the war on drugs: the mythology of antibiotics edward l. goodman, md, facp, fidsa, fshea may 9, 2005
TRANSCRIPT
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The War on Drugs:The Mythology of Antibiotics
Edward L. Goodman, MD, FACP, FIDSA, FSHEA
May 9, 2005
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An Epidemic of Drastic Proportions: demographics
• Affects people of all ages– Disproportionately involves the very young and very
old
– Involves the more affluent and well insured
• Costs in the billions– Producers reap huge profits
– Pushers are among elite
– Users are not addicted• Sometimes still demand a drug fix
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Effects of the Epidemic
• Direct toxicity of the drugs– Diarrhea from most– Deafness from a few– Renal failure from quite a few– Skin rash from all– Secondary infections from all– IV phlebitis from all
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Indirect Effects: Secondary Infections
• Pneumonia– Vent associated
• Bacteremia/fungemia– Line associated
• MDR Urinary tract infections– Catheter associated
• Prolonged hospital stay• Excessive costs
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Description of “Pushers”
• Well educated• Well intentioned• Extremely Defensive
– Fearful of lawyers– Use that as an excuse
• Forgetful– Forgotten lessons of graduate school
• Addicted to the culture of cultures
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The Truth
• Producers = PHARMA
• Pushers = physicians
• Victims = all of us
• Drugs = antimicrobials
• Root Causes = ignorance of microbiology, epidemiology, pharmacology
• DRUGS OF FEAR
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More of the Truth
• Antibiotic use (appropriate or not) leads to microbial resistance
• Resistance results in increased morbidity, mortality, and cost of healthcare
• Antibiotics are used as “drugs of fear” (Kunin et al. Annals 1973;79:555)
• Appropriate antimicrobial stewardship will prevent or slow the emergence of resistance among organisms (Clinical Infectious Diseases 1997; 25:584-99.)
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Antibiotic Misuse
• Published surveys reveal that:– 25 - 33% of hospitalized patients receive
antibiotics (Arch Intern Med 1997;157:1689-1694)
– At PHD during 1999, 2000 and 2001, 50-60% of patients received antibiotics
– 22 - 65% of antibiotic use in hospitalized patients is inappropriate (Infection Control 1985;6:226-230)
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Consequences of Misuse of Antibiotics
• Contagious RESISTANCE– Nothing comparable for overuse of
procedures, surgery, other drugs
• Morbidity - drug toxicity• Mortality - MDR bacteria harder to treat• Cost
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Appropriate Use of Antibiotics
• Need 8-10 lectures
• Many useful reference sources– Sanford Guide (hard copy or electronic)– Epocrates (epocrates.com)– Hopkins abx-guide (hopkins-abx.guide.org)– ID Society – practice guidelines (idsociety.org)
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Inappropriate Use of Antibiotics
• Asymptomatic UTI in non pregnant patients• “Acute sinusitis” before trial of 7-10 days of
symptomatic treatment (NEJM 8/26/04)• Respiratory cultures when there is no clinical
evidence of pneumonia• Positive catheter tip cultures when no bacteremia• Coagulase negative staph in single blood cultures• FUO with no clinical site of infection• Prophylaxis for surgery beyond 24 hours
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More Inappropriate Uses
• Aseptic meningitis when already pretreated– Consider observe 6-8 hours, then retap
• Abnormal CXR when no clinical symptoms for pneumonia
• Swabs of open wounds growing potential pathogens
• THE LIST COULD GO ON FOREVER!
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Antibiotic Myths
• More is better
• IV is better than oral
• Longer duration is better
• Multiple drugs are better
• Vancomcyin: a whole mythology of its own
• Miscellaneous
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Is More Better?
