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长效抗凝血杀鼠剂溴敌隆对新西兰白兔盲肠微生物群的影响

Alterations in the cecal microbiome of New Zealand White rabbits due to the long-acting anticoagulant rodenticide brodifacoum.

作者信息

Naqib Ankur, Ahmad Intakhar, McDonald Zachary, Kalinin Sergey, Rocha Jackie, Tandon Ankit, Rayala Ramanjaneyulu, Feferman Leonid, Chlipala George E, Chen Hui, Lindeblad Matthew, Rubinstein Israel, Green Stefan, van Breemen Richard, Feinstein Douglas L

机构信息

Genomics and Microbiome Core Facility, Rush University, Chicago, Illinois, 60612, USA.

Department of Anesthesiology, University of Illinois, Chicago, Illinois 60612, USA.

出版信息

Toxicol Commun. 2025;9(1). doi: 10.1080/24734306.2025.2500111. Epub 2025 May 12.

Abstract

Long-acting anti-coagulant rodenticides (LAARs) are well characterized with respect to inhibition of vitamin K1 synthesis and effects on blood coagulation. However, the effects of LAARs on the microbiome have not been explored. We administered brodifacoum (BDF), one of the more potent LAARs, to adult male New Zealand White rabbits, and carried out 16S RNA sequencing on cecal samples collected after different times. Samples were also obtained from rabbits treated with the bile sequestrant cholestyramine (CSA) which accelerates BDF clearance from the body, and from CSA-only treated rabbits. Changes at both the phylum and genus levels in relative abundance were observed after 2- and 3-days exposure to BDF. The majority of those microbiota changes were prevented by co-treatment with CSA. Identification of metabolic pathways potentially altered by BDF using Picrust2 identified several L-arginine-related pathways. Exposure to BDF caused increases in plasma L-arginine concentration as well as nitrites, suggesting increased activity of nitric oxide synthase. We also observed increases due to BDF in plasma concentrations of L-arginine-related molecules including L-citrulline, L-ornithine, and methylated L-arginines. These results demonstrate that LAAR poisoning can induce microbiome dysbiosis and influence metabolic pathways and metabolites involved in inflammation and vasodilation.

摘要

长效抗凝血灭鼠剂(LAARs)在抑制维生素K1合成以及对血液凝固的影响方面已有充分的特征描述。然而,LAARs对微生物群的影响尚未得到研究。我们给成年雄性新西兰白兔施用了更有效的LAARs之一溴敌隆(BDF),并对在不同时间采集的盲肠样本进行了16S RNA测序。样本还取自用胆汁螯合剂消胆胺(CSA)治疗的兔子,CSA可加速BDF从体内清除,以及仅用CSA治疗的兔子。在接触BDF 2天和3天后,观察到门和属水平相对丰度的变化。与CSA联合治疗可防止这些微生物群变化中的大多数。使用Picrust2鉴定可能被BDF改变的代谢途径,确定了几个与L-精氨酸相关的途径。接触BDF导致血浆L-精氨酸浓度以及亚硝酸盐增加,表明一氧化氮合酶活性增加。我们还观察到BDF导致血浆中与L-精氨酸相关的分子浓度增加,包括L-瓜氨酸、L-鸟氨酸和甲基化L-精氨酸。这些结果表明,LAAR中毒可诱导微生物群失调,并影响参与炎症和血管舒张的代谢途径和代谢产物。

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