Estimation of the difference in colistin plasma levels in critically ill patients with favorable or unfavorable clinical outcomes

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Abstract

In recent decades, antimicrobial resistance (AMR) has led to an increased use of therapeutic alternatives. Among these options, colistin continues to be an option for the treatment of multi-resistant (MDR) Gram-negative bacterial infections. However, due to its high toxicity (nephrotoxi-city and neurotoxicity) and narrow therapeutic window, colistin treatment must be utilized care-fully. Colistin-treated patients have been observed to have higher mortality due to inadequate therapeutic levels. The objective of this study was to estimate the difference in colistin plasma levels in critically ill patients, and its relationship to favorable or unfavorable clinical outcomes. This prospective observational study was conducted between September 2017 and June 2020 at the Univer-sidad de La Sabana Clinic, in patients who had been treated with colistimethate sodium (CMS) for at least 72 h until day 7 of drug treatment in the critical care unit of a university hospital. There were no statistically significant differences in colistin levels between groups with favorable or unfavorable clinical outcomes (0.16 SD vs. 0.54 SD p-value = 0.167). There was higher mortality in patients with subtherapeutic levels (18% vs. 0%), and additionally, there was a greater rate of renal failure in the group with higher therapeutic levels (50% vs. 20.7%). Due to the loss of power of the study, we were unable to demonstrate a possible difference between colistin levels related to favorable or unfavorable clinical outcomes at day 7. However, we recommend further studies to evaluate the impact of measuring levels in terms of mortality and security.

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Sanabria, J., Garzón, V., Pacheco, T., Avila, M. P., Garcia, J. C., Jaimes, D., … Abril, D. (2021). Estimation of the difference in colistin plasma levels in critically ill patients with favorable or unfavorable clinical outcomes. Pharmaceutics, 13(10). https://doi.org/10.3390/pharmaceutics13101630

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