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5PSQ-098 Experience in the treatment of Clostridium difficile infection

Background and importance Clostridium difficile infection (CDI) can cause acute diarrhoea. One of the complications of CDI is recurrences. There are risk factors for multiple recurrences of the disease. Vancomycin and oral metronidazole are considered the treatment of choice. Other drugs, such as fi...

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Bibliographic Details
Published in:European journal of hospital pharmacy. Science and practice 2022-03, Vol.29 (Suppl 1), p.A151-A152
Main Authors: Gómez Delgado, M, López Escoz, R, Gonzalez Padilla, M, Sanchez Yañez, E, Moya Carmona, I
Format: Article
Language:English
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Summary:Background and importance Clostridium difficile infection (CDI) can cause acute diarrhoea. One of the complications of CDI is recurrences. There are risk factors for multiple recurrences of the disease. Vancomycin and oral metronidazole are considered the treatment of choice. Other drugs, such as fidaxomicin and bezlotuxumab, may help in the control of recurrences.Aim and objectivesTo analyse the use of fidaxomicin and bezlotuxumab in our hospital.To analyse recurrences after treatment with fidaxomicin and early bezlotuxumab administration.Material and methodsRetrospective study including all patients treated with fidaxomicin from January 2014 to April 2021. Variables collected: age, gender, previous treatment (vancomycin/metronidazol), days and regimen of treatment, recurrence or death at 8 weeks. Risk factors evaluated: age >65 years, use of antibiotics in the previous 3 months, ICD in the last 6 months, severe disease (oncological patient, immunosuppressed, renal failure). Tapered dosage of fidaxomicin oral was defined as 200 mg/12 hours (5 days) and 200 mg/48 hours (D7–D25).Data were obtained from the pharmacy dispensation program and the patients’ digital clinical records.ResultsForty-one patients were included, 25 women (61%), mean age 69 (21–99) years, 73.2% (n=30) were older than 65 years. 95.1% (n=39) had received antibiotics in the previous 3 months, 51.2% (n=21) had suffered CDI in the last 6 months, 60.9% (n=26) had severe baseline disease and 21.9% (n=9) were immunosuppressed. As first line, 41.4% (n=17) received vancomycin and metronidazole, 44% (n=18) received vancomycin and 14.6% (n=6) received fidaxomicin. 63.4% (n=26) received fidaxomicin 200 mg/12 hours (10 days), in 14.6% (n=9) the extended regimen was used and 22% (n=6) received 200 mg/12 hours for longer. 82.9% (n=34) of fidaxomicin-treated patients had no CDI recurrence at 8 weeks. 22% (n=9) of the patients died. Nine fidaxomicin-treated patients were administered bezlotuxumab and none subsequently developed CDI. All were older than 65 years and 66.6% (n=6) were oncology patients.Conclusion and relevanceThe CDI treatment was mostly adjusted to the recommendedations in the therapeutic guidelines, with vancomycin/metronidazole as first-line and fidaxomicin in recurrences. The use of bexlotuxumab was adapted to the considerations of the Therapeutic Positioning Index and was used in patients with a higher risk of recurrence.Although in the pivotal studies the recurrence rate with bexlotu
ISSN:2047-9956
2047-9964
DOI:10.1136/ejhpharm-2022-eahp.318