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Dr Santosh M Narayankar
Clostridium difficile Infection
Antibiotic Associated Diarrhea(AAD)
 Common side effect of antibiotic
 Multiple mechanisms
 2-25% of antibiotic treatments
 Results from colonic microflora alteration
AAD-Mechanisms Of Diarrhea
 Motilin Receptor Agonist- Erythromycin
 Stimulate Bowel Peristalsis- Clvulanate
 Intestinal Flora Alteration-
Decreased Carb Metabolism
Altered Bile Acid Metabolism
 Overgrowth of pathogenic organisms
Major Infectious Agents
Causative agent unknown in most of the cases
 Candida overgrowth- controversial
 Clostridium Perfringes- Food poisoning, Necrotizing
enterocolitis (15%)
 Staph Aureus-Food poisioning,diarrhea (7%)
 Klebsiella Oxytoca -Antibiotic AssociatedHemorrhagic
Colitis (AAHC)
 Clostridium Difficile - 30% AAD in hospital
Differences between AAD- CDI And From
Other Causes
Clostridium Difficile
Infection(CDI)
Clostridium Difficile
 Gram Positive
 Anaerobe
 Spore forming
 Toxin producing-A & B
 Feco -oral route
 Non invasive
 Asymptomatic to severe
C. difficile 30% of AAD cases but is an important pathogen to identify
because it often requires specific antimicrobial therapy and can lead to
life-threatening complications
Definitions
CDI-Epidemiology
 Healthy adults
 In patients
 Healthy infants
0 to 3%
10-21%
25-80%
C. difficile associated diarrhoea (CDAD) in India
reveal a prevalence rate ranging from 7.1-26.6% with
fewer cases of fulminant infections
High risk for CDI
 Antimicrobial agent
 Older age >65 years
 In patient care
 Increased co morbidities
 PPI
 Chemotherapy
 HIV infection
 IBD
 Manipulation of GIT –
tube feeding,surgery
 Duration of
hospitalisation
Antimicrobial Agents-Predispose to
Clostridium difficile Infection
Any antibiotic, any dose, for any duration
Pathogenesis CDI
Clostridium Difficile Pathogenecity Locus
Structure and function of Clostridium
difficile toxins
Clinical features -CDI
 Asymptomatic
Clinical Clinical criteria
Mild Diarrhea (<6 BM/day), No fever
No peritoneal signs,
No evidence of sepsis
Moderate Diarrhea (6-12 BM/day), fever ,frankly visible stable lower GI
bleeding
Severe Diarrhea(>12 BM/day), fever ,hemodynamic instability, marked
and continuous abdominal pain, ileus, absence of bowel sounds,
evidence of sepsis, or intensive care unit level of care is required
Severity
Diagnosis
 Only stools from patients with diarrhea should be tested
 NAAT for C. difficile toxin genes such as PCR are
superior to toxins A + B EIA
 Glutamate dehydrogenase (GDH) screening tests can
be used in two- or three-step screening algorithms with
subsequent toxin A and B EIA testing, but the sensitivity
of such strategies is lower than NAATs
 Repeat testing should be discouraged
 Testing for cure should not be done
Stool Tests for the Diagnosis of
Clostridium difficile Infection
Colonoscopic Images-CDI
 Raised adherent yellow
plaques that vary in size
from 2 to 5 mm are visible
on the colonic mucosa.
 In some areas, coalescing
pseudo membranes are
evident.
 There is some erythema
of the colonic mucosa
between the
pseudomembranes,but
the epithelium is intact
Pseudo membranous Colitis
Histopathology
 Focal ulceration of
the colonic mucosa
is evident with
exudation of a
pseudomembrane
made up of
inflammatory cells,
fibrin, and necrotic
debris
 The adjoining
mucosa is intact
Volcano Or Summit Lesion
Accordion Sign On CT
Produced by a series of broad oedematous colonic haustral folds
Toxic mega colon X-ray & CT
Treatment-General approach
Treatment-Mild To Moderate
 Strong suspicion for CDI- Empiric therapy
 Antimicrobial agent(s) should be discontinued, if
possible
 Should be treated with metronidazole 500 mg orally
three times per day for 10 days.
 Failure to respond to metronidazole within 5 – 7 days
should prompt consideration of a change in therapy to
vancomycin at standard dosing.
Treatment-Mild to Moderate
 Who are intolerant / allergic to metronidazole and for
pregnant / breastfeeding women, vancomycin should
be used at standard dosing.
 Hartman’s pouch, ileostomy, or colon diversion,
vancomycin therapy delivered via enema.
 Anti-peristaltic agents to control diarrhea from
confirmed or suspected CDI should be avoided
Severe CDI
 Supportive care should be delivered
 CT scanning of the abdomen and pelvis
 No Abd Distension -Vancomycin delivered orally (125 mg
four times per day) plus intravenous metronidazole (500
mg three times a day)
 Abdominal Distension -Vancomycin delivered orally (500
mg four times per day) and per rectum (500 mg in a
volume of 100 ml four times a day) plus intravenous
metronidazole (500 mg three times a day).
