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New trends, aminoglycoside toxicity and multidrug resistance

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Loma Linda University Children's Hospital. New trends, aminoglycoside toxicity ... Gram negative bacilli ( GNB) resistant to extended spectrum beta lactamases ... – PowerPoint PPT presentation

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Title: New trends, aminoglycoside toxicity and multidrug resistance


1
New trends, aminoglycoside toxicity and multidrug
resistance
  • Kim Wan (NICU pharmacist)
  • Dept of Pharmacy Services
  • LLUMC
  • May, 2007

2
Aminoglycoside
  • Includes Streptomycin, Gentamicin, Tobramycin,
    Neomycin, Kanamycin, Amikacin
  • Auditory changes are irreversible
  • Has inherent potential for causing
    nephrotoxicity and ototoxicity

3
Nephrotoxicity
  • Accumulation of drugs in the proximal renal
    tubular epithelia cells.
  • Saturated at relative low concentration
  • Higher peak level do not associate with greater
    toxicity

4
Ototoxicity
  • Aminoglycoside induced high frequency hearing
    loss results from progressive loss of function
    from the outer hair cells to the inner hair cells
  • Can occur with normal levels ( prolonged use)
  • Tends to accumulate within the inner ear

5
Aminoglycoside
  • Dosing should be based on indication, dosing
    weight, and renal function
  • Blood urea nitrogen, serum creatinine, creatinine
    clearance
  • Drug level monitoring, avoiding troughgt2mcg/ml
    (gent and tobramycin) lt5 mcg/ml for
    streptomycin
  • Peak level to stay within therapeutics
    (4-8mcg/ml)gentamicin/tobramycin Streptomycin
    15-40mcg/ml

6
Aminoglycoside
  • Dosing adjustment based upon result of serum drug
    concentration monitoring
  • Dosing for neonates should also based on age
  • Peak level drawn at 1 hr post IM injection ( iv
    30 minutes after end of 30 min. infusion)
  • Trough with 30 minutes before next dose

7
Prevention
  • Use non-ototoxic antibiotics
  • Avoid potentiating agents ( e.g. loop diuretics)

8
Multiple drug resistance (MDRO)
  • Defined as microorganisms (bacteria) are
    resistant to one or more classes of antimicrobial
    agents
  • e.g. MRSA, VRE resistant to most antimicrobial
    agents

9
Clinical importance
  • Options for treating patients for susceptible
    pathogens are limited
  • e.g. VRE during 1990virtually no antimicrobial
    agents to treat VRE
  • Increase length of stay, cost and mortality

10
Epidemiology of MDROs
  • Prevalence varies temporally, geographically and
    by healthcare setting
  • Level of care of especially tertiary care
    facilities
  • Antimicrobial resistance rates are strongly
    corrected with hospital size, tertiary-level care
    and facility type
  • Gram negative bacilli ( GNB) resistant to
    extended spectrum beta lactamases ( ESBLS),
    fluroquinolones, carbapenems and aminoglycoside
    also increased in prevalence

11
Concepts in transmission
  • Once MDROs is introduced to a healthcare setting,
    transmission and persistence of resistant strain
    to vulnerable patients, selective pressure by
    antimicrobial use.
  • Increase potential transmission from colonized
  • or infected patients

12
Community associated MRSA
  • CA MRSA infection commonly presents as relative
    minor skin and soft tissues, but severe invasive
    disease, including necrotizing pneumonia,
    necrotizing faciitis, severe osteomyelitis, and a
    sepsis syndrome with increased

13
MDRO prevention
  • Optimal management of vascular and urinary
    catheters
  • Prevention of lower respiratory tract infection
    in intubated patients
  • Accurate diagnosis of infectious etiologies
  • Judicious antimicrobial selection and utilization

14
MDRO prevention and control
  • Improvements in hand hygiene
  • Use Contact precautions until patients are
    culture negative for a target MDRO
  • Active surveillance cultures , education
  • Enhanced environmental cleaning
  • Improvement in communication about patients with
    MDROs with and between healthcare facilities

15
New challenge
  • More elderly
  • More patients from long term care facilities
  • Sicker patients
  • Increased treatment on an outpatient basis
  • More ICU beds

16
New challenge
  • New infectious diseases
  • More resistant pathogens
  • Availability of new antibiotics
  • New diagnosis
  • New vaccine development

17
Reference
  • Siegl, Jane D. Management of Multidrug-Resistant
    Organisms in Healthcare Settings, 2006, CDC.
  • Kimble, Kodah. Applied Therapeutics, the Clinical
    use of Drugs, 4th editions, 1989
  • www.infectionacademy.org/meetings/berlin_presentat
    ions/Suttorp_Berlin.ppt -
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