冠状动脉疾病合并心房颤动患者的肠道微生物群和心脏代谢危险因素

Iryna O. Melnychuk
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CRF which was explored are total cholesterol (TC), triglycerides (TG), low density lipoproteins (LDL), high density lipoproteins (HDL), lipoprotein α (Lpα), apolipoprotein A1 (ApoA1), apolipoprotein B (ApoB), C-reactive protein (CRP), interleukin-6 (IL-6), trymetilamine (TMA) and trymetilamine-N-oxide (TMAO).&#x0D; Results: The significant changes of gut microbiota composition were found in CAD patients with AF paroxysm in comparison with CAD patients without arrythmia as increasing Actinomycetota phulum (P<0.05); increasing Actinobacter Spp. and decreasing Blautia Spp., Roseburia Inulinivorans, Bacteroides Thetaiotaomicron (P<0.05). Moreover, Actinobacter Spp., Akkermansia Muciniphila, Streptococcus Spp., Bacteroides Thetaiotaomicron, Bifidobacterium Spp. have the highest amount of significant correlations with CRF (body mass index, LDL levels; P<0.05). 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引用次数: 0

摘要

目的:评估冠状动脉疾病(CAD)和心房颤动(AF)患者肠道微生物群组成的特殊性,并评估其与已知心脏代谢危险因素(CRF)的关系。材料与方法:300例患者分为3组:ⅰ组-无心律失常的CAD患者149例,ⅱ组-合并心律失常的CAD患者124例,对照组(CG) -无心律失常的CAD患者27例。16-S rRNA测序检查肠道微生物群组成。研究的CRF包括总胆固醇(TC)、甘油三酯(TG)、低密度脂蛋白(LDL)、高密度脂蛋白(HDL)、脂蛋白α (Lpα)、载脂蛋白A1 (ApoA1)、载脂蛋白B (ApoB)、c反应蛋白(CRP)、白细胞介素6 (IL-6)、甲苯胺(TMA)和甲苯胺- n-氧化物(TMAO)。 结果:冠心病合并心房颤动发作患者的肠道菌群组成与非心律失常患者相比有显著变化:放线菌群数量增加(P<0.05);放线菌(Actinobacter Spp.)数量增加,蓝藻菌(Blautia Spp.)、红玫瑰菌(Roseburia Inulinivorans)、拟杆菌(Bacteroides Thetaiotaomicron)数量减少(P<0.05)。其中,放线菌、嗜粘杆菌、链球菌、拟杆菌、双歧杆菌与CRF(体重指数、LDL水平)的显著相关性最高;术中,0.05)。通过roc分析,我们发现乳酸杆菌、双歧杆菌、拟杆菌、蓝杆菌、放线菌和直肠真杆菌在冠心病患者房颤发作中的作用是可以接受的(roc曲线下面积(AUC)& 0.7)。我们发现CAD患者房颤发作AUC最高的肠道菌群组合为放线菌Spp(放线菌Spp + 0.32 *链球菌Spp, AUC = 0.9008;1.56 *放射线杆菌Spp. - Blautia Spp., AUC = 0.9008;1.84 *放射线杆菌Spp. - Akkermansia Muciniphila, AUC = 0.9008)。经多因素线性回归分析,冠心病患者房颤发作时间与血浆IL-6、TMAO、粪便放线菌和嗜粘杆菌有关(房颤发作时间= 0.68*(放线菌,lg/CFU/ml) - 3.33*(嗜粘杆菌,lg/CFU/ml) - 0.6*IL6 - 0.34*TMAO - 0.98)。 结论:冠心病患者发作性心房颤动的发生与肠道菌群状况密切相关。寻找肠道菌群和CRF校正的新途径将是今后研究的热点。
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GUT MICROBIOTA AND CARDIOMETABOLIC RISK FACTORS IN CORONARY ARTERY DISEASE PATIENTS WITH ATRIAL FIBRILLATION
The aim: To estimate gut microbiota composition peculiarities in patients with coronary artery disease (CAD) and atrial fibrillation (AF) and to evaluate their connections with known cardiometabolic risk factors (CRF). Materials and methods: 300 patients formed 3 groups: I group – 149 CAD patients without rhythm disorders, II group – 124 patients with CAD and AF paroxysm and control group (CG) – 27 patients without CAD and arrhythmias. 16-S rRNA sequencing checked gut microbiota composition. CRF which was explored are total cholesterol (TC), triglycerides (TG), low density lipoproteins (LDL), high density lipoproteins (HDL), lipoprotein α (Lpα), apolipoprotein A1 (ApoA1), apolipoprotein B (ApoB), C-reactive protein (CRP), interleukin-6 (IL-6), trymetilamine (TMA) and trymetilamine-N-oxide (TMAO). Results: The significant changes of gut microbiota composition were found in CAD patients with AF paroxysm in comparison with CAD patients without arrythmia as increasing Actinomycetota phulum (P<0.05); increasing Actinobacter Spp. and decreasing Blautia Spp., Roseburia Inulinivorans, Bacteroides Thetaiotaomicron (P<0.05). Moreover, Actinobacter Spp., Akkermansia Muciniphila, Streptococcus Spp., Bacteroides Thetaiotaomicron, Bifidobacterium Spp. have the highest amount of significant correlations with CRF (body mass index, LDL levels; P<0.05). By the ROC-analysis we found the acceptable role of Lactobacillus Spp., Bifidobacterium Spp., Bacteroides Thetaiotaomicron, Blautia Spp., Actinobacter Spp. and Eubacterium Rectale in AF paroxysm occurrence in CAD patients (area under ROC-curve (AUC)<0.7). We found gut microbiota combinations with highest AUC for AF paroxysm in CAD patient: all of them include Actinobacter Spp (Actinobacter Spp. + 0.32 * Streptococcus Spp., AUC = 0.9008; 1.56 * Actinobacter Spp. – Blautia Spp., AUC = 0.9008;1.84 * Actinobacter Spp. – Akkermansia Muciniphila, AUC = 0.9008). AF paroxysm duration in CAD patients depends of plasma IL-6, TMAO, fecal Actinobacter Spp. and Akkermansia Muciniphila by the linear multifactorial regression analysis (AF paroxysm duration = 0.68*(Actinobacter Spp., lg/CFU/ml) – 3.33*(Akkermansia Muciniphila, lg/CFU/ml) – 0.6*IL6 – 0.34*TMAO – 0.98). Conclusions: Gut microbiota condition is closely connected with occurrence AF of paroxysm in CAD patients. To find out the new ways of gut microbiota and CRF correction will be interesting in future investigations.
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