vancomycin and other agents with activity against gram-positive aerobes Flashcards
glycopeptides
vancomycin
streptogramins
quinupristin-dalfopristin (synercid)
oxazolidinones
linezolid, tedizolid
lipopeptides
daptomycin
lipoglycopeptides
telavancin, dalbavancin, oritavancin
vancomycin chemistry
Vancomycin is derived from Streptomyces orientalis and has a unique structure in that it is a complex tricyclic glycopeptide* with a molecular weight of 1500 Daltons.
vancomycin MOA
Vancomycin inhibits the synthesis of the bacterial cell wall* by blocking glycopeptide polymerization at a site different from that of the β-lactams.
Vancomycin inhibits synthesis and assembly during the second stage* of cell wall synthesis by firmly binding to the D-alanyl-D-alanine portion of cell wall precursors. Vancomycin prevents cross-linking and further elongation of peptidoglycan, which weakens the cell wall making it susceptible to lysis.
Vancomycin is slowly bactericidal in a time-dependent manner, except against Enterococcus spp. where it displays bacteriostatic activity.
vancomycin MOR**
In vancomycin resistant Enterococcus (VRE) and vancomycin resistant Staphylococcus aureus (VRSA), resistance to vancomycin is due to modification of the D-alanyl-D-alanine vancomycin-binding site* of the peptide side chain of peptidoglycan precursors by expression of the vanA (or vanB, vanC, vanD or vanE) gene. The terminal D-alanine is replaced by D-lactate, which results in the loss of a critical hydrogen bond that usually facilitates high-affinity binding of vancomycin to its target. The end result is the loss of antibacterial activity.
In vancomycin intermediate Staphylococcus aureus (VISA), resistance to vancomycin is due to thickening of the peptidoglycan layer of the cell wall, restricting access of vancomycin to its site of activity.
vancomycin spectrum of activity
Vancomycin displays activity against many Gram-positive aerobic and anaerobic bacteria
-Groups A, B, C, D, F, and G streptococci
-Viridans streptococci
-Streptococcus pneumoniae (including penicillin-resistant strains, PRSP)
-Enterococcus faecalis and faecium (ONLY BACTERIOSTATIC)
-Staphylococcus aureus and coagulase-negative staphylococci {CNS} (both** methicillin-susceptible {MSSA - not DOC} and methicillin-resistant strains {MRSA - DOC})
-Corynebacterium spp.
-Listeria monocytogenes
-Actinomyces
-Clostridium spp. (INCLUDING C. difficile)
In vitro studies demonstrate synergy between vancomycin and gentamicin or streptomycin against Enterococcus spp., and between vancomycin and gentamicin against viridans streptococci and Staphylococcus spp.
Gram-positive organisms that display resistance to vancomycin include select isolates of Enterococcus faecalis and E. faecium; and most isolates of E. gallinarum, E. casseliflavus, E. durans, Pediococcus spp., and Leuconostoc spp.
Vancomycin is NOT active against Gram-negative aerobes or anaerobes.*
vancomycin pharmacology overview
Interpatient variability exists in the pharmacokinetic characteristics of volume of distribution and clearance** of vancomycin. The PD parameter associated with efficacy has not yet been clearly defined (?AUC/MIC of 400).
vancomycin absorption
Absorption of vancomycin from the gastrointestinal tract is negligible** after oral administration. Absorption may occur with oral administration in the presence of intense inflammatory colitis, with detectable serum concentrations occasionally observed in patients with renal insufficiency.
**For the treatment of systemic infections, intermittent intravenous infusion is the preferred route of administration (not IM).
vancomycin distribution
Vancomycin is widely distributed into body tissues and fluids, including pleural fluid, synovial fluid, ascites, adipose tissue, and bile. Vancomycin displays variable penetration into the CSF, even in the presence of inflamed meninges.
Vancomycin takes approximately ONE HOUR to distribute from the plasma compartment into peripheral tissues and fluids.
Interpatient variability exists in the volume of distribution:
-Vd adults = 0.50 to 0.65 L/kg
-Neonates and infants have a larger Vd than adults. From birth to the first year of life, the Vd declines from an initial value of over 0.7 L/kg to the adult value of 0.5 L/kg.
-Total body weight (TBW) should be used for vancomycin dosing** as it results in a more accurate approximation of the Vd.
vancomycin elimination
Intravenous vancomycin is primarily eliminated unchanged by the kidney via glomerular filtration.
In adults with normal renal function, the elimination half-life = 6 to 8 hours. The half-life progressively increases as renal function decreases.** In patients with end-stage renal disease, the elimination half-life of vancomycin approaches 7 to 14 days. *
Vancomycin is NOT appreciably removed by hemodialysis. Vancomycin may be removed during peritoneal dialysis or continuous hemofiltration.
vancomycin serum concentration monitoring
There are NO well-controlled clinical trials relating vancomycin serum concentrations to efficacy or toxicity.
