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细菌-宿主共生系统中左旋多巴代谢的时间分辨评估及其对帕金森病分子病理学的影响。

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

作者信息

Kim Doyeon, Nguyen Tin Tin Manh, Moon Yechan, Kim Jin-Mo, Nam Hoonsik, Cha Dong Seok, An Yong Jin, de Guzman Arvie Camille V, Park Sunghyouk

机构信息

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

College of Pharmacy Woosuk University, Jeonbuk, 55338, South Korea.

出版信息

Small Methods. 2025 Mar;9(3):e2400469. doi: 10.1002/smtd.202400469. Epub 2024 Jul 26.

Abstract

The 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.

摘要

肠道微生物群会影响药物代谢和治疗效果。然而,缺乏一种通用的无标记方法来监测细菌或宿主的代谢贡献阻碍了更深入的研究。在此,引入了一种二维核磁共振(NMR)方法,该方法能够实时监测抗帕金森药物左旋多巴(L-多巴)在活细菌以及细菌-宿主(秀丽隐杆线虫)共生系统中的代谢情况。该定量方法显示,尽管粪肠球菌的不同菌株属于单一物种且都拥有参与L-多巴代谢的酪氨酸脱羧酶(TyrDC)基因,但它们在活宿主中产生的多巴胺量不同。细菌代谢活性的差异与帕金森病在α-突触核蛋白聚集以及行为表型方面不同的分子病理学相关。研究还表明,基因的存在或表达并非代谢活性的指标,这突出了体内定量代谢评估的重要性。这种简单的方法可广泛应用于任何化学药物,以阐明药物微生物组学关系,并可能有助于在药物开发中快速筛选细菌代谢效应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1279/11926514/069941ecddd8/SMTD-9-2400469-g004.jpg

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