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GLEM - 9-1-2007 Use and misuses of fluoroquinolones 1 The good and the bad uses of fluoroquinolones in Urology Paul M. Tulkens Unité de pharmacologie cellulaire et moléculaire & Centre de Pharmacie clinnique Université catholique de Louvain International Society for Anti-infective Pharmacology (ISAP) www.facm.ucl.ac.be www.isap.org
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  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 1

    The good and the bad uses of fluoroquinolones in Urology

    Paul M. TulkensUnité de pharmacologie cellulaire et moléculaire

    & Centre de Pharmacie clinniqueUniversité catholique de Louvain

    International Society for Anti-infective Pharmacology (ISAP)

    www.facm.ucl.ac.bewww.isap.org

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 2

    Are antibiotics following a path to madness ?

    discovery in soil bacteria and fungi

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 3

    Are antibiotics following a path to madness ?

    and then we all saw the blooming tree of semi-synthetic and totally synthetic antibiotics

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 4

    Are antibiotics following a path to madness ?

    and the General Surgeon told us that the fighth was over

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 5

    Are antibiotics following a path to madness ?

    ButBut……

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 6

    Antibiotics and resistance...

    • Is there a problem ?Rising resistance and correlation with antibiotic use …

    • Resistance in urinary nosocomial isolates …what about quinolones uses in the community and the hospital ?

    • What are quinolones (adavantages – downsides) ?what are appropriate uses … and misuses ?

    • Can this also reduce health care costs ? …

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 7

    Overuse is one of the problems …the classical situation in the community …

    Risk of resistance to β-lactams among invasive isolates of Streptoccus pneumoniae regressed againstoutpatient sales of beta-lactam antibiotics in 11 European countries• resistance data are from 1998 to 1999; antibiotic sales data 1997. • DDD = defined daily doses

    Bronzwaer SL, Cars O, et al. Emerg Infect Dis 2002 Mar;8(3):278-82

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 8

    Organisms and resistance in nosocomial urological specimens …

    E. coliPseudomonasEnteroccusKlebsiellaEnterobacterProteusCN S.Candida0thers

    Johansen et al. Intern. J. Antimicrob. 2006; 28,Suppl.1:91-107A study from the European Society of Infections in Urology (ESIU)

    Distribution of microbial species in 486 patients with

    nosocomially acquired urinary tract infection

    asymptomaticcystitispyelonephritisurosepsisothersunknown

    E. coli

    asymptomaticcystitispyelonephritisurosepsisothersunknown

    P. aeruginosa

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 9

    Organisms and resistance in nosocomial urological specimens …

    Amoxiclav S I R

    2d-3d gen. cephalosporin S I R

    ciprofloxacin S I R

    Resistance of E. coli

    to amoxiclav

    to 2d/3d gen. cephalosp.

    to ciprofloxacinJohansen et al. Intern. J. Antimicrob. 2006; 28,Suppl.1:91-107A study from the European Society of Infections in Urology (ESIU)

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 10

    Resistance of P. aeruginosa (all origins *)

    Mesaros et al. CMI, in press; http://www.facm.ucl.ac.be

    * no recent and global specific data on NAUTI…

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 11

    Do we use too much Gram (-) fluoroquinolones in Belgium ?

    principaux antibiotiques

    0

    1,000,000

    2,000,000

    3,000,000

    4,000,000

    5,000,000

    6,000,000

    7,000,000

    Jan-

    97

    May

    -97

    Sep

    -97

    Jan-

    98

    May

    -98

    Sep

    -98

    Jan-

    99

    May

    -99

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    -99

    Jan-

    00

    May

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    Jan-

    01

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    -01

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    May

    -02

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    May

    -03

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    04

    May

    -04

    Sep

    -04

    Jan-

    05

    May

    -05

    DD

    D

    beta-lactamestetracyclinesmacrolidesquinolones Gram -quinolones Gram +sulfa-trimet

    A: in the community per month

    DD

    D /

    mon

    th (w

    hole

    cou

    ntry

    )

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 12

    Do we use too much Gram (-) fluoroquinolones in Belgium ?