Surgery –When?
 Hypotension requiring vasopressor therapy
 Clinical signs of sepsis and organ dysfunction (renal
and pulmonary)
 Mental status changes
 White blood cell count ≥ 50,000 cells / μ l
 Lactate ≥ 5 mmol / l
 Or failure to improve on medical therapy after 5 days.
Treatment-IDSA guideline update 2018
Management of recurrence
 IBD pts hospitalized with a disease flare should
 Undergo testing for CDI
 Simultaneous initiation of empiric therapy directed
against CDI and treatment of an IBD flare
 Escalation of immunosuppression medications should
be avoided
 Surgically created pouch after colectomy may develop
CDI and should be tested if they have symptoms.
Management of patients with CDI and co-
morbid conditions
Management of patients with CDI and co-
morbid conditions
 Underlying immunosuppression - should tested
 Any diarrheal illness in women who are pregnant or
periparturient should -Prompt testing
Fecal Microbiota Transplantation
 Cure rates greater than 85% and many greater than
90%.
 First RCT was performed by van Nood and
colleagues with FMT for rCDI through the
nasoduodenal route. Given that 81% of patients with
rCDI had resolution of C. difficile associated disease
(CDAD) after 1 infusion compared with 31% of
patients receiving vancomycin only (P<.001),the study
was terminated early following interim analysis.
 There have been 2 randomized controlled trials
showing efficacy of FMT via colonoscopy
Infection Control and Prevention
 Antibiotic stewardship
 Contact precautions
 Isolation
 Hand hygiene and barrier precautions,
 Single-use disposable equipment should be used
 Disinfection of environmental surfaces
 Insufficient evidence that probiotics prevent C. difficile
infection
C Difficile Vaccine
 Which contains inactivated toxoid A and B.
 Immunogenic and in a small case series,
vaccination was associated with resolution of
recurrent C. difficile diarrhea
 If effective, these therapeutic approaches also
may be useful to prevent C. difficile-associated
diarrhea in high-risk persons, such as older adults
and infirm patients receiving antibiotic therapy in
the hospital
Bezlotoxumab, a monoclonal antibody against TcdB
recently approved by the US Food and Drug
Administration (FDA), reduces the rate of CDI
recurrence in adults.
 However, the protective effect of this passive
immunization strategy is short-lived.
Thank You

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Antibiotic associated diarrhea & Clostridium difficile infection

  • 1. Dr Santosh M Narayankar Clostridium difficile Infection
  • 2. Antibiotic Associated Diarrhea(AAD)  Common side effect of antibiotic  Multiple mechanisms  2-25% of antibiotic treatments  Results from colonic microflora alteration
  • 3. AAD-Mechanisms Of Diarrhea  Motilin Receptor Agonist- Erythromycin  Stimulate Bowel Peristalsis- Clvulanate  Intestinal Flora Alteration- Decreased Carb Metabolism Altered Bile Acid Metabolism  Overgrowth of pathogenic organisms
  • 4. Major Infectious Agents Causative agent unknown in most of the cases  Candida overgrowth- controversial  Clostridium Perfringes- Food poisoning, Necrotizing enterocolitis (15%)  Staph Aureus-Food poisioning,diarrhea (7%)  Klebsiella Oxytoca -Antibiotic AssociatedHemorrhagic Colitis (AAHC)  Clostridium Difficile - 30% AAD in hospital
  • 5. Differences between AAD- CDI And From Other Causes
  • 7. Clostridium Difficile  Gram Positive  Anaerobe  Spore forming  Toxin producing-A & B  Feco -oral route  Non invasive  Asymptomatic to severe C. difficile 30% of AAD cases but is an important pathogen to identify because it often requires specific antimicrobial therapy and can lead to life-threatening complications
  • 9. CDI-Epidemiology  Healthy adults  In patients  Healthy infants 0 to 3% 10-21% 25-80% C. difficile associated diarrhoea (CDAD) in India reveal a prevalence rate ranging from 7.1-26.6% with fewer cases of fulminant infections
  • 10. High risk for CDI  Antimicrobial agent  Older age >65 years  In patient care  Increased co morbidities  PPI  Chemotherapy  HIV infection  IBD  Manipulation of GIT – tube feeding,surgery  Duration of hospitalisation
  • 11. Antimicrobial Agents-Predispose to Clostridium difficile Infection Any antibiotic, any dose, for any duration
  • 14. Structure and function of Clostridium difficile toxins
  • 15. Clinical features -CDI  Asymptomatic Clinical Clinical criteria Mild Diarrhea (<6 BM/day), No fever No peritoneal signs, No evidence of sepsis Moderate Diarrhea (6-12 BM/day), fever ,frankly visible stable lower GI bleeding Severe Diarrhea(>12 BM/day), fever ,hemodynamic instability, marked and continuous abdominal pain, ileus, absence of bowel sounds, evidence of sepsis, or intensive care unit level of care is required
