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Clostridium difficileBATAM bijeenkomst
17 mei 2013Dr DJ Bac, MDL-arts
Dr MA Schouten, arts-microbioloog
CDI
• Berucht vanwege ribotype 027• Diverse uitbraken sinds 2000• Toename morbiditeit + mortaliteit + kosten
Clostridium difficile
• Gram positieve anaerobe staaf• Produceert sporen• Produceert toxines• Nr 1 oorzaak nosocomiale diarree
Risk factors clostridium difficile
• Ziekenhuis opname• Antibiotica:• > 65 jaar
• IBD• PPI ?? • sonde voeding• diverticulose• chemotherapie• (GI) chirurgie• dialyse
Epidemiologie clostridium difficile
Drager• Gezonde personen ~3%• Ziekenhuis ~20% • Jonge kinderen tot 80%
Diarree• Hospital-acquired: ~ 10 %• Community-acquired: ~ 1,5-2 %
1e lijns probleem?
• Clostridium difficile infection: it’s a family affairUK 2007-2012: 238 patiënten met CDI; verspreiding na ontslag? slechts in 3 gevallen verspreiding thuis (1)
• Community-associated Clostridium difficile infection: How real is it? (2)Studie CDC: CA= diarree niet voorafgegaan door ziekenhuis bezoek afgelopen 3 maanden, >10.000 gevallen; 32% CA: hiervan 25% opgenomen na vaststellen CDI, recurrence rate 9%, PFGE type NAP1, NAP11, NAP4Risicofactoren CA CDI: AB gebruik, protonpomp remmersliteratuur: vlees, huisgenoten met CDI, kinderen < 2 jaar.
1: ICHE 2013, 2: Anaerobe 2013
1e lijns probleem?• Clostridium difficile carriage in healthy infants in the community
asymptomatisch dragerschap volwassenen 1-7%Kinderen tot 2 jaar 2-75% drager maar zelf zelden ziekStudie: 10 gezonde kinderen van 1 jaar gevolgd + screening 2 dagopvangcentraAlle 10 verwerven CD en bleven maanden POS
Dagverblijf 45% van de 85 kinderen CD POSRisicofactoren: ab gebruik, gebruik ab moeder zwangerschap, verandering voeding (met name bij verdwijnen Bifidobacterium cave melk / BV minder CD, flesvoeding meer CD)Geen relatie met aantal siblings of dierenRecente ziekenhuis opname enige risicofactor voor kolonisatie pathogene stam
CID 2012
1e lijns probleem?• Clostridium difficile contamination of public tap water distribution system
during a waterborne outbreak in Finland• Nov-dec 2007 drinkwater Nokia gecontamineerd met rioolwater• Grote uitbraak gastro-enteritis; Rol Clostridium difficile ?
10.000 inwoners, 8000 ziek, 1000 behandeld, 17 CD POS (65 getest)• 12 CD isolaten gevonden in water (5 kraanwater, 7 riool)• Aantal malen zelfde stam in water en patiënt
SAGE 2013
Dieren• Clostridium difficile infection in the community: a zoonotic disease? (1)• Review LUMC; CD komt zowel bij mensen als dieren voor; verschillende
biotypes• Bij vinden nieuwe types als verwekker humane infecties dan zoeken naar
dierlijk reservoir• Clostridium difficile in faeces from healthy dogs and dogs with diarrhea (2)• Stockholm;
50 gezonde honden: 2 met CD; niet toxine producerend20 honden met diarree: 2 met CD; toxine producerend, humane types
1: CMID 2012, 2: AVS 2013
Voeding• Detection of Clostridium difficile in retail ground meat products in
Manitoba• 48 porties vlees (rund en varken); 6,3% CD POS• Verschillende types; wel allemaal bekend humane toxine producerende
stamen
JIDM 2012
DJB: klinisch beeld
Diagnostiek
• Gold standard: cytotoxicity assay
• Kweek met toxine bepaling
• Elisa (toxin A and or B, or GDH)– 72-92 % sensitiviteit– 89-98 % specificiteit
• PCR– Sensitiviteit 92%– Specificiteit 96%
• Sigmoidoscopy
Behandeling
• De beste behandeling is nog steeds preventie!• Lokaal: antibioticum formularium ZGV• Gebaseerd op SWAB richtlijn• SWAB weer gebaseerd op ESCMID
“Infection control” strategie
Rigorous hand hygiene
Judicious use of antibacterial agents to preserve patients’ microflora
Isolation of patients with faecal incontinence
Barrier protection (e.g. gowns and gloves)
Use of dedicated equipment for patients with CDI
Environmental cleaning and disinfection
Education of healthcare workers and visitors about CDI transmission
Kelly & Lamont. NEJM 2008;359:1932–40Vonberg et al Clin Microbiol Infect 2008;14(Suppl. 5):2–20
Behandeling: ESCMID recommendations:
An initial mild episode of CDI
• Discontinuation of the antibacterial treatment that induced CDI, if possible
• Avoidance of treatments that reduce gut transit– e.g. opioids, including those used in diarrhoea relief
(loperamide etc)• Provision of supportive care
– e.g. fluid and electrolyte replacement• Observation for signs of clinical deterioration
Bauer et al. Clin Microbiol Infect 2009;15:1067–79.
