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丁酸盐对高血压患者结肠中受损基因表达的影响。

Influence of Butyrate on Impaired Gene Expression in Colon from Patients with High Blood Pressure.

机构信息

Key Laboratory of Plant Germplasm Enhancement and Specialty Agriculture, Wuhan Botanical Garden, Chinese Academy of Sciences, Wuhan 430074, China.

Department of Physiology and Aging, University of Florida College of Medicine, Gainesville, FL 32610, USA.

出版信息

Int J Mol Sci. 2023 Jan 31;24(3):2650. doi: 10.3390/ijms24032650.

Abstract

Hypertension (HTN) is associated with gut dysbiosis and the depletion of butyrate-producing bacteria in animal models and people. Furthermore, fecal material transfer from donor hypertensive patients increases blood pressure in normotensive recipient animals and ameliorates HTN-associated pathophysiology. These observations have implications in the impaired interactions between the gut and gut microbiota in HTN. Although this concept is supported in animal models, little is known about human HTN. Therefore, our objective for this study was to compare gene expression with transcriptomics and its potential to influence microbiota in subjects with normal and high blood pressure (HBP). Colon samples from reference subjects with normal blood pressure (REF) and HBP were used for RNA-seq to analyze their transcriptomes. We observed the significant downregulation of gene sets governing immune responses (e.g., and ), gut epithelial function (e.g., and ), gut microbiota (e.g., and ) and genes associated with cardiovascular and gut diseases (e.g., and ) in HBP subjects; the expression of genes within these pathways correlated with blood pressure. Potential drug targets in the gut epithelium were identified using the Drug Gene International Database for possible use in HTN. They include peroxisome proliferator-activated receptor gamma ( active serum/glucocorticoid regulated kinase 1 and 3 beta-hydroxysteroid isomerase type II inhibitor Finally, butyrate, a microbiota-derived short-chain fatty acid, restored the disrupted expression of certain functional genes in colonic organoids from HBP subjects. Patients with HBP exhibit a unique transcriptome that could underlie impaired gut-microbiota interactions. Targeting these interactions could provide a promising new therapeutic intervention for hypertension management.

摘要

高血压(HTN)与肠道菌群失调和产丁酸细菌耗竭有关,在动物模型和人类中均有体现。此外,来自高血压供体患者的粪便物质转移可使血压正常的受体动物血压升高,并改善与 HTN 相关的病理生理。这些观察结果提示了 HTN 中肠道与肠道微生物群之间相互作用受损。尽管这一概念在动物模型中得到了支持,但关于人类 HTN 的了解甚少。因此,我们本研究的目的是比较正常血压(REF)和高血压(HBP)受试者的基因表达与转录组学及其对微生物群的潜在影响。使用 RNA-seq 分析参考受试者的结肠样本(REF 和 HBP)的转录组。我们观察到 HBP 受试者中负责免疫反应的基因集(例如, 和 )、肠道上皮功能(例如, 和 )、肠道微生物群(例如, 和 )以及与心血管和肠道疾病相关的基因(例如, 和 )显著下调;这些通路中的基因表达与血压相关。使用 Drug Gene International Database 确定了肠道上皮中的潜在药物靶点,以便在 HTN 中可能使用。它们包括过氧化物酶体增殖物激活受体 γ( 活性血清/糖皮质激素调节激酶 1 和 3β-羟甾醇异构酶 II 抑制剂 )。最后,丁酸,一种微生物群衍生的短链脂肪酸,可恢复 HBP 受试者结肠类器官中某些功能基因的失调表达。高血压患者表现出独特的转录组,这可能是肠道微生物群相互作用受损的基础。针对这些相互作用可能为高血压管理提供一种有前途的新治疗干预措施。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9580/9917256/b6c8f29b07a7/ijms-24-02650-g001.jpg

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