4.7 Article

Clostridioides difficile Infection in Cancer and Immunocompromised Patients: Relevance of a Two-step Diagnostic Algorithm and Infecting Ribotypes on Clinical Outcomes

Journal

CLINICAL INFECTIOUS DISEASES
Volume 72, Issue 10, Pages E460-E465

Publisher

OXFORD UNIV PRESS INC
DOI: 10.1093/cid/ciaa1184

Keywords

Clostridioides difficile; ribotype; toxin; cancer

Funding

  1. institutional funds at The University of Texas MD Anderson Cancer Center

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This study investigated Clostridioides difficile infection in cancer patients, finding that patients with EIA+ were older, more likely to fail therapy and experience recurrence, with the presence of ribotypes associated with poor outcomes increasing the risk of treatment failure.
Background. Patients with cancer are particularly vulnerable to Clostridioides difficile infection (CDI). Guidelines recommend a two-step diagnostic algorithm to differentiate carriers from CDI; however, there are limited data for this approach while including other confounding risk factors for diarrhea such as radiation, cytotoxic chemotherapy, and adoptive cell based therapies. Methods. We conducted a prospective, non-interventional, single center, cohort study of cancer patients with acute diarrhea and C. difficile, identified in stools by nucleic acid amplification tests (NAAT) and culture. Fecal toxin A/B was detected by enzyme immunoassay (EIA) and isolates were ribotyped using 16s rRNA fluorescent sequencing. Patients were followed for 90 days to compare outcomes according to malignancy type, infecting ribotype, and EIA status. Results. We followed 227 patients with a positive NAAT. Of these, 87% were hospitalized and 83% had an active malignancy. EIA was confirmed positive in 80/227 (35%) of patients. Those with EIA+ were older (60 +/- 18 years vs 54 +/- 19 years., P = .01), more likely to fail therapy [24/80 (30%) vs 26/147 (18%), P= .04] and experience recurrence [20/80 (25%) vs 21/147(14%), P < .05]. We found a low prevalence (22%) of ribotypes historically associated with poor outcomes (002, 018, 027, 56, F078-126, 244) but their presence were associated with treatment failure [17/50 (34%) vs 33/177 (19%), P = .02]. Conclusions. When compared to cancer patients with fecal NAAT+/EIA-, patients with NAAT+/EIA+ CDI are less likely to respond to therapy and more likely to experience recurrence, particularly when due to ribotypes associated with poor outcomes.

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