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Journal Article

Citation

Weersink RA, Drenth JPH, Borgsteede SD. JHEP Rep. 2022; 4(12): e100528.

Copyright

(Copyright © 2022, Elsevier Publishing)

DOI

10.1016/j.jhepr.2022.100528

PMID

36275347

PMCID

PMC9583451

Abstract

We thank Tapper and colleagues for their interesting and relevant article on deprescribing benzodiazepines in patients with cirrhosis. The authors conclude that deprescribing zolpidem reduces the risk of falls and fractures in these patients. Yet, the article does not provide an explanation of why specifically zolpidem, and not traditional benzodiazepines, is associated with fractures and falls. We have reason to believe these findings can be explained by the largely altered pharmacokinetics of zolpidem in patients with cirrhosis. Moreover, pharmacokinetic considerations might favour benzodiazepines with a short half-life and glucuronidation as an elimination route above other benzodiazepines. In this letter, we would like to add these pharmacological aspects to the findings of Tapper et al. concerning the safety of benzodiazepines in patients with cirrhosis.

Benzodiazepines are all lipophilic drugs that target receptors in the brain. As with other lipophilic drugs, the liver clears benzodiazepines from the blood. Yet, the extent of clearance depends on the specific drug. In patients with cirrhosis, the ability of the liver to clear medicines from the systemic circulation is affected. This results in increased exposure to drugs and consequently an increased risk of adverse drug reactions. Increased exposure is most prominent for zolpidem. A pharmacokinetic study on zolpidem showed that peak plasma levels were doubled in patients with cirrhosis.

More importantly, elimination half-life increased from about 2 h in individuals without cirrhosis to 10 h in those with cirrhosis, and total exposure was fivefold higher in the group of patients with cirrhosis. The impaired clearance and longer half-life increase the duration of action, the risk of drowsiness in the morning and consequently the risk of falls and fractures. As mentioned, other benzodiazepines are also cleared by the liver. Yet, such large increases in exposure were not seen with these other benzodiazepines.Benzodiazepines have also been linked to an increased risk of (worsening) hepatic encephalopathy.

In the current study, deprescribing benzodiazepines did not decrease the incidence of hepatic encephalopathy. In patients with compensated cirrhosis, the impact of benzodiazepines is more likely to be seen in the early stages of hepatic encephalopathy (grade 1 or 2), and measurement was outside the remit of the study. Moreover, the risk of (worsening of) hepatic encephalopathy is highest in the first weeks of starting the benzodiazepine, as demonstrated by Gronbeak et al. Several cases of hepatic encephalopathy associated with zolpidem have been described in the literature, which suggest that the higher exposure to zolpidem in patients with cirrhosis impacts the risk of hepatic encephalopathy.


Language: en

Keywords

Benzodiazepines; Pharmacology; Cirrhosis; Zolpidem

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