1 / 33

Clostridium difficile Infections: Diagnosis, Treatment, and Prevention

Clostridium difficile Infections: Diagnosis, Treatment, and Prevention. Theresa Cuoco, MD. Outline. Introduction Risk Factors for Disease Methods for Detection Antibiotic Therapy Nonstandard Adjunctive Interventions Infection Control and Prevention. Introduction.

gezana
Download Presentation

Clostridium difficile Infections: Diagnosis, Treatment, and Prevention

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript

  1. Clostridium difficile Infections: Diagnosis, Treatment, and Prevention Theresa Cuoco, MD

  2. Outline • Introduction • Risk Factors for Disease • Methods for Detection • Antibiotic Therapy • Nonstandard Adjunctive Interventions • Infection Control and Prevention

  3. Introduction • Gram positive, spore forming, toxin producing • 1935: “difficult clostridium” (isolation on conventional media) • Obligate anaerobic bacterium • Survives 10-15 minutes following exposure to air • Hardy spore • Resistant to heat, acid, alcohol, and abx; ingested, and germinates • Transmitted via fecal-oral route • Causes disease by production of toxins that bind to receptors on colonic epithelium • A enterotoxin: attracts neutrophils and monocytes • B cytotoxin: mediates mucosal damage (10x more potent)

  4. Definition • The presence of symptoms • Usually diarrhea (at least 3 unformed stools in 24hrs) • <1% of cases: no diarrhea; ileus and colonic distention • AND EITHER • Stool test positive or • Colonoscopic or histopathologic findings of pseudomembranous colitis • 96% of patients received abx within 14 days prior to onset of diarrhea; nearly all within past 3 months • Median time to onset 2-3 days after colonization

  5. Spectrum ofClostridium difficile Infection (CDI) • Asymptomatic carrier • Colonization with nontoxigenic strain affords protection • High circulating titers of IgG antitoxin • Mild diarrhea (≥ 3 stools in 24hr) • Fever, cramping, abdominal pain, leukocytosis • Severe diarrhea (≥ 10 stools in 24hr) • Pseudomembranous colitis • Fulminant colitis • Severe pain, distention, fever, shock, lactic acidosis, WBC • Toxic megacolon with paralytic ileus

  6. Increasing Severity Age-adjusted Death Rate Due to Enterocolitis from C. difficile 1999 to 2006 Per 100,000 Population [From: Heron 2009(http://www.cdphe.state.co.us/hf/patientsafety/CDItoolkit.pdf)

  7. Hypervirulent Strain: NAP1/B1/027 • “North American Pulsed-field Type” • Deletion in gene that down regulates toxin production • Produces 16-23 times more toxin • Produces a binary toxin • Resistance to fluoroquinolones • Increased sporulation

  8. Risk Factors for Development of CDI • Antibiotic use: disruption of colonic flora • Broad spectrum, multiple abx, and duration of therapy • Host immune status • Advanced age, duration of hospitalization, & female gender • Comorbidities • GI procedures and enteral feeding • Gastric acid suppression (risk 1.4-2.75 times higher with PPI) • Chemotherapeutic agents (antimicrobial/immunosuppressive) • Hematopoietic stem cell transplantation

  9. Antibiotics Implicated

  10. Diagnosis and Detection of CDI • Only performed on unformed stool unless ileus suspected • Testing asymptomatic patients, including use as a test of cure NOT recommended • Repeat testing during same diarrheal episode discouraged

  11. Detection of CDI • Cytotoxicity Assay • Culture • Immunoassays • Toxin Gene Detection • Endoscopic evidence

  12. Cytotoxicity Assay • Stool mixed with cultured test cells • Monitored for toxin effects (cell rounding) • Requires up to 48 hours • Often used as reference test in the evaluation of other diagnostic tests • Highly sensitive; not practical

  13. Culture • Cycloserine, cefoxitin, fructose agar (CCFA) • Most sensitive • Can take 2 to 9 days • Colonies with specific odor and fluoresce with Woods lamp

  14. Immunoassays – “EIA” • Majority of labs use this technique – quick, inexpensive • Some only detect toxin A and strains emerging with only toxin B • Moderate and variable sensitivity 63-94% • Frequent false negatives • Specificity 75-100% • Alternative 2 step process: high negative predict value • EIA detection of Glutamate Dehydrogenase (GDH): enzyme produced by C diff • toxin testing

  15. Toxin Gene Detection: PCR • Detects presence of gene involved in toxin production • Rapid, sensitive and specific • Used at MUSC

  16. Pseudomembranes Endoscopic appearance Gross appearance Raised yellow or off-white plaques up to 2 cm in diameter scattered or confluent edema, erythema, friability, and inflammation

  17. Treatment • Discontinue inciting antibiotic • Implement infection control measures • Confirm with testing • Empiric therapy may be warranted based on severity of symptoms • Avoid antiperistaltic agents – precipitates megacolon • Determine clinical severity • Mild-moderate, severe, severe-complicated

  18. Mild to Moderate Disease • Metronidazole vs Vancomycin equivocal • Metronidazole – first line • 500 mg po q8 or 250 mg po q6 • 500 mg IV q8 if oral therapy not feasible • Limitations: peripheral neuropathy, nausea, metallic • Vancomycin • 125 mg po Q6 **must be given orally • Duration: 10-14 days • If underlying infection requiring prolonged abx, continue CDI treatment throughout abx course + 1 additional week

