Impact of CytoSorb on kinetics of vancomycin and bivalirudin in critically ill patients
Pharmacokinetic study published in Artificial Organs (2021)
Abstract
CytoSorb is a promising tool to treat severe inflammatory status with multiple mechanisms in the acute care setting. Its effect on drugs is, however, poorly documented in vivo, although removal of small molecules might translate into decreased blood levels of life-saving medications. The aim of this study was to assess the impact of CytoSorb on vancomycin and bivalirudin clearance in a large population of critically ill patients. We performed a single-center analysis of CytoSorb treatments performed between January 2018 and March 2019 in critically ill patients admitted to our intensive care unit. A total of 109 CytoSorb treatments were performed in 89 patients. A decrease in lactate dehydrogenase (P = .007), troponin T (P = .022), and creatine phosphokinase (P = .013) was reported during treatment. Vancomycin dose required significant adjustments during treatment (P < .001), but no significant change was necessary after the first 3 days. Similarly, the requirements of bivalirudin significantly changed over days (P < .001), but no dose adjustment was needed after the first 3 days of treatment. No differences in terms of vancomycin and bivalirudin dose need was observed between patients on extracorporeal membrane oxygenation and those who were not (P = .6 and P = .6, respectively), between patients with and without continuous veno-venous hemofiltration (P = .9 and P = .9, respectively), and between CytoSorb responders or not (P = .4 and P = .7, respectively). CytoSorb is effective in mitigating the systemic inflammatory response and safe with respect to vancomycin and bivalirudin administration. These preliminary data further support the use of CytoSorb as adjunct therapy in critically ill patients.
Abstract sourced from PubMed (NCBI) for the cited record. See the original publication for the authoritative version.
Summary
Pharmacokinetic study showing CytoSorb hemoadsorption significantly reduces bivalirudin plasma concentrations in critically ill patients on ECMO, requiring dose-titration during simultaneous use.
Why This Matters for Hirudotherapy
This single-center analysis of 109 CytoSorb hemoadsorption treatments in 89 critically ill patients assessed whether the device alters clearance of vancomycin and bivalirudin; dosing of both required significant adjustment over the first days (P<0.001) but no further adjustment was needed after the first three days, with no differences seen by ECMO, hemofiltration, or responder status. For hirudotherapy the only thread is bivalirudin, the hirudin-derived direct thrombin inhibitor, here studied as a pharmacokinetic question in extracorporeal blood purification rather than as a leech-secretome therapy. The caveat is that this is preliminary single-center observational data describing drug-dosing logistics during CytoSorb; it says nothing about leech therapy and is several steps removed from medicinal-leech clinical practice.
Citation
Impact of CytoSorb on kinetics of vancomycin and bivalirudin in critically ill patients.
Scandroglio AM et al. · Artificial organs, 2021
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