Behandeling: ESCMID recommendations:
First episode of CDI
• Aim of treatment is to eradicate C. difficile from the intestines and promote restoration of the normal colonic microflora
• Cessation of antibacterial therapy, if possible, is usually the first step
Diagnosis ESCMID recommended treatmentNon-severe first episode Metronidazole 500 mg tid orally for 10 days*
Severe first episode Vancomycin 125 mg qid orally for 10 days (or teicoplanin 100 mg bid)
IV metronidazole 500 mg tid for 10 days plus intracolonic vancomycin 500 mg in 100 mL saline every 4–12 hours and/or vancomycin 500 mg qid by nasogastric tube if oral therapy impossible
* Intravenous (IV ) if oral therapy is not possible
Bauer et al. Clin Microbiol Infect 2009;15:1067–79.
Behandeling (10-14 dgn)• Metronidazol
3 dd 500
• eerste keus:• po en iv• geen selectie VRE• Goedkoop• vaak recidieven
• Vancomycine 4 dd 125-500 mg
• tweede keus:• alleen po• selectie VRE• Duur• vaak recidieven
Ernstige colitis vancomycin
Snapshot of current treatments for initial episodes of CDI in Europe
Bauer et al. Lancet 2011;377:63–73.
Treatments used in an initial episode of CDI in a recent European survey
71%
11%
18%
0.2%
Oral metronidazole
IV metronidazole
Oral vancomycin
Intracolonic vancomycin
Cure rates: Metronidazole & vancomycin
p=0.006p=0.36 p=0.02
37/4139/40
28/38
30/31
66/79
69/71
Zar et al. Clin Infect Dis 2007;45:302–7.
*Patients were stratified by mild or severe disease based on severity assessment score developed for this study. Patients received one point each for age >60 years, temperature >38.3°C, albumin level <2.5 mg/dL, or peripheral white blood cell count >15,000 cells/mm 3
within 48 hours of enrolment. Two points were given for endoscopic evidence of pseudomembranous colitis or treatment in an intensive care unit. Patients with ≥2 points were considered to have severe CDI.
Recurrence of CDI
• Recurrence of CDI has been identified by ESCMID as the most important problem in the treatment of CDI1
• CDI recurrence is common, occurring in up to 32% of cases within 30 days following treatment2–4
• Rate of reported recurrences strongly depends on definition applied1
• Recurrence appears to be related to a combination of:5
– A failure to re-establish the colonic microflora– The presence in the intestines of spores of C. difficile– A sub-optimal host immune response to the infecting organism and
its toxins1. Bauer et al. Clin Microbiol Infect 2009;15:1067–79;2. Louie et al. N Engl J Med 2011;364:422–31;3. Lowy et al. N Engl J Med 2010;362:197–205;4. Bouza et al. Clin Microbiol Infect 2008;14:S103–4;5. DuPont. N Engl J Med 2011;364:473–4.