Because of interpatient variability in Vd and Cl of vancomycin, serum concentration monitoring may be warranted in some patients to help avoid excessive serum concentrations such as in patients with renal dysfunction, changing renal function, receiving aggressive dosing, or receiving long-term therapy.
“Target” peak concentrations = 30 to 40 μg/ml; “Target” trough concentrations = 10 to 15 μg/ml (some clinicians target higher trough concentrations for the treatment of meningitis, endocarditis, pneumonia, and osteomyelitis due to MRSA with vanco MICs of 2 mg/L)
Peak concentrations should be obtained one hour after the end of infusion* and trough concentrations should be drawn just prior to the dose.
dosing of vancomycin
The differences in the vancomycin pharmacokinetic parameters must be considered when determining a vancomycin dose for each patient. Factors that should be considered include the patient’s volume status, renal function, age, gender, weight, concomitant drug therapy, and infection being treated, severity of infection, etc.
Several vancomycin-dosing nomograms are available to assist with dosing based on a patient’s age, weight, and renal function.
Adults with normal renal function: 10 to 15 mg/kg* (typically 1 to 1.5 grams) every 12 hours
Adults with impaired renal function: 10 to 15 mg/kg/dose* (typically 1 to 1.5 grams) with interval based on renal function (every 18, 24, 36, 48 hours)
Vancomycin Dosing Interval Depends on Renal Function:
- CrCl over70 = Every 12 hours
- CrCl 40 - 69 = Every 24 hours
- CrCl 25 - 39 = Every 48 hours
- CrCl under 25 = Every 72 hours or longer
- Neonates and children: 10 to 15 mg/kg/dose every 6 to 24 hours based on gestational age or renal function
- **TBW (up to ∼ 200kg) should be used for dosing in obese patients - maximum initial doses should not exceed 2000mg to 3000 mg
vancomycin clinical uses
Infections due to methicillin-resistant staphylococci** (MRSA, CNS) including bacteremia, pneumonia, empyema, endocarditis, peritonitis, osteomyelitis, and skin/soft tissue infections. Intraventricular vancomycin has been rarely used as adjunctive therapy for the treatment of meningitis.
Serious Gram-positive infections in patients allergic to β-lactam antibiotics.
Infections caused by resistant* Gram-positive organisms such as Corynebacterium jeikeium or penicillin-resistant Streptococcus pneumoniae (PRSP).
Perioperative prophylaxis to reduce the risk of infection in patients undergoing cardiac, neurosurgical, orthopedic, or vascular surgical procedures where the local or regional rates of MRSA are high.
**ORAL vancomycin is the drug of choice for the treatment of moderate to severe Clostridium difficile colitis (125 mg PO Q 6 hours)
vancomycin AEs
red-man syndrome, nephrotoxicity and ototoxicity, dermatalogic, hematologic, other
the overall incidence of adverse effects decreased with purification of branded vancomycin; however, generic products are now available
red-man syndrome with vancomycin**
Characterized by flushing, pruritus, and a maculopapular or erythematous rash on the face, neck, chest, and upper extremities. The reaction may also be accompanied by hypotension.
Begins within 5 to 15 minutes of starting the vancomycin infusion and resolves spontaneously over several hours after the discontinuation of the infusion. The reaction has also been rarely reported after oral and intraperitoneal administration.
Reaction is related to the rate of vancomycin infusion** (faster than 15 mg per minute); rapid infusion causes the release of histamine and other vasodilating substances.
To minimize or prevent this reaction, vancomycin doses of 1 gram should be infused over at least one hour and larger doses should be infused over 90 to 120 minutes. Other measures to alleviate this reaction include further lengthening of the infusion (over 2 or 3 hours) and premedication with antihistamines or corticosteroids.
nephrotoxicity and ototoxicity with vancomycin
Occurs rarely with vancomycin monotherapy (under 5%); more common in patients receiving concomitant ototoxins and nephrotoxins (10 to 15%).
Risk factors include the presence of underlying renal insufficiency, the use of prolonged therapy or high doses, ? high serum trough vancomycin concentrations, and concomitant use of other ototoxins or nephrotoxins.
The correlation between serum vancomycin concentrations and toxicity remains to be clarified.
Nephrotoxicity is manifested by transient increases in BUN or serum creatinine, and occasionally the presence of granular casts in the urine. The occurrence of nephrotoxicity is usually transient and reversible.
Vancomycin may cause damage to the auditory branch of the 8th cranial nerve. Tinnitus and high-frequency hearing loss may precede the onset of deafness, and necessitates the discontinuation of therapy. Hearing loss is irreversible.
dermatologic AEs with vancomycin
Hypersensitivity skin reactions occur in under 5% of patients who receive vancomycin. Reactions include exfoliative dermatitis, linear IgA bullous dermatosis, macular rashes, vasculitis, and Stevens-Johnson.
