[Individualized treatment strategies for Clostridium difficile infections].

P Solbach, P Dersch, O Bachmann
Author Information
  1. P Solbach: Klinik für Gastroenterologie, Hepatologie und Endokrinologie, Medizinische Hochschule Hannover, Carl-Neuberg-Str. 1, 30625, Hannover, Deutschland. solbach.philipp@mh-hannover.de.
  2. P Dersch: Deutsches Zentrum für Infektionsforschung (DZIF), TTU Gastrointestinale Infektionen, Standort Hannover-Braunschweig, Hannover/Braunschweig, Deutschland.
  3. O Bachmann: Klinik für Gastroenterologie, Hepatologie und Endokrinologie, Medizinische Hochschule Hannover, Carl-Neuberg-Str. 1, 30625, Hannover, Deutschland.

Abstract

Upon hospitalization, up to 15.5% of patients are already colonized with a toxigenic Clostridium difficile strain (TCD). The rate of asymptomatic colonization is 0-3% in healthy adults and up to 20-40% in hospitalized patients. The incidence and mortality of C. difficile infection (CDI) has significantly increased during recent years. Mortality lies between 3 and 14%. CDI is generally caused by intestinal dysbiosis, which can be triggered by various factors, including antibiotics or immune suppressants. If CDI occurs, ongoing antibiotic therapy should be discontinued. The choice of treatment is guided by the clinical situation: Mild courses of CDI should be treated with metronidazole. Oral vancomycin is suitable as a first-line therapy of mild CDI occurring during pregnancy and lactation, as well as in cases of intolerance or allergy to metronidazole. Severe courses should be treated with vancomycin. Recurrence should be treated with vancomycin or fidaxomicin. Multiple recurrences should be treated with vancomycin or fidaxomicin; if necessary, a vancomycin taper regimen may also be used. An alternative is fecal microbiota transplant (FMT), with healing rates of more than 80%. Bezlotoxumab is the first available monoclonal antibody which neutralizes the C. difficile toxin B, and in combination with an antibiotic significantly reduces the rate of a new C. difficile infection compared to placebo. A better definition of clinical and microbiota-associated risk factors and the ongoing implementation of molecular diagnostics are likely to lead to optimized identification of patients at risk, and an increasing individualization of prophylactic and therapeutic approaches.

Keywords

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MeSH Term

Aminoglycosides
Anti-Bacterial Agents
Clostridioides difficile
Clostridium Infections
Fecal Microbiota Transplantation
Female
Fidaxomicin
Humans
Metronidazole
Recurrence
Secondary Prevention
Vancomycin

Chemicals

Aminoglycosides
Anti-Bacterial Agents
Metronidazole
Vancomycin
Fidaxomicin

Word Cloud

Created with Highcharts 10.0.0CDItreatedvancomycinpatientsC difficileClostridiumdifficilerateinfectionsignificantlyfactorsongoingantibiotictherapytreatmentclinicalcoursesmetronidazolefidaxomicinmicrobiotariskUponhospitalization155%alreadycolonizeda toxigenicstrainTCDasymptomaticcolonization0-3%healthyadults20-40%hospitalizedincidencemortalityincreasedrecentyearsMortalitylies3 and14%generallycausedintestinaldysbiosiscantriggeredvariousincludingantibioticsimmunesuppressantsoccursdiscontinuedchoiceguidedsituation:MildOralsuitablea first-linemildoccurringpregnancylactationwellcasesintoleranceallergySevereRecurrenceMultiplerecurrencesnecessarya vancomycintaperregimenmayalsousedalternativefecaltransplantFMThealingrates80%Bezlotoxumabfirstavailablemonoclonalantibodyneutralizestoxin Bcombinationreducesa newcomparedplaceboA betterdefinitionmicrobiota-associatedimplementationmoleculardiagnosticslikelyleadoptimizedidentificationincreasingindividualizationprophylactictherapeuticapproaches[Individualizedstrategiesinfections]Diarrheahospital-acquiredFecaltransplantationGastroenteritisinfectiousMetronidazoleVancomycin

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