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药理治疗决定了石榴提取物营养保健品对代谢综合征肠道微生物群的调节作用:一项随机临床试验。

Pharmacological Therapy Determines the Gut Microbiota Modulation by a Pomegranate Extract Nutraceutical in Metabolic Syndrome: A Randomized Clinical Trial.

机构信息

Laboratory of Food & Health, Research Group on Quality, Safety and Bioactivity of Plant Foods, CEBAS-CSIC, Campus de Espinardo, Murcia, 30100, Spain.

Service of Endocrinology, Reina Sofía University Hospital, Avda. Intendente Jorge Palacios s/n, Murcia, 30003, Spain.

出版信息

Mol Nutr Food Res. 2021 Mar;65(6):e2001048. doi: 10.1002/mnfr.202001048. Epub 2021 Feb 11.

DOI:10.1002/mnfr.202001048
PMID:33458928
Abstract

SCOPE

Poly-pharmacological therapy shapes the gut microbiota (GM) in metabolic syndrome (MetS) patients. The effects of polyphenols in poly-medicated MetS patients are unknown.

METHODS AND RESULTS

A randomized, placebo-controlled, double-blinded, and crossover trial in poly-medicated MetS patients (n=50) explored whether the effects of a pomegranate extract nutraceutical (PE, 320 mg phenolics/day for 1 month) are affected by the drug therapy. Considering the lipid-lowering (LL-), anti-hypertensive (HP-) and(or) anti-diabetic (AD-) treatments: GM (16S rRNA sequencing), short-chain fatty acids, 40 inflammatory-metabolic and endotoxemia-related biomarkers, associations between biomarkers and GM with 53 cardiometabolic dysfunctions-related single-nucleotide polymorphisms (