Vancomycin: Difference between revisions

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(: added spectrum of activity)
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*Inhibits cross-linking of peptidoglycans in the cell wall
 
*Inhibits cross-linking of peptidoglycans in the cell wall
   
=== Mechanisms of Resistance ===
+
===Mechanisms of Resistance===
   
* Alterations in peptidoglycans conferred by chromosomal or plasmid-mediated ''vanA'', ''vanB'', or ''vanC''
+
*Alterations in peptidoglycans conferred by chromosomal or plasmid-mediated ''vanA'', ''vanB'', or ''vanC''
   
=== Spectrum of Activity ===
+
===Spectrum of Activity===
   
* Broadly active against Gram-positive bacteria, including anaerobes
+
*Broadly active against Gram-positive bacteria, including anaerobes
* Not active against Gram-negative bacteria
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*Not active against Gram-negative bacteria
* Notable resistance occurs in:
+
*Notable resistance occurs in:
** [[Clostridium innocuum]]
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**[[Clostridium innocuum]]
** [[Enterococcus gallinarum]], [[Enterococcus casseliflavus]], and [[Enterococcus flavus]] (chromosomal ''vanC'')
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**[[Enterococcus gallinarum]], [[Enterococcus casseliflavus]], and [[Enterococcus flavus]] (chromosomal ''vanC'')
** [[Erysipelothrix rhusiopathiae]]
+
**[[Erysipelothrix rhusiopathiae]]
** [[Lactobacillus]], except [[Lactobacillus acidophilus]] and [[Lacobacillus delbrueckii]]
+
**[[Lactobacillus]], except [[Lactobacillus acidophilus]] and [[Lacobacillus delbrueckii]]
** [[Leuconostoc]]
+
**[[Leuconostoc]]
** [[Pediococcus]]
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**[[Pediococcus]]
** [[Weissella]]
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**[[Weissella]]
   
 
===Pharmacodynamics===
 
===Pharmacodynamics===
   
 
*Efficacy predicted by AUC to MIC ratio
 
*Efficacy predicted by AUC to MIC ratio
  +
  +
=== Breakpoints ===
  +
{| class="wikitable"
  +
! rowspan="2" |Species
  +
! colspan="4" |Breakpoints (μg/mL)
  +
|-
  +
!S
  +
!SDD
  +
!I
  +
!R
  +
|-
  +
|[[Staphylococcus aureus]]
  +
|≤2
  +
|—
  +
|4-8
  +
|≥16
  +
|-
  +
|[[Staphylococcus species]] other than ''aureus''
  +
|≤4
  +
|—
  +
|8-16
  +
|≥32
  +
|-
  +
|[[Enterococcus species]]
  +
|≤4
  +
|—
  +
|8-16
  +
|≥32
  +
|-
  +
|[[Streptococcus pneumoniae]]
  +
|≤1
  +
|—
  +
|—
  +
|—
  +
|-
  +
|[[β-hemolytic streptococci]]
  +
|≤1
  +
|—
  +
|—
  +
|—
  +
|}
   
 
==Indications==
 
==Indications==

Revision as of 16:59, 21 August 2020

Background

Mechanism of Action

  • Inhibits cross-linking of peptidoglycans in the cell wall

Mechanisms of Resistance

  • Alterations in peptidoglycans conferred by chromosomal or plasmid-mediated vanA, vanB, or vanC

Spectrum of Activity

Pharmacodynamics

  • Efficacy predicted by AUC to MIC ratio

Breakpoints

Species Breakpoints (μg/mL)
S SDD I R
Staphylococcus aureus ≤2 4-8 ≥16
Staphylococcus species other than aureus ≤4 8-16 ≥32
Enterococcus species ≤4 8-16 ≥32
Streptococcus pneumoniae ≤1
β-hemolytic streptococci ≤1

Indications

  • Suspected or confirmed MRSA

Dosing

  • Common dose
    • Loading dose of 25-30 mg/kg given once for serious infections
    • 15 mg/kg/dose with timing based on renal function (q12h if normal)
    • Titrate based on monitoring parameters (below)
    • Adjustments assume linear pharmacokinetics,so a doubling of the daily dose, for example, should double the trough or AUC:MIC

Obesity

  • Dosing should use actual body weight, with a maximum loading dose of 3 g

Monitoring

  • Based on PK/PD modelling, the trough level was previously used to dose vancomycin
    • Serum trough drawn within hour before fourth dose
    • 10-15 for low-risk infections
    • 15-20 for high-risk Staphylococcus aureus infections such as osteomyelitis, meningitis, and bacteremia
  • Current guidelines recommend AUC:MIC monitoring using Bayesian calculators1
    • Use peak 60 min after infusion and trough 1 to 60 minutes before next dose, and record times accurately
    • Target AUC/MICBMD ratio of 400 to 600 for serious Staphylococcus aureus infections

Adverse Reactions

Renal Failures

  • Risk factors
    • Prolonged courses >21 days
    • Higher trough
    • Concomitant nephrotoxic medication
    • Older age
    • CKD/AKI
    • Liver disease
    • Peritonitis
    • Neutropenia
    • Male sex
  • Mechanism of injury: oxidative stress in the proximal tubular cells

Red Person Syndrome

  • Rash, pruritis, and hypotension, with onset of vancomycin, resolves on stopping
  • Very high incidence previously
  • Histamine-mediated
  • Can decrease dose or prolong infusion, prophylactic antihistamines

References

  1. ^  Michael J Rybak, Jennifer Le, Thomas P Lodise, Donald P Levine, John S Bradley, Catherine Liu, Bruce A Mueller, Manjunath P Pai, Annie Wong-Beringer, John C Rotschafer, Keith A Rodvold, Holly D Maples, Benjamin M Lomaestro. Therapeutic monitoring of vancomycin for serious methicillin-resistant Staphylococcus aureus infections: A revised consensus guideline and review by the American Society of Health-System Pharmacists, the Infectious Diseases Society of America, the Pediatric Infectious Diseases Society, and the Society of Infectious Diseases Pharmacists. American Journal of Health-System Pharmacy. 2020. doi:10.1093/ajhp/zxaa036.