• What does “more” (higher doses) accomplish?– Higher serum levels, and thus
– Higher tissue levels
• But when are higher levels needed?– Privileged sanctuary where drugs penetrate poorly
• CSF/vitreous
• Heart valve vegetations
• Implants/prostheses/biofilms
– Defenseless host
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Pharmacodynamics
• MIC=lowest concentration to inhibit growth
• MBC=the lowest concentration to kill
• Peak=highest serum level after a dose
• AUC=area under the concentration time curve
• PAE=persistent suppression of growth following exposure to antimicrobial
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Parameters of antibacterial efficacy
• Time above MIC - beta lactams, macrolides, clindamycin, glycopeptides
• 24 hour AUC/MIC - aminoglycosides, fluoroquinolones, azalides, tetracyclines, glycopeptides, quinupristin/dalfopristin
• Peak/MIC - aminoglycosides, fluoroquinolones
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Time over MIC associated with better killing
• Should exceed MIC for at least 50% of dose interval for beta lactams and vancomycin
• Higher doses may allow longer time over MIC
• For most beta lactams, optimal time over MIC can be achieved by continuous infusion (except unstable drugs such as imipenem, ampicillin)
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Please see full prescribing information.Please see full prescribing information.
32
Clarithromycin Extended-Release Tablets Allow for Convenient QD DosingClarithromycin Extended-Release Tablets Allow for Convenient QD Dosing
Once-daily dosing with clarithromycin extended-release tablets provides equivalent 24-hour area under the curve (AUC) for both clarithromycin and its active metabolite, 14-OH clarithromycin, relative to an equal dose of clarithromycin tablets, which is dosed BID1
Once-daily dosing with clarithromycin extended-release tablets provides equivalent 24-hour area under the curve (AUC) for both clarithromycin and its active metabolite, 14-OH clarithromycin, relative to an equal dose of clarithromycin tablets, which is dosed BID1
Reference: 1. Biaxin/Biaxin XL package insert, Abbott Laboratories.Reference: 1. Biaxin/Biaxin XL package insert, Abbott Laboratories.
*Mean plasma concentrations obtained in nonfasting state in healthy volunteers*Mean plasma concentrations obtained in nonfasting state in healthy volunteers
Steady-State Clarithromycin Plasma Concentrations-Time Profiles*1
Mea
n Pl
asm
a C
once
ntra
tions
(µg/
mL)
Time After Dosing0 4 h 8 h 12 h 16 h 20 h 24 h
0.0
1.0
2.0
3.0
4.0 BIAXIN XL (clarithromycin extended-release tablets) 2 x 500 mg QDBIAXIN (clarithromycin tablets, USP) 500 mg QD
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Higher serum/tissue levels are associated with faster killing
• Aminoglycosides – Peak/MIC ratio of >10-12 optimal
– Achieved by “Once Daily Dosing”
– PAE helps
• Fluoroquinolones – 10-12 ratio achieved for enteric GNR
• PAE helps
– not achieved for Pseudomonas
– Not always for Streptococcus pneumoniae
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AUC/MIC = AUIC
• For Streptococcus pneumoniae, FQ should have AUIC >= 30
• For gram negative rods where Peak/MIC ratio of 10-12 not possible, then AUIC should >= 125.
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CCmaxmax (peak) (peak)
Time above MICTime above MIC
AUCAUC
MICMIC9090
Time (h)Time (h)
An
tib
ioti
cA
nti
bio
tic
seru
m c
on
cen
trat
ion
seru
m c
on
cen
trat
ion
MICMIC
Pharmacodynamic Parameters Pharmacodynamic Parameters of Fluoroquinolonesof Fluoroquinolones
AUCAUC
• For optimal antimicrobial For optimal antimicrobial effect:effect:– C– Cmaxmax/MIC should be /MIC should be
> 8-10> 8-10oror
• – – AUC/MIC should be AUC/MIC should be > 125 for GNR, >30 for > 125 for GNR, >30 for
GPCGPC
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“More is Better” continued
• Since beta lactams don’t kill any better at higher concentrations– Why give them IV?– Why increase dose?– Just give often enough
• Confounding factor– Higher dose gives higher serum levels which
may exceed MIC for longer time
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When is IV better than enteral?
