Time‐Resolved Evaluation of L‐Dopa Metabolism in Bacteria‐Host Symbiotic System and the Effect on Parkinson's Molecular Pathology

Author:

Kim Doyeon1,Nguyen Tin Tin Manh1,Moon Yechan1,Kim Jin‐Mo1,Nam Hoonsik1,Cha Dong Seok2,An Yong Jin1,de Guzman Arvie Camille V.1ORCID,Park Sunghyouk1ORCID

Affiliation:

1. Natural Products Research Institute College of Pharmacy Seoul National University Seoul 08826 South Korea

2. College of Pharmacy Woosuk University Jeonbuk 55338 South Korea

Abstract

AbstractThe gut microbiome influences drug metabolism and therapeutic efficacy. Still, the lack of a general label‐free approach for monitoring bacterial or host metabolic contribution hampers deeper insights. Here, a 2D nuclear magnetic resonance (NMR) approach is introduced that enables real‐time monitoring of the metabolism of Levodopa (L‐dopa), an anti‐Parkinson drug, in both live bacteria and bacteria‐host (Caenorhabditis elegans) symbiotic systems. The quantitative method reveals that discrete Enterococcus faecalis substrains produce different amounts of dopamine in live hosts, even though they are a single species and all have the Tyrosine decarboxylase (TyrDC) gene involved in L‐dopa metabolism. The differential bacterial metabolic activity correlates with differing Parkinson's molecular pathology concerning alpha‐synuclein aggregation as well as behavioral phenotypes. The gene's existence or expression is not an indicator of metabolic activity is also shown, underscoring the significance of quantitative metabolic estimation in vivo. This simple approach is widely adaptable to any chemical drug to elucidate pharmacomicrobiomic relationships and may help rapidly screen bacterial metabolic effects in drug development.

Funder

National Research Foundation of Korea

Ministry of Education

Publisher

Wiley

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