Literature DB >> 30598508

Commensal Gut Bacteria Convert the Immunosuppressant Tacrolimus to Less Potent Metabolites.

Yukuang Guo1, Camila Manoel Crnkovic1, Kyoung-Jae Won1, Xiaotong Yang1, John Richard Lee1, Jimmy Orjala2, Hyunwoo Lee2, Hyunyoung Jeong2.   

Abstract

Tacrolimus exhibits low and variable drug exposure after oral dosing, but the contributing factors remain unclear. Based on our recent report showing a positive correlation between fecal abundance of Faecalibacterium prausnitzii and oral tacrolimus dose in kidney transplant patients, we tested whether F. prausnitzii and other gut abundant bacteria are capable of metabolizing tacrolimus. Incubation of F. prausnitzii with tacrolimus led to production of two compounds (the major one named M1), which was not observed upon tacrolimus incubation with hepatic microsomes. Isolation, purification, and structure elucidation using mass spectrometry and nuclear magnetic resonance spectroscopy indicated that M1 is a C-9 keto-reduction product of tacrolimus. Pharmacological activity testing using human peripheral blood mononuclear cells demonstrated that M1 is 15-fold less potent than tacrolimus as an immunosuppressant. Screening of 22 gut bacteria species revealed that most Clostridiales bacteria are extensive tacrolimus metabolizers. Tacrolimus conversion to M1 was verified in fresh stool samples from two healthy adults. M1 was also detected in the stool samples from kidney transplant recipients who had been taking tacrolimus orally. Together, this study presents gut bacteria metabolism as a previously unrecognized elimination route of tacrolimus, potentially contributing to the low and variable tacrolimus exposure after oral dosing.
Copyright © 2019 by The American Society for Pharmacology and Experimental Therapeutics.

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Year:  2018        PMID: 30598508      PMCID: PMC6367689          DOI: 10.1124/dmd.118.084772

Source DB:  PubMed          Journal:  Drug Metab Dispos        ISSN: 0090-9556            Impact factor:   3.922


  21 in total

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Review 2.  Precision Medicine Goes Microscopic: Engineering the Microbiome to Improve Drug Outcomes.

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Review 4.  Gastrointestinal biofilms in health and disease.

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Journal:  Nat Rev Gastroenterol Hepatol       Date:  2021-01-28       Impact factor: 46.802

Review 5.  Influence of the microbiome on solid organ transplant survival.

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Review 6.  Recent advances in the ontogeny of drug disposition.

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Review 7.  Bringing microbiome-drug interaction research into the clinic.

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8.  Identification of Antibiotic Administration as a Potentially Novel Factor Associated With Tacrolimus Trough Variability in Kidney Transplant Recipients: A Preliminary Study.

Authors:  YuanPu Zheng; Anjali Masand; Michael Wagner; Sandip Kapur; Darshana Dadhania; Michelle Lubetzky; John Richard Lee
Journal:  Transplant Direct       Date:  2019-08-23

9.  Colonizing multidrug-resistant bacteria and the longitudinal evolution of the intestinal microbiome after liver transplantation.

Authors:  Medini K Annavajhala; Angela Gomez-Simmonds; Nenad Macesic; Sean B Sullivan; Anna Kress; Sabrina D Khan; Marla J Giddins; Stephania Stump; Grace I Kim; Ryan Narain; Elizabeth C Verna; Anne-Catrin Uhlemann
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Review 10.  Targeting gut microbiota for precision medicine: Focusing on the efficacy and toxicity of drugs.

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Journal:  Theranostics       Date:  2020-09-14       Impact factor: 11.556

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