  19. Initial Recurrent Disease • “Recurrence of symptoms within 8-10 weeks after cessation of specific antibiotic therapy” • Up to 20-25% of patients adequately treated • Confirm diagnosis • Up to ½ of recurrent episodes are reinfections rather than relapses with original strain • Most present 1-3 weeks after discontinuing abx therapy (but up to 2-3 months) • Why? Persistent spores, impaired host immune response • Treatment with same regimen as initial but stratify based on disease severity

  20. Second Recurrence • Confirm diagnosis • Subset with high rate of repeat recurrence • Avoid metronidazole due to cumulative neurotoxicity • Vancomycin: tapered and/or pulsed dosing – allows spores to germinate • 125 mg po QID for 7-14 days • 125 mg po BID for 7 days • 125 mg po QD for 7 days • 125 mg QOD for 7 days • 125 mg po q 3 days for 14 days • Fidaxomicin 200 mg po BID for 10 days

  21. Subsequent recurrence • Confirm diagnosis • Vancomycin 125 mg po QID for 14 days followed by rifaximin 400 mg BID for 14 days • Based on small case series • Fidaxomicin 200 mg po BID for 10 days

  22. Fidaxomicin (Dificid) • Macrocyclic macrolide antibiotic • Bactericidal • Narrower antimicrobial spectrum = less disruption of normal flora • FDA approved in 2011 • What’s the hype?

  23. Fidaxomicin Limited to non-NAP1 strains

  24. Severe CDI: markers • Severe diarrhea • >10 bowel movements/day • Leukocytosis • >15K – severe • >25 increased fatality • High or rising serum Cr • (50% increase) • Low serum albumin (<2.5 mg/dL) • Severe abdominal distention, pain • Ileus or toxic megacolon • Colonic thickening on CT • Ascites on CT • Pseudomembranes on endoscopy • Hemodynamic instability • Organ Failure Pepin J, et al. Can Med J Assoc 2004: 171:466-472. Bartlett JG, Gerding DN. Clin Infect Dis 2008: 46(Suppl):S12-S18

  25. Severe CDI • No consensus definition • Zar et al Clin Infect Dis 2007: ≥2 points = severe • Treatment: Vancomycin 125 mg po QID for 10-14days • No supportive evidence for higher dosing • Improved rates of cure with vanc vs metronidazole but not significant when using strict intention to treat analysis

  26. Severe, Complicated CDI • Hypotension, shock,ileus, or megacolon • Vancomycin 500 mg po or per NGT ± metronidazole 500 mg IV q8 • If complete ileus: add vancomycin 500 mg in 100cc NS as retention enema q6 • Surgery considered if age ≥ 65 and WBC ≥20, lactate > 2.2, peritoneal signs, severe ileus, toxic megacolon • Increased periop mortality with lactate > 5 and WBC > 50 • Subtotal colectomy with ileostomy and rectum spared

  27. Nonstandard Adjunctive InterventionsWhy explored? • Standard antibiotics ineffective in 8-36% • NO current antibiotics kill spores • Rates of infection and relapse are increasing • Specific therapies: • Probiotics/Prebiotics • Anion binding resins • Fecal flora reconstitution • C diff immune whey (antibody) • IVIG

  28. Prevention Strategies • Low level evidence for link of prevention to outcomes • “People” measures • Environmental Measures • Antimicrobial restrictions • “Bundled prevention strategies”

  29. Person measures • Immediate infection control measures once CDI is suspected • Gowns/gloves • Hand washing with soap and water • Friction and detergent action • Private room with contact precautions • If single room not possible, cohort patients with separate commodes

  30. Environmental Cleaning and Disinfection • Disposable rectal thermometers • In place of electronic • Inadequately cleaned commodes or bedpans • Chlorine/hypochlorite containing cleaners

  31. Antimicrobial Stewardship • Minimize frequency, duration of therapy, and number of antibiotic agents • Reduce use of “high risk” antimicrobials • Stewardship programs based on local epidemiology • Restriction of cephalosporins and clindamycin

  32. Bibliography Butler M, Bliss D, Drekonja D, Filice G, Rector T, MacDonald R, Wilt T. Effectiveness of Early Diagnosis, Prevention, and Treatment of Clostridium difficile Infection. Comparative Effectiveness Review prepared for Agency for Healthcare Research and Quality. December 2001. Cohen SH, Gerding DN, Johnson S, Kelly CP, Loo VG, McDonald LC, Pepin J, Wilcox MH. Clinical Practice Guidelines for Clostridium difficile Infection in Adults: 2010 Update by the Society for Healthcare Epidemiology of America (SHEA) and the Infectious Diseases Society of America (IDSA). Infection Control and Hospital Epidemiology. May 2010, Vol 31, No 5. Dial S, Alrasadi K, Manoukian C, Huang A, Menzies D. Risk of Clostridium difficile diarrhea among hospital inpatients prescribed proton pump inhibitors: cohort and case-control studies. CMAJ; July 6, 2004: 171 (1). Louie TJ, Miller MA, Mullane KM, Weiss K, Lentnek A, Golan Y, Gorbach S, Sears P, Shue YK. Fidaxomicin versus Vancomycin for Clostridium difficile Infection. N Engl J Med 2011; 364:422-31. Zar, FA, Bakkanagari SR, Moorthi KM, Davis MB. A comparison of vancomycin and metronidazole for the treatemtn of Clostridium difficile-associated diarrhea, stratified by disease severity.Clin Infect Ds 2007; 45: 302

More Related