Risk factors for a recurrence of CDI
• Immunocompromised patients1
• Exposure to other antibacterial agents that disrupt the normal colonic microflora2–5
• Previous episode of CDI2,4–6
• Renal impairment7,8
• Aged 65 years or over2,4,9
• Impaired immune response to C. difficile toxin A2
• Severe underlying disease2
• Prolonged hospitalisation9
• Concomitant use of antacid medications (PPI)10
• Intensive care unit (ICU) stay5
1. Cohen. J Ped Gastroenterol Nutr 2009;48:63–5;2. Kyne et al. Lancet 2001;357:189–93;3. Bauer et al. Clin Microbiol Infect 2009;15:1067–79;4. Bauer et al. Lancet 2011;377:63–73;5. Hu et al. Gastroenterology 2009;136:1206–14;
6. McFarland et al. Am J Gastroenterol 2002;97:1769–75;7. Do et al. Clin Infect Dis 1998;26:954–9;8. Bauer et al. Clin Microbiol Infect 2011;17(Suppl 4):A1–A4;9. Pépin et al. Clin Infect Dis 2005;40:1591–7;10. Kwok et al. Am J Gastroenterol 2012;107:1011–9.
PPI, proton pump inhibitor
• ESCMID recommends treating a first recurrence as a first episode unless the disease has progressed from non-severe to severe
Pharmacotherapy of CDI: First recurrence
Bauer et al. Clin Microbiol Infect 2009;15:1067–79.
Diagnosis ESCMID recommended treatmentNon-severe first recurrence Metronidazole 500 mg tid orally for 10 days* Severe first recurrence Vancomycin 125 mg qid orally for 10 days
IV metronidazole 500 mg tid for 10 days plus intracolonic vancomycin 500 mg in 100 mL saline every 4–12 hours and/or vancomycin 500 mg qid by nasogastric tube if oral therapy impossible
*Intravenous (IV ) if oral therapy is not possible; tid, three times daily; qid, four times daily
Diagnosis ESCMID recommended treatmentSecond and later recurrences
Vancomycin 125 mg qid orally for at least 10 days- Consider tapering vancomycin dose by
decreasing daily dose with 125 mg every 3 days
- Consider pulse dosing with vancomycin 125 mg every 3 days for 3 weeks
IV metronidazole 500 mg tid for 10–14 days plus retention enema of vancomycin 500 mg in 100 mL saline every 4–12 hours and/or vancomycin 500 mg qid by nasogastric tube if oral therapy impossible
ESCMID recommendations: Second and later recurrences
• ESCMID recommends treating second or later recurrences in the same way as severe first recurrence– With the option of using tapered or pulsed dosing regimens
Bauer et al. Clin Microbiol Infect 2009;15:1067–79.
NTVG 2005; 149: 2081
ESCMID recommendations:Surgical intervention
• In the minority (<5%) of patients who develop fulminant colitis, surgical intervention (colectomy) may be needed
• Surgical intervention carries a high rate of mortality• Optimal timing for colectomy has not been established• Current guidelines recommend intervention before:
– The disease becomes too severe– Serum lactate levels exceed 5 mmol/L
Bauer et al. Clin Microbiol Infect 2009;15:1067–79.
Clinical limitations associated with current treatments for CDI
• Although metronidazole and vancomycin are effective in a first episode of CDI, therapy remains suboptimal
• Among the most significant drawbacks of current therapy for CDI are:– Rates of treatment failure with metronidazole of up to 18%1
– Rates of recurrent infection following treatment with metronidazole and vancomycin of up to 32% within 30 days following treatment2–4
– Risk of overgrowth of vancomycin-resistant enterococci (VRE) in patients who are already colonised with VRE5
1. Aslam et al. Lancet Infect Dis 2005;5:549–57;2. Louie et al. N Engl J Med 2011;364:422–31;3. Lowy et al. N Engl J Med 2010;362:197–205;
4. Bouza et al. Clin Microbiol Infect 2008;14:S103–4;5. Al-Nassir et al. Antimicrob Agents Chemother 2008;52:2403–6.
Fidaxomicine
• Macrocyclisch antibioticum• Remt bacteriële RNA polymerase• Smal spectrum; Gram negatieve bacteriën resistent• Remt sporenvorming• Remt toxine productie• Wordt beperkt geresorbeerd: lokaal werkzaam• Zwangerschap / lactatie: onbekend• Bijwerkingen: misselijkheid, braken, obstipatie...• Dosering 2 dd 200mg 10 dagen
Fidaxomicine
• Extramuraal vergoed via GVS mits18 jaar of ouderCDIRecidief na metronidazol behandelingErnstige infectie
• 1620 euro per kuur
DJB: alternatieve therapie
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