  • 17. Diagnosis  Only stools from patients with diarrhea should be tested  NAAT for C. difficile toxin genes such as PCR are superior to toxins A + B EIA  Glutamate dehydrogenase (GDH) screening tests can be used in two- or three-step screening algorithms with subsequent toxin A and B EIA testing, but the sensitivity of such strategies is lower than NAATs  Repeat testing should be discouraged  Testing for cure should not be done
  • 18. Stool Tests for the Diagnosis of Clostridium difficile Infection
  • 19. Colonoscopic Images-CDI  Raised adherent yellow plaques that vary in size from 2 to 5 mm are visible on the colonic mucosa.  In some areas, coalescing pseudo membranes are evident.  There is some erythema of the colonic mucosa between the pseudomembranes,but the epithelium is intact
  • 20. Pseudo membranous Colitis Histopathology  Focal ulceration of the colonic mucosa is evident with exudation of a pseudomembrane made up of inflammatory cells, fibrin, and necrotic debris  The adjoining mucosa is intact Volcano Or Summit Lesion
  • 21. Accordion Sign On CT Produced by a series of broad oedematous colonic haustral folds
  • 22. Toxic mega colon X-ray & CT
  • 24. Treatment-Mild To Moderate  Strong suspicion for CDI- Empiric therapy  Antimicrobial agent(s) should be discontinued, if possible  Should be treated with metronidazole 500 mg orally three times per day for 10 days.  Failure to respond to metronidazole within 5 – 7 days should prompt consideration of a change in therapy to vancomycin at standard dosing.
  • 25. Treatment-Mild to Moderate  Who are intolerant / allergic to metronidazole and for pregnant / breastfeeding women, vancomycin should be used at standard dosing.  Hartman’s pouch, ileostomy, or colon diversion, vancomycin therapy delivered via enema.  Anti-peristaltic agents to control diarrhea from confirmed or suspected CDI should be avoided
  • 26. Severe CDI  Supportive care should be delivered  CT scanning of the abdomen and pelvis  No Abd Distension -Vancomycin delivered orally (125 mg four times per day) plus intravenous metronidazole (500 mg three times a day)  Abdominal Distension -Vancomycin delivered orally (500 mg four times per day) and per rectum (500 mg in a volume of 100 ml four times a day) plus intravenous metronidazole (500 mg three times a day).
  • 27. Surgery –When?  Hypotension requiring vasopressor therapy  Clinical signs of sepsis and organ dysfunction (renal and pulmonary)  Mental status changes  White blood cell count ≥ 50,000 cells / μ l  Lactate ≥ 5 mmol / l  Or failure to improve on medical therapy after 5 days.
  • 30.  IBD pts hospitalized with a disease flare should  Undergo testing for CDI  Simultaneous initiation of empiric therapy directed against CDI and treatment of an IBD flare  Escalation of immunosuppression medications should be avoided  Surgically created pouch after colectomy may develop CDI and should be tested if they have symptoms. Management of patients with CDI and co- morbid conditions
  • 31. Management of patients with CDI and co- morbid conditions  Underlying immunosuppression - should tested  Any diarrheal illness in women who are pregnant or periparturient should -Prompt testing
  • 32. Fecal Microbiota Transplantation  Cure rates greater than 85% and many greater than 90%.  First RCT was performed by van Nood and colleagues with FMT for rCDI through the nasoduodenal route. Given that 81% of patients with rCDI had resolution of C. difficile associated disease (CDAD) after 1 infusion compared with 31% of patients receiving vancomycin only (P<.001),the study was terminated early following interim analysis.  There have been 2 randomized controlled trials showing efficacy of FMT via colonoscopy
  • 33. Infection Control and Prevention  Antibiotic stewardship  Contact precautions  Isolation  Hand hygiene and barrier precautions,  Single-use disposable equipment should be used  Disinfection of environmental surfaces  Insufficient evidence that probiotics prevent C. difficile infection
  • 34. C Difficile Vaccine  Which contains inactivated toxoid A and B.  Immunogenic and in a small case series, vaccination was associated with resolution of recurrent C. difficile diarrhea  If effective, these therapeutic approaches also may be useful to prevent C. difficile-associated diarrhea in high-risk persons, such as older adults and infirm patients receiving antibiotic therapy in the hospital
  • 35. Bezlotoxumab, a monoclonal antibody against TcdB recently approved by the US Food and Drug Administration (FDA), reduces the rate of CDI recurrence in adults.  However, the protective effect of this passive immunization strategy is short-lived.

Notas do Editor

  1. NASH, nonalcoholic steatohepatitis.