Clostridioides difficile: Difference between revisions

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Clostridioides difficile
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===Microbiology===
===Microbiology===


*Spore-forming, anaerobic, [[Stain::Gram-positive]] [[Cellular shape::bacillus]]
*Spore-forming, [[Cellular respiration::anaerobic]], [[Stain::Gram-positive]] [[Shape::bacillus]]


===Risk factors===
===Risk factors===


*Antibiotic exposure, typically broad-spectrum antibiotics especially those with anaerobic coverage[[CiteRef::brown2013me]]
*Antibiotic exposure, typically broad-spectrum antibiotics especially those with anaerobic coverage[[CiteRef::brown2013me]]
**Clindamycin
**[[Clindamycin]]
**Fluoroquinolones (especially with NAP1 strain)
**[[Fluoroquinolones]] (especially with NAP1 strain)
**Cephalosporins
**[[Cephalosporins]]
**Monobactams
**[[Monobactams]]
**Carbapenems
**[[Carbapenems]]
*PPI use
*[[PPI]] use
*[[Chemotherapy]]
*[[Hematopoietic stem cell transplantation]]


=== Pathophysiology ===
===Pathophysiology===


* Two toxins
*Two toxins
** Toxin A (enterotoxin) causes intestinal secretion and mucosal damage
**Toxin A (enterotoxin) causes intestinal secretion and mucosal damage
** Toxin B (cytotoxin) is a virulence factor
**Toxin B (cytotoxin) is a virulence factor
* Virulence depends on strain (e.g. NAP1 quite virulent with high risk of severe disease and relapse)
*Virulence depends on strain (e.g. NAP1 quite virulent with high risk of severe disease and relapse)
* Spores can persist in GI tract up to 2 to 8 weeks despite treatment
*Spores can persist in GI tract up to 2 to 8 weeks despite treatment


==Clinical Manifestations==
==Clinical Manifestations==


*Profuse watery diarrhea
*Profuse watery diarrhea
*When following antibiotics:
**Risk is highest within two weeks of starting antibiotics until 1 week after stopping antibiotics
**Risk increases with the duration of antibiotics
**Risk depends on the antibiotic used[[CiteRef::brown2013me]]
***High risk: [[clindamycin]], [[fluoroquinolones]], and non-penicillin β-lactams (i.e. [[cephalosporins]], [[monobactams]], and [[carbapenems]])
***Low risk: [[macrolides]], [[trimethoprim-sulfamethoxazole]], and [[penicillins]]
***No risk: [[tetracyclines]]


===Severity===
===Severity===
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**Thought to be related to a lack of the binding target of ''C. difficile'' toxin
**Thought to be related to a lack of the binding target of ''C. difficile'' toxin
*Clinical disease is rare before 12 to 24 months of age
*Clinical disease is rare before 12 to 24 months of age

== Diagnosis ==

* Usually done with either nucleic acid testing for the toxin gene, or with an EIA test for GDH and toxin A/B enzyme
{| class="wikitable"
!Test
!Sensitivity
!Specificity
|-
|GDH immunoassay
|94-96%
|92-95%
|-
|Toxin A/B enzyme immunoassay
|58-83%
|99%
|-
|Parallel GDH and toxin A/B immunoassay
|58-82%
|99.5%
|-
|Toxin B PCR
|91-96%
|96-98%
|}


==Management==
==Management==
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*For '''rectal vancomycin''', add 500 mg to 100 mL normal saline and give as retention enema every 6 hours
*For '''rectal vancomycin''', add 500 mg to 100 mL normal saline and give as retention enema every 6 hours
*A sample '''vancomycin taper''': 125 mg po QID for 14 days, then 125 mg po TID for 7 days, then 125 mg po BID for 7 days, then 125 mg po daily for 7 days, then 125 mg po q2-3d for 2 to 8 weeks
*A sample '''vancomycin taper''': 125 mg po QID for 14 days, then 125 mg po TID for 7 days, then 125 mg po BID for 7 days, then 125 mg po daily for 7 days, then 125 mg po q2-3d for 2 to 8 weeks

=== High Dose Vancomycin ===

* No clear data supporting high-dose [[vancomycin]], even in severe CDAD[[CiteRef::bader2020re]]

=== Tapered-Pulsed Fidaxomicin ===

* Case series suggest it may be helpful, though recurrence rate still up to 40%[[CiteRef::skinner2021a]]
* [[Fidaxomicin]] 200 mg once daily for 7 days followed by 200 mg [[fidaxomicin]] every other day for the remaining 13 doses

