)

Pharmacology

  • Half-life: 6-8 hours (normal renal function); 6-10 days (anuria)
  • Metabolism: None
  • Excretion: Urine

See Also

Adult Dosing

Pediatric Dosing

Special Populations

  • Pregnancy Rating:
  • Lactation:
  • Renal Dosing
    • Adult
    • Pediatric
  • Hepatic Dosing
    • Adult
    • Pediatric

Contraindications

  • Allergy to class/drug

Adverse Reactions

Serious

Common

Pharmacology

  • Half-life:
  • Metabolism:
  • Excretion:
  • Mechanism of Action:

Antibiotic Sensitivities[1]

Group Organism Sensitivity
Gram Positive Strep. Group A, B, C, G S
Strep. Pneumoniae S
Viridans strep X1
Strep. anginosus gp X1
Enterococcus faecalis S
Enterococcus faecium I
MSSA S
MRSA S
CA-MRSA S
Staph. Epidermidis I
C. jeikeium S
L. monocytogenes S
Gram Negatives N. gonorrhoeae R
N. meningitidis R
Moraxella catarrhalis X1
H. influenzae X1
E. coli R
Klebsiella sp R
E. coli/Klebsiella ESBL+ R
E coli/Klebsiella KPC+ R
Enterobacter sp, AmpC neg R
Enterobacter sp, AmpC pos R
Serratia sp X1
Serratia marcescens R
Salmonella sp R
Shigella sp R
Proteus mirabilis X1
Proteus vulgaris R
Providencia sp. X1
Morganella sp. X1
Citrobacter freundii X1
Citrobacter diversus X1
Citrobacter sp. X1
Aeromonas sp X1
Acinetobacter sp. R
Pseudomonas aeruginosa R
Burkholderia cepacia R
Stenotrophomonas maltophilia R
Yersinia enterocolitica X1
Francisella tularensis X1
Brucella sp. R
Legionella sp. X1
Pasteurella multocida X1
Haemophilus ducreyi X1
Vibrio vulnificus X1
Misc Chlamydophila sp X1
Mycoplasm pneumoniae X1
Rickettsia sp R
Mycobacterium avium X1
Anaerobes Actinomyces X1
Bacteroides fragilis X1
Prevotella melaninogenica X1
Clostridium difficile S
Clostridium (not difficile) S
Fusobacterium necrophorum X1
Peptostreptococcus sp. S

Key

  • S susceptible/sensitive (usually)
  • I intermediate (variably susceptible/resistant)
  • R resistant (or not effective clinically)
  • S+ synergistic with cell wall antibiotics
  • U sensitive for UTI only (non systemic infection)
  • X1 no data
  • X2 active in vitro, but not used clinically
  • X3 active in vitro, but not clinically effective for Group A strep pharyngitis or infections due to E. faecalis
  • X4 active in vitro, but not clinically effective for strep pneumonia

See Also

References

  1. Sanford Guide to Antimicrobial Therapy 2014
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