• Patient unable to take enteral meds/food
• Patient unable to absorb enterally– Short bowel syndrome– Malabsorption– Vascular collapse– Ileus
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“Completely” BioavailableIV and enteral essentially identical
GIVE ENTERALLY IF POSSIBLE
• Respiratory quinolones (90-98%)
• Fluconazole (90%)
• Trimethoprim sulfa (85%)
• Metronidazole (90%)
• Doxycycline/minocycline (93/95%)
• Clindamycin (90%)
• Linezolid (100%)
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Well Absorbed No IV formulation to compare
• Cephalexin (90%)• Amoxycillin (75%)• Dicloxacillin (50%)• Clarithromycin (50%)
• Since none of these are concentration dependent, enteral therapy should suffice if levels >MIC for >50% dosing interval– Easily achieved for these agents
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Is Longer Duration Better?
• In every study comparing two lengths of therapy, shorter is as good– Two weeks Pen & Gent for viridans strept SBE = 4
weeks of Pen alone– Two weeks of PO Cipro and Rif for right sided OSSA
endocarditis = 4 weeks of IV Nafcillin– Five days of Levaquin 750 for CAP = 10 days of 500
daily (CID 10/03)– Eight days Rx for HAP (non Pseudomonas) = 14 days
(ATS/IDSA 1/05)– Three days of T/S or FQ for cystitis = 10 days
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Is Longer Worse?
• Increases antibiotic resistance
• Exposes patient to more toxicity
• Increases cost
• May actually increase the risk of some infections
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When are Multiple Antibiotics Indicated?
• Empiric therapy when organism(s) not known
• For mixed infections when one drug won’t cover
• For synergy
• To retard or prevent the development of resistance
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When is Synergy Needed?
• If it allows reduction in dosage of toxic components of a combination– Flucytosince with AMB can shorten the course
and lower the dose of AMB for Crypto meningitis (non HIV patients)
– No other good example
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Synergy Needed
• When monotherapy is not bactericidal– Enterococcal endocarditis
• Neither penicillin nor aminoglycoside are ‘cidal by themselves
• When combined ‘cidal activity produced
– Other enterococcal infections do not need ‘cidal therapy including bacteremia unassociated with IE
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When is Cidal Therapy Needed
• Bacterial Endocarditis
• Bacterial Meningitis
• Maybe neutropenic or immunocompetent host
• Maybe osteomyelitis
• Not for almost all other bacterial infections
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When are Multiple Drugs Needed to Prevent/Retard Development of
Resistance?• HIV therapy
• Chemotherapy of active TB
• ? Severe P. aeruginosa bacteremia/ pneumonia– No real data that dual Rx prevents emergent
beta lactam resistance– Instead it provides a second drug in case beta
lactam resistance emerges
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Vancomycin Myths
• “Ultimate drug for gram positive”– Clearly inferior to Nafcillin for sensitive staph– Slowly bactericidal– High failure rate in MRSA infections– Will likely be supplanted by Daptomycin/Linezolid
• “Vancomycin is a toxic drug”– No clear evidence of renal or oto-toxicity in monoRx– When combined with aminoglycoside, 30-40% risk of
toxicity
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More Vanco Myths
• “Must do serum levels” (predicted on prior myth)– Non concentration dependent
• So peaks unnecessary except for meningitis
– No correlation with efficacy/toxicity ever demonstrated in literature
– Cannot measure true peaks • Long alpha phase• Must do log decay curve
• Troughs may allow less frequent dosing
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More Myths
• Keflex is still a appropriate for outpatient SSI, respiratory infections– >50% of staph aureus are MRSA– Poor activity vs. pen resist pneumococcus,
Hemophilus
• Fluoroquinolones are superior for UTI, sinusitis, bronchitis, pneumonia– Not unless resistant organisms
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The Solution
• Vaccinate against preventable infections• Reduction in promiscuous cultures
– Lead to unnecessary Rx
• Antimicrobial stewardship– Restriction of drugs by
• Payors• Antimicrobial Management Programs
• EDUCATION• Computerized Physician Order Entry