Clostridium difficile–Associated Disease, Including Pseudomembranous Colitis Part 5 Recurrent CDAD Overall, ~15–30% of patients experience recurrences of CDAD, either as relapses caus
Trang 1Chapter 123 Clostridium difficile–Associated Disease,
Including Pseudomembranous Colitis
(Part 5)
Recurrent CDAD
Overall, ~15–30% of patients experience recurrences of CDAD, either as relapses caused by the original organism or as reinfections following treatment (Table 123-2) Recurrence rates are higher among patients ≥65 years old and among patients who remain in the hospital after the initial episode of CDAD Patients who have a first recurrence of CDAD have a high rate of second recurrence (33–65%) In the first recurrence, re-treatment with metronidazole is comparable to treatment with vancomycin Recurrent disease, once thought to be relatively mild, has been documented to pose a significant (11%) risk of serious complications (shock, megacolon, perforation, colectomy, or death within 30 days) There is no standard treatment for multiple recurrences, but long or repeated metronidazole courses should be avoided because of potential neurotoxicity Approaches include the administration of vancomycin followed by the yeast
Saccharomyces boulardii; the administration of vancomycin followed by synthetic
Trang 2fecal bacterial enema; and the intentional colonization of the patient with a
nontoxigenic strain of C difficile None of these biotherapeutic approaches has
been approved by the FDA for use in the United States Other strategies include (1) the use of vancomycin in tapering doses or with pulse dosing every other day for 4–6 weeks and (2) sequential treatment with vancomycin (125 mg four times daily) followed by rifaximin (400 mg twice daily) for 14 days IV immunoglobulin, which has also been used with some success, presumably
provides antibodies to C difficile toxins
Fulminant CDAD
Fulminant (rapidly progressive and severe) CDAD presents the most difficult treatment challenge Patients with fulminant disease often do not have diarrhea, and their illness mimics an acute surgical abdomen Sepsis (hypotension, fever, tachycardia, leukocytosis) may result from severe CDAD An acute abdomen (with or without toxic megacolon) may include signs of obstruction, ileus, colon-wall thickening, and ascites on abdominal CT, often with peripheral-blood leukocytosis (≥20,000 cells/µL) Whether or not the patient has diarrhea, the differential diagnosis of an acute abdomen, sepsis, or toxic megacolon should include CDAD if the patient has received antibiotics in the past 2 months Cautious sigmoidoscopy or colonoscopy to visualize PMC and an abdominal CT examination are the best diagnostic tests in patients without diarrhea
Trang 3Medical management of fulminant CDAD is suboptimal because of the difficulty of delivering metronidazole or vancomycin to the colon by the oral route
in the presence of ileus Vancomycin (given via nasogastric tube and by retention enema) plus IV metronidazole have been used in uncontrolled studies with some success, but surgical colectomy may be life-saving if there is no response to medical management The incidence of fulminant CDAD requiring colectomy appears to be increasing in the evolving epidemic
Prognosis
The mortality rate attributed to CDAD, previously found to be 0.6–3.5%, has reached 6.9% in recent outbreaks and is progressively higher with increasing age Most patients recover, but recurrences are common
Prevention and Control
Strategies for the prevention of CDAD are of two types: those aimed at preventing transmission of the organism to the patient and those aimed at reducing
the risk of CDAD if the organism is transmitted Transmission of C difficile in
clinical practice has been prevented by gloving of personnel, elimination of the use of contaminated electronic thermometers, and use of hypochlorite (bleach) solution for environmental decontamination of patients' rooms Hand hygiene is critical; hand washing is recommended in CDAD outbreaks because alcohol hand gels are not sporicidal CDAD outbreaks have been best controlled by restricting
Trang 4the use of specific antibiotics, such as clindamycin and second- and third-generation cephalosporins Outbreaks of CDAD due to clindamycin-resistant strains have resolved promptly when clindamycin use was restricted
Further Readings
Aslam S et al: Treatment of Clostridium difficile–associated disease: Old
therapies and new strategies Lancet Infect Dis 5:549, 2005 [PMID: 16122678]
Johnson S et al: Interruption of recurrent Clostridium difficile–associated
diarrhea episodes by serial therapy with vancomycin and rifaximin Clin Infect Dis 44:846, 2007 [PMID: 17304459]
Kyne L et al: Association between antibody response to toxin A and
protection against recurrent Clostridium difficile diarrhea Lancet 357:189, 2001
[PMID: 11213096]
——— et al: Asymptomatic carriage of Clostridium difficile and serum
levels of IgG antibody against toxin A N Engl J Med 342:390, 2000
Loo VG et al: A predominantly clonal multi-institutional outbreak of
Clostridium difficile–associated diarrhea with high morbidity and mortality N
Trang 5Engl J Med 353:2442, 2005 [PMID: 16322602]
McDonald LC et al: Clostridium difficile infection in patients discharged
from US short-stay hospitals, 1996-2003 Emerg Infect Dis 12:409, 2006 [PMID: 16704777]
——— et al: An epidemic, toxin gene–variant strain of Clostridium
difficile N Engl J Med 353:2433, 2005
McFarland LV: Alternative treatments for Clostridium difficile disease:
What really works? J Med Microbiol 54:101, 2005 [PMID: 15673502]
Pepin J et al: The management and outcomes of a first recurrence of
Clostridium difficile associated disease in Quebec Clin Infect Dis 42:758, 2006
[PMID: 16477549]
Zar FA et al: A comparison of vancomycin and metronidazole for the
treatment of Clostridium difficile–associated diarrhea, stratified by disease
severity Clin Infect Dis 45:302, 2007 [PMID: 17599306]
Bibliography
Trang 6Bartlett JG: Narrative review: The new epidemic of Clostridium difficile–
associated enteric disease Ann Intern Med 145:758, 2006 [PMID: 17116920]
Kuijper EJ et al: Emergence of Clostridium difficile–associated disease in
North America and Europe Clin Microbiol Infect 12(Suppl 6):2, 2006
Musher D et al: Relatively poor outcome after treatment of Clostridium
difficile colitis with metronidazole Clin Infect Dis 40:1586, 2005 [PMID:
15889354]
Pepin J et al: Increasing risk of relapse after treatment of Clostridium
difficile colitis in Québec, Canada Clin Infect Dis 40:1591, 2005 [PMID:
15889355]