    A: in the community : trends over yearstotal par classe et par an

    0

    10,000,000

    20,000,000

    30,000,000

    40,000,000

    50,000,000

    60,000,000

    70,000,000

    80,000,000

    90,000,000

    100,000,000

    mai97-98 mai98-99 mai99-00 mai00-01 mai01-02 mai02-03 mai03-04 mai04-05

    DD

    D

    totalbeta-lactamestetracyclinesmacrolidesquinolones anti Gram-quinolones anti Gram+sulfa-trimet

    DD

    D /

    year

    (who

    le c

    ount

    ry)

    total≈ 25

    DDDper 1,000 inh.per day

    all FQ≈ 3

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 13

    Use of quinolones in the Community in Europe …

    Outpatient use of quinolones in 25 European countries in 2003*

    Blue error bar represents the difference in national quinolone use in 2003 expressed in DID between ATC/DDD versions 2004 and 2003 due to the change of DDD for levofloxacine from 250 to 500 mg.

    * For Iceland total data are use; for Poland 2002 data are used.

    0.0

    0.5

    1.0

    1.5

    2.0

    2.5

    3.0

    3.5

    4.0Po

    rtuga

    l

    Italy

    Bel

    gium

    Luxe

    mbo

    urg

    Spai

    n

    Fran

    ce

    Gre

    ece

    Hun

    gary

    Cro

    atia

    Slov

    akia

    Aus

    tria

    Slov

    enia

    Pola

    nd

    Cze

    ch R

    ep.

    Ger

    man

    y

    Swed

    en

    Isra

    el

    Finl

    and

    Net

    herla

    nds

    Irela

    nd

    Icel

    and

    Esto

    nia

    UK

    Nor

    way

    Den

    mar

    k

    DD

    D /

    1000

    inha

    bita

    nts/

    day

    Third-generation

    Second-generation

    First-generation OfloxacinCiprofloxacinLevofloxacin

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 14

    Use of quinolones in Hospitals in Europe …

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 15

    Antibiotics given in nosocomial urinary tract infections(hospitalized patients)

    0

    5

    10

    15

    20

    25

    30

    35

    40

    45

    beta-lact aminogl. fluoroquin. CTZ/TMP

    GermanyRest of EuropeWorld%

    use

    d

    Johansen et al. Intern. J. Antimicrob. 2006; 28,Suppl.1:91-107A study from the European Society of Infections in Urology (ESIU)

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 16

    Thus, we are facing a problem… and looking for a solution …

    • Resistance rates are strong arguments for a critical antimicrobial policy

    • Empiric therapy has to be initiated rapidly but culture must be taken before.

    • Adjustment is important …

    • Prophylaxis and treatment must be based on a continuous surveillance in Urology departments.

    • Collaboration between urologists and microbiologists is decisive for good infection control.

    • Facilities for preliminary culture of pathogens inside the urological ward may be useful

    Johansen et al. Intern. J. Antimicrob. 2006; 28,Suppl.1:91-107A study from the European Society of Infections in Urology (ESIU)

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 17

    Where do we go from now ?

    • Understand what quinolones are ?

    • Are they causing more resistance ?

    • What could be their limits

    • What do guidelines say ?

    • Do we use too much ?

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 18

    Which (fluoro)quinolones ?

    • norfloxacin --• ciprofloxacin ++• pefloxacin -• ofloxacin +

    • nalidixic acid

    • levofloxacin + (S-isomer of ofloxacin)

    • moxifloxacin ++• gatifloxacin

    Gram - Gram +

    2000

    1965

    trovafloxacin

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 19

    Main useful pharmacological properties and drawbacks ?

    On the positive side• bactericidal• concentration (Cmax) and dose (24h-AUC)-dependent, allowing for rational

    fine tuning of the therapy including against resistant strains, based on simple rules for posology…

    Cmax/MIC > 10; 24h-AUC/MIC > 125 • good tolerance in general • excellent bioavailability (rapid oral switch possible…)

    On the negative side• a few side effects that require attention (tendinitis, CNS, ...) and

    incompatibility with divalent traivalent cations (Ca++, Al+++)• emergence of resistance

    – target mutation (relatively easy ...)– unanticipated cross-resistances due to efflux…– breakpoints (limits of susceptibility) have been set historically to high (NCCLS),

    are better with EUCAST, but still need attention

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 20

    Quinolones side effects...

