Human gut Actinobacteria boost drug absorption by secreting P-glycoprotein ATPase inhibitors

Than S. Kyaw; Chen Zhang; Moriah Sandy; Kai Trepka; Shenwei Zhang; Luis A. Ramirez Hernandez; Lorenzo Ramirez; Janice J.N. Goh; Kristie Yu; Vincent Dimassa; Elizabeth N. Bess; Jacob G. Brockert; Darren S. Dumlao; Jordan E. Bisanz; Peter J. Turnbaugh

doi:10.1016/j.isci.2024.110122

Human gut Actinobacteria boost drug absorption by secreting P-glycoprotein ATPase inhibitors

Than S. Kyaw
, Chen Zhang
, Moriah Sandy
, Kai Trepka
, Shenwei Zhang
, Luis A. Ramirez Hernandez
, Lorenzo Ramirez
, Janice J.N. Goh
, Kristie Yu
, Vincent Dimassa
, Elizabeth N. Bess
, Jacob G. Brockert
, Darren S. Dumlao
, Jordan E. Bisanz
, Peter J. Turnbaugh

Research output: Contribution to journal › Article › peer-review

4 Scopus citations

Abstract

Drug efflux transporters are a major determinant of drug efficacy and toxicity. A canonical example is P-glycoprotein (P-gp), an efflux transporter that controls the intestinal absorption of diverse compounds. Despite a rich literature on the dietary and pharmaceutical compounds that impact P-gp activity, its sensitivity to gut microbial metabolites remains an open question. Surprisingly, we found that the cardiac drug-metabolizing gut Actinobacterium Eggerthella lenta increases drug absorption in mice. Experiments in cell culture revealed that E. lenta produces a soluble factor that post-translationally inhibits P-gp ATPase efflux activity. P-gp inhibition is conserved in the Eggerthellaceae family but absent in other Actinobacteria. Comparative genomics identified genes associated with P-gp inhibition. Finally, activity-guided biochemical fractionation coupled to metabolomics implicated a group of small polar metabolites with P-gp inhibitory activity. These results highlight the importance of considering the broader relevance of the gut microbiome for drug disposition beyond first-pass metabolism.

Original language	English (US)
Article number	110122
Journal	iScience
Volume	27
Issue number	6
DOIs	https://doi.org/10.1016/j.isci.2024.110122
State	Published - Jun 21 2024

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10.1016/j.isci.2024.110122

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Kyaw, T. S., Zhang, C., Sandy, M., Trepka, K., Zhang, S., Ramirez Hernandez, L. A., Ramirez, L., Goh, J. J. N., Yu, K., Dimassa, V., Bess, E. N., Brockert, J. G., Dumlao, D. S., Bisanz, J. E., & Turnbaugh, P. J. (2024). Human gut Actinobacteria boost drug absorption by secreting P-glycoprotein ATPase inhibitors. iScience, 27(6), Article 110122. https://doi.org/10.1016/j.isci.2024.110122

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title = "Human gut Actinobacteria boost drug absorption by secreting P-glycoprotein ATPase inhibitors",

abstract = "Drug efflux transporters are a major determinant of drug efficacy and toxicity. A canonical example is P-glycoprotein (P-gp), an efflux transporter that controls the intestinal absorption of diverse compounds. Despite a rich literature on the dietary and pharmaceutical compounds that impact P-gp activity, its sensitivity to gut microbial metabolites remains an open question. Surprisingly, we found that the cardiac drug-metabolizing gut Actinobacterium Eggerthella lenta increases drug absorption in mice. Experiments in cell culture revealed that E. lenta produces a soluble factor that post-translationally inhibits P-gp ATPase efflux activity. P-gp inhibition is conserved in the Eggerthellaceae family but absent in other Actinobacteria. Comparative genomics identified genes associated with P-gp inhibition. Finally, activity-guided biochemical fractionation coupled to metabolomics implicated a group of small polar metabolites with P-gp inhibitory activity. These results highlight the importance of considering the broader relevance of the gut microbiome for drug disposition beyond first-pass metabolism.",

author = "Kyaw, \{Than S.\} and Chen Zhang and Moriah Sandy and Kai Trepka and Shenwei Zhang and \{Ramirez Hernandez\}, \{Luis A.\} and Lorenzo Ramirez and Goh, \{Janice J.N.\} and Kristie Yu and Vincent Dimassa and Bess, \{Elizabeth N.\} and Brockert, \{Jacob G.\} and Dumlao, \{Darren S.\} and Bisanz, \{Jordan E.\} and Turnbaugh, \{Peter J.\}",

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year = "2024",

month = jun,

day = "21",

doi = "10.1016/j.isci.2024.110122",

language = "English (US)",

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T1 - Human gut Actinobacteria boost drug absorption by secreting P-glycoprotein ATPase inhibitors

AU - Kyaw, Than S.

AU - Zhang, Chen

AU - Sandy, Moriah

AU - Trepka, Kai

AU - Zhang, Shenwei

AU - Ramirez Hernandez, Luis A.

AU - Ramirez, Lorenzo

AU - Goh, Janice J.N.

AU - Yu, Kristie

AU - Dimassa, Vincent

AU - Bess, Elizabeth N.

AU - Brockert, Jacob G.

AU - Dumlao, Darren S.

AU - Bisanz, Jordan E.

AU - Turnbaugh, Peter J.

PY - 2024/6/21

Y1 - 2024/6/21

N2 - Drug efflux transporters are a major determinant of drug efficacy and toxicity. A canonical example is P-glycoprotein (P-gp), an efflux transporter that controls the intestinal absorption of diverse compounds. Despite a rich literature on the dietary and pharmaceutical compounds that impact P-gp activity, its sensitivity to gut microbial metabolites remains an open question. Surprisingly, we found that the cardiac drug-metabolizing gut Actinobacterium Eggerthella lenta increases drug absorption in mice. Experiments in cell culture revealed that E. lenta produces a soluble factor that post-translationally inhibits P-gp ATPase efflux activity. P-gp inhibition is conserved in the Eggerthellaceae family but absent in other Actinobacteria. Comparative genomics identified genes associated with P-gp inhibition. Finally, activity-guided biochemical fractionation coupled to metabolomics implicated a group of small polar metabolites with P-gp inhibitory activity. These results highlight the importance of considering the broader relevance of the gut microbiome for drug disposition beyond first-pass metabolism.

AB - Drug efflux transporters are a major determinant of drug efficacy and toxicity. A canonical example is P-glycoprotein (P-gp), an efflux transporter that controls the intestinal absorption of diverse compounds. Despite a rich literature on the dietary and pharmaceutical compounds that impact P-gp activity, its sensitivity to gut microbial metabolites remains an open question. Surprisingly, we found that the cardiac drug-metabolizing gut Actinobacterium Eggerthella lenta increases drug absorption in mice. Experiments in cell culture revealed that E. lenta produces a soluble factor that post-translationally inhibits P-gp ATPase efflux activity. P-gp inhibition is conserved in the Eggerthellaceae family but absent in other Actinobacteria. Comparative genomics identified genes associated with P-gp inhibition. Finally, activity-guided biochemical fractionation coupled to metabolomics implicated a group of small polar metabolites with P-gp inhibitory activity. These results highlight the importance of considering the broader relevance of the gut microbiome for drug disposition beyond first-pass metabolism.

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AN - SCOPUS:85195189117

SN - 2589-0042

VL - 27

JO - iScience

JF - iScience

IS - 6

M1 - 110122

ER -

Human gut Actinobacteria boost drug absorption by secreting P-glycoprotein ATPase inhibitors

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