==Prevention==

=== Probiotics ===

* Insufficient evidence to recommend for or against

=== Primary Prophylaxis ===

*Prophylaxis with oral [[vancomycin]] 125 mg PO daily continued until 5 days after end of systemic antimicrobials may be beneficial in preventing CDAD in high-risk patients[[CiteRef::johnson2019ef]]
**Included patients with age≥70 years or who were hospitalized in the past 90 days

=== Secondary Prophylaxis ===

* Oral [[vancomycin]] is occasionally used as secondary prophylaxis after a recent (within 3 to 12 months) episode of CDAD
* Per the IDSA guidelines, there is insufficient evidence to recommend for or against


==Further Reading==
==Further Reading==

Latest revision as of 17:28, 19 September 2024

Background

Microbiology

  • Spore-forming, anaerobic, Gram-positive bacillus

Risk factors

Pathophysiology

  • Two toxins
    • Toxin A (enterotoxin) causes intestinal secretion and mucosal damage
    • Toxin B (cytotoxin) is a virulence factor
  • Virulence depends on strain (e.g. NAP1 quite virulent with high risk of severe disease and relapse)
  • Spores can persist in GI tract up to 2 to 8 weeks despite treatment

Clinical Manifestations

Severity

Severity Definition2
Mild WBC ≤15 AND creatinine ≤1.5 x baseline
Severe, uncomplicated WBC >15 OR creatinine >1.5 x baseline OR hypoalbuminemia
Severe, complicated Hypotension OR shock OR ileus OR megacolon

Children

  • Asymptomatic carriage is common in infants (37% at 1 month, decreasing to adult levels of 3-5% by 3 years) 3
    • Thought to be related to a lack of the binding target of C. difficile toxin
  • Clinical disease is rare before 12 to 24 months of age

Diagnosis

  • Usually done with either nucleic acid testing for the toxin gene, or with an EIA test for GDH and toxin A/B enzyme
Test Sensitivity Specificity
GDH immunoassay 94-96% 92-95%
Toxin A/B enzyme immunoassay 58-83% 99%
Parallel GDH and toxin A/B immunoassay 58-82% 99.5%
Toxin B PCR 91-96% 96-98%

Management

Severity First-line2 Alternatives
Initial episode
Mild to moderate Vancomycin 125 mg po QID for 10-14 days Fidaxomicin 200 mg po BID for 10 days
Metronidazole 500 mg po TID for 10-14 days
Severe, uncomplicated Vancomycin 125 mg po QID for 10-14 days
Fidaxomicin 200 mg po BID for 10 days
Severe, complicated Vancomycin 125-500 mg po QID for 10-14 days plus metronidazole 500 mg IV q8h Fidaxomicin 200 mg po BID for 10 days plus metronidazole 500 mg IV q8h
Consider rectal vancomycin if ileus
Recurrent episode
First recurrence, mild to moderate Vancomycin 125 mg po QID for 14 days Fidaxomicin 200 mg po BID for 10 days
First recurrence, severe, uncomplicated Vancomycin 125 mg po QID for 14 days
Fidaxomicin 200 mg po BID for 10 days
Second or subsequent recurrence Vancomycin as prolonged tapered or pulsed regimen Consider fecal microbiota tranplantation after vancomycin
  • For rectal vancomycin, add 500 mg to 100 mL normal saline and give as retention enema every 6 hours
  • A sample vancomycin taper: 125 mg po QID for 14 days, then 125 mg po TID for 7 days, then 125 mg po BID for 7 days, then 125 mg po daily for 7 days, then 125 mg po q2-3d for 2 to 8 weeks

High Dose Vancomycin

  • No clear data supporting high-dose vancomycin, even in severe CDAD4

Tapered-Pulsed Fidaxomicin

  • Case series suggest it may be helpful, though recurrence rate still up to 40%5
  • Fidaxomicin 200 mg once daily for 7 days followed by 200 mg fidaxomicin every other day for the remaining 13 doses

Prevention

Probiotics

  • Insufficient evidence to recommend for or against

Primary Prophylaxis

  • Prophylaxis with oral vancomycin 125 mg PO daily continued until 5 days after end of systemic antimicrobials may be beneficial in preventing CDAD in high-risk patients6
    • Included patients with age≥70 years or who were hospitalized in the past 90 days

Secondary Prophylaxis

  • Oral vancomycin is occasionally used as secondary prophylaxis after a recent (within 3 to 12 months) episode of CDAD
  • Per the IDSA guidelines, there is insufficient evidence to recommend for or against

Further Reading

References

  1. ^   Clostridium difficile Infection in Infants and Children. Pediatrics. 2012;131(1):196-200. doi:10.1542/peds.2012-2992.