    Van Bambeke F, Michot JM, Van Eldere J, Tulkens PM. Quinolones in 2005: an update. Clin Microbiol Infect. 2005 Apr;11(4):256-80. PMID: 15760423

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 21

    Quinolones side effects...: which are the populations (really) at risk ?

    • pregnant women and children

    • elderly, especially with corticoid therapy

    • athletes in training (beware of the runners...)

    • co-administration of NDSAIDs or drugs known for potential of CytP450 interactions

    • heart disease

    • patients receiving neutralization anti-acids (Ca++/ Mg++ / Al+++) or Fe++

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 22

    Resistance…

    • long thought to be restricted to chromosomic mutations of the targets (DNA gyrase / topoisomerase)

    – high frequency of spontaneous mutations (10-7)

    – but limited horizontal and interbacterial spread …

    • but, later on, observed in relation to decreased accumulation– loss of porins in Gram (-) bacteria

    – (over)expression of efflux

    • now, seen through plasmidic-associated mechanisms (QnR)– risk of rapid horizontal spread …

    • and very recently though fluoroquinolone-modifying enzymes !! (clinical significance still uncertain…)

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 23

    Resistance by target mutation: parallel and dissociated resistance and strong-versus weak fluoroquinolones

    weak

    stronger

    dissociated

    susceptibility limit (arbitrary)

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 24

    Application: look at MIC distributions where YOU are …to find "weak" quinolones

    0

    50

    100

    1500

    0,02

    0,06

    0,19 0,5

    1,5 4 12 32

    oflox levo cipro

    MIC distributions in Leuven…

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 25

    0.01 0.10 1.00 10.00

    10-2

    1

    concentration

    10-4

    10-6

    10-8

    10-10 MPC 10 = 9

    Dong et al: AAC 1999; 43:1756-1758

    Mutant Prevention Concentration …

    "Classic" bactericidal effect

    Elimination of resistantorganisms

    Surv

    ivin

    g ba

    cter

    ia

    MIC 99 = 0.8

    poorly sensitive organisms…

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 26

    0.01 0.10 1.00 10.00

    10-2

    1

    concentration

    10-4

    10-6

    10-8

    10-10 MPC 10 = 9

    Dong et al; AAC 43:1756-1758

    Mutant Prevention Concentration …Su

    rviv

    ing

    bact

    eria

    MIC 99 = 0.8Concentration which will inhibit the majorityof the organisms

    Concentration needed to prevent the selection of resistant organisms

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 27

    "Window" where selection of mutants/resistantsmay take place …

    Time after administration

    MIC

    MPC

    conc

    entra

    tion

    MSW

    concept from Drlica & Zhao, Rev. Med. Microbiol. 2004, 15:73-80

    Mutation selection window

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 28

    Mutant Prevention Concentration of ciprofloxacin and levofloxacinin P. aeruginosa (clinical isolates) with "normal" susceptibility

    (MIC = 0.33 and 0.9 mg/L) …

    cipro levo

    MPC cipro = 3Cmax ∼ 2.5 µg/ml

    MPC levo = 9.5(Cmax ∼ 5 µg/ml

    Hansen et al. I.J.Antimicrob. Agents 2006;27:120-124

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 29

    Efflux and MIC ?• efflux is a universal mechanism for cell

    protection against membrane-diffusing agents• many drugs diffuse though membranes and

    become opportunistic substrates of efflux pumps

    • for AB, efflux decreases the amount of drug in bacteria and impairs activity, increasing the MIC …

    • insufficient drug exposure favors the selection of less sensitive organisms

    the increase in MIC is modest and often leaves the strain categorized (falsely …) as "sensitive"…true MIC determination may, therefore, become more and more critical … Van Bambeke et al.

    J Antimicrob Chemother. 2003;51:1055-65.

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 30

    How does efflux work (Gram - bacteria) ?

    periplasm

    porin

    cytosol

    susceptible bacteriaresistant bacteria

    pump

    pore

    lipoprotein

    H+

    H+

    expressed in wild-type strains!

    MexB

    MexA

    OprM

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 31

    How does efflux work (Gram - bacteria) ?

    periplasm

    porin

    cytosol

    susceptible bacteriaresistant bacteria

    pump

    pore

    lipoprotein

    H+

    H+

    expressed in wild-type strains!

    MexB

    MexA

    OprM

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 32

    Why do you need to detect efflux ?

    how many of your samples would actually fall here ….

    But will be brought back to wild type distribution in the presence of efflux inhibitor ...

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 33

    Application: look at MIC distributions where YOU are …

    0

    50

    100

    1500

    0,02

    0,06

    0,19 0,5

    1,5 4 12 32

    oflox levo cipro

    MIC distributions in Leuven…

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 34

    Application: look at MIC distributions where YOU are …

    0

    50

    100

    1500

    0,02

    0,06

    0,19 0,5

    1,5 4 12 32

    oflox levo cipro

    MIC distributions in Leuven…EUCAST limit of "wild" population

    efflux…

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 35

    Why does efflux cause cross-resistance ?(example with P. aeruginosa)

    MexAB-OprM

    MexCD-OprJ

    MexEF-OprN

    MexHI-OprD

    MexJK-OprM

    MexXY-OprM

    β-lac ML TET AG FQ Chl

    Van Bambeke et al. JAC (2003) 51:1055-65; Aeschlimann, Pharmacotherapy (2003) 23:916-24

    constitutive expressioninducible expression

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 36

    Fluoroquinolones: get a peak and an AUC !

    Time (h)

    Con

    cent

    ratio

    n

    MIC

    in order to optimize: AUC24h/MIC Cmax/MIC

    should be > 125 *

    should be > 10

    Get both a peak and a AUC !!

    • Cmax = Dose / Vd• AUC = Dose / Clearance

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 37

    Application: choose a strong quinolone and use low enough break-points … or better … ask for an MIC and use PK/PD …

    Van Bambeke F, Michot JM, Van Eldere J, Tulkens PM. Quinolones in 2005: an update. Clin Microbiol Infect. 2005 Apr;11(4):256-80. PMID: 15760423

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 38

    Fluoroquinolones downsides in a (scientific) nutshell and how to cope with them

    • true risk of emergence of resistancehave local epidemiological surveyshave cultures and susceptibility data (MIC) for all isolates in difficult situationsdose appropriately ...use potent (not weak) quinolones...do not use if not needed...

    • a few side effectsavoid populations at risk

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 39

    How do we go from here to clinical practice ?

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 40

    How do we go from here to clinical practice ?

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 41

    How do we go from here to clinical practice ?

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 42

    How do we go from here to clinical practice ?

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 43

    What about Belgium ?

    Ampe et al., 15th ECCMID, 2005

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 44

    Complicated cystitis:

    Empiric therapyLarge spectrum antibiotic • First choice:

    fluoroquinolone– Large spectrum– High concentratie in urine

    and urinary tract

    Directed therapy• According to the results of

    the antibiogram• Choose antibiotic with the

    smallest spectrum

    Duration of treatment: 7 to 14 days

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 45

    Mild pyelonephritis• Empiric therapy

    First choice:• Oral fluoroquinolon in monotherapy• Ambulant therapy if possible:

    – Patient can take oral medication– No severe sepsis– No renal insufficiency

    • No association of aminoglycoside except in severe sepsis • No first generation fluoroquinolone because of low serum concentrations• No ampicillin or first generation cephalosporins (or co-trimoxazole)

    because of resistance pattern in Belgium

    – If contra-indication to fluoroquinolones:• amoxicillin-clavulanic acid• Second generation cephalosporins• temocillin

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 46

    Severe pyelonephritis (hospital)

    • Empiric therapy– first choice:

    • Fluoroquinolone• Initially parenteral therapy• Switch IV-oral and ambulant

    therapy when possible– Alternatives:

    • Temocillin• Second generation

    cephalosporin• Amoxicilline-clavulanic acid• if septic shock:

    Association of aminoglycoside to cephalo-2 or amoxiclav

    Directed therapyBased on urine culture with

    antibiogram– first choice :

    • Fluoroquinolone• Cotrimoxazol• Only if enterococ:

    – amoxicillin– ampicillin– If necessary combination with

    aminoglycoside

    – Ambulant therapy: see next slide

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 47

    Switch IV-per os and ambulant treatment

    • Based on:– Clinical recovery (symptoms and fever disappeared)– Antibiogram of the urine culture– If possible after 24-48 h– Ambulant therapy if possible:

    – Patient can take oral medication– No severe sepsis– No renal insufficiency

    – Patients who fail to improve after 48-72 h of ambulant therapy based on urine culture and the initial antibiotic:

    • parenteral fluoroquinolone or• alternative

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 48

    Regimens

    Antibiotic duration dose

    Ciprofloxacin 7 – 14 days* 250-500 mg X 2, po200-400 mg X 2, IV

    Levofloxacin 250-500 mg X1, po or IVOfloxacin 200-400 mg X1, po or IV

    Amoxi-clav 14 days 500 mg X 3, po1 g X 4, IV

    Cefuroxim 500 mg X 2, po750 mg – 1.5 g X 3, IV

    Temocillin 1 g X 2, IVCotrimoxazol 160/800 mg X2, po of IVAmpicillin 1 g X 4, IVAmoxicillin 400 mg X 3 of X 4, po

    BAPCOC guidelines, 2002* 7 days: mild infection; 14 days: severe infection

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 49

    Severe pyelonephritis in the pregnant woman

    • allowed

    – Nitrofurantoin– Cephalosporins– Amoxicillin– Cotrimoxazol (folic acid

    antagonism minimal if short treatment using recommanded dose)

    • Not allowed

    – Fluoroquinolones– Cotrimoxazol during last

    weeks of pregnancy (risic op hyperbilirubinemia and icterus in the neonatus)

    – Fosfomycin (avoid during first 3 months)

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 50

    Acute prostatis : treatment

    First choice:• Fluoroquinolones

    – Ciprofloxacin if suspicion of P. aeruginosa, 500 mg X 2 po

    Second choice :• Cotrimoxazol, 800/160 mg X 2 poAlternatieves:• Cephalosporins (cefuroxim)• Amoxicillin + clavulanic acid

    Minimal duration : 2 weeks, often 4 weeks (prevention of chronic infection)

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 51

    Chronic prostatis: treatment

    Problems:• Little antibiotics penetrate well in the non-

    inflammated prostate• Infection focus can consist of little calculi or

    abcesses that are difficult to treat.• High probability of relapsing infections

    DIFFICULT TO TREAT

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 52

    Chronic prostatis: antibiotic treatment

    Primary antibiotics• Only lipophilic and basic molecule penetrate the acidic

    environnement of the prostate:

    – Good for: • ciprofloxacin: (500 mg 2X/day): 30 days • Trimethoprim (800/160 mg 2x/day): 3 months• Macrolides (not for empiric therapy because of spectrum)

    – Bad for: • penicillins • cephalosporins • Tetracyclins• Nitrofurantoin• vancomycin

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 53

    A clinical algorithm ...

    Knowledge or ou“educated” suspicion of the causative agent

    Pathology andepidemiology Local MIC data

    Is the organism probably highly

    susceptible ?

    Obtain an MIC

    no

    Use common dosage but with attention to PK/PD

    yes

    Adjust the dosage on a full PK/PD basis

    S / I / Ris

    insufficient !!

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 54

    Success ?

    re-evaluate• the dosage• the therapeutic scheme• the antibiotic classbased on PK/PD properties

    no

    Consider step-down therapy

    if acceptable on a microbiological point of view

    yes

    A clinical algorithm (follow.) ...

    Use these pieces of information to establish recommendations based on local epidemiology and on the knowledge of the

    PK/PD properties and of the risk for resistance

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 55

    And what about health care costs ?

    • Pharmacoeconomics of antibiotics is still largely underdeveloped outside the USA (but US-based models cannot easily be applied);

    • However, comparisons identifying differences in – amount of money needed to reach a given (better ? ) clinical outcome; – expenses related to the same (or better) quality of life and patient's satisfaction;

    may already suggest interesting avenues for further fine-tuning therapeutic guidelines

    PharmacoeconomicsPharmacoeconomics

    Economic• cost minimization• cost benefit• cost effectiveness• cost utility

    Economic• cost minimization• cost benefit• cost effectiveness• cost utility

    Humanistic• quality of life• patient's preference• patient's satisfaction

    Humanistic• quality of life• patient's preference• patient's satisfaction

    L. Sanchez, In Pharmacotherapy, DiPiro et al. eds, p.2, 1999

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 56

    Prices in Belgium…total par classe et par an

    0

    25,000,000

    50,000,000

    75,000,000

    100,000,000

    125,000,000

    150,000,000

    mai97-98 mai98-99 mai99-00 mai00-01 mai01-02 mai02-03 mai03-04 mai04-05

    NET

    totalbeta-lactamestetracyclinesmacrolidesquinolones anti Gram-quinolones anti Gram+sulfa-trimet

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 57

    Rational bases for the choice of an antibiotic

    • Know your LOCAL epidemiology

    obtain MIC distributions from your microbiologists…

    • know the PK profile of the drugs you consider to purchase

    aim at obtaining > 90 % efficacy against the organisms of interest (AUC, peak, time above MIC) with a standard dosage, …

    • include a safety margin (MPC …)

    • Compare products on that basis first …

    • Remember that • no antibiotic (if possible) is the best…• but that treatment failures (when treatment is needed) cost a lot …

    (so that cheap but 2d class antibiotics may not be a bargain...)

  • GLEM - 9-1-2007Use and misuses of fluoroquinolones 58

    Please, act rationally…

    www.facm.ucl.ac.be

    F. Van Bambeke, Pharm.Y. Glupczynski, MDA. Spinewine, Pharm.S. Carryn, Pharm.E. Ampe, Pharm....

    W.A. Craig, MDM.N. Dudley, Pharm.G.L. Drusano, MDJ.J. Schentag, Pharm.A. McGowan, MDX. Zao, PhDV. Firsov, MDS. Zinner, MDA. Dalhoff, PhD...

    www.isap.org

    The good and the bad uses of fluoroquinolones in UrologyAre antibiotics following a path to madness ?Are antibiotics following a path to madness ?Are antibiotics following a path to madness ?Are antibiotics following a path to madness ?Antibiotics and resistance...Overuse is one of the problems …�the classical situation in the community …Organisms and resistance in nosocomial urological specimens …Organisms and resistance in nosocomial urological specimens …Resistance of P. aeruginosa (all origins *)Do we use too much Gram (-) fluoroquinolones in Belgium ? Do we use too much Gram (-) fluoroquinolones in Belgium ? Use of quinolones in the Community in Europe … Use of quinolones in Hospitals in Europe … Antibiotics given in nosocomial urinary tract infections�(hospitalized patients) Thus, we are facing a problem… and looking for a solution …Where do we go from now ?Which (fluoro)quinolones ?Main useful pharmacological properties and drawbacks ?Quinolones side effects...Quinolones side effects...: �which are the populations (really) at risk ?Resistance…Resistance by target mutation: parallel and dissociated resistance and strong-versus weak fluoroquinolonesApplication: look at MIC distributions where YOU are …�to find "weak" quinolonesMutant Prevention Concentration …Mutant Prevention Concentration …"Window" where selection of mutants/resistants �may take place …Mutant Prevention Concentration of ciprofloxacin and levofloxacin in P. aeruginosa (clinical isolates) with "normal" susceptiEfflux and MIC ?How does efflux work (Gram - bacteria) ? How does efflux work (Gram - bacteria) ? Why do you need to detect efflux ? Application: look at MIC distributions where YOU are …Application: look at MIC distributions where YOU are …Why does efflux cause cross-resistance ?�(example with P. aeruginosa) Fluoroquinolones: get a peak and an AUC !Application: choose a strong quinolone and use low enough break-points … or better … ask for an MIC and use PK/PD …Fluoroquinolones downsides in a �(scientific) nutshell and how to cope with themHow do we go from here to clinical practice ?How do we go from here to clinical practice ?How do we go from here to clinical practice ?How do we go from here to clinical practice ?What about Belgium ?Complicated cystitis:Mild pyelonephritisSevere pyelonephritis (hospital)Switch IV-per os and ambulant treatmentRegimens Severe pyelonephritis in the pregnant womanAcute prostatis : treatmentChronic prostatis: treatmentChronic prostatis: antibiotic treatment A clinical algorithm ...A clinical algorithm (follow.) ...And what about health care costs ?Prices in Belgium…Rational bases for the choice of an antibioticPlease, act rationally…


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