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Pharmacomicrobiomics: Immunosuppressive Drugs and Microbiome Interactions in Transplantation. | LitMetric

AI Article Synopsis

  • The human microbiome plays a significant role in both health and disease, influencing how drugs are metabolized, which can lead to varying side effects and unexpected responses to medications.
  • Pharmacomicobiomics is an emerging field that studies the interactions between the microbiome and pharmaceuticals, taking advantage of advancements in genome sequencing and bioinformatics.
  • Current research highlights how the microbiome affects drug metabolism in transplant recipients, particularly with drugs like tacrolimus and mycophenolate, though more extensive clinical studies are necessary to fully understand these interactions and their clinical implications.

Article Abstract

The human microbiome is associated with human health and disease. Exogenous compounds, including pharmaceutical products, are also known to be affected by the microbiome, and this discovery has led to the field of pharmacomicobiomics. The microbiome can also alter drug pharmacokinetics and pharmacodynamics, possibly resulting in side effects, toxicities, and unanticipated disease response. Microbiome-mediated effects are referred to as drug-microbiome interactions (DMI). Rapid advances in the field of pharmacomicrobiomics have been driven by the availability of efficient bacterial genome sequencing methods and new computational and bioinformatics tools. The success of fecal microbiota transplantation for recurrent Clostridioides difficile has fueled enthusiasm and research in the field. This review focuses on the pharmacomicrobiome in transplantation. Alterations in the microbiome in transplant recipients are well documented, largely because of prophylactic antibiotic use, and the potential for DMI is high. There is evidence that the gut microbiome may alter the pharmacokinetic disposition of tacrolimus and result in microbiome-specific tacrolimus metabolites. The gut microbiome also impacts the enterohepatic recirculation of mycophenolate, resulting in substantial changes in pharmacokinetic disposition and systemic exposure. The mechanisms of these DMI and the specific bacteria or communities of bacteria are under investigation. There are little or no human DMI data for cyclosporine A, corticosteroids, and sirolimus. The available evidence in transplantation is limited and driven by small studies of heterogeneous designs. Larger clinical studies are needed, but the potential for future clinical application of the pharmacomicrobiome in avoiding poor outcomes is high.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11327386PMC
http://dx.doi.org/10.1097/TP.0000000000004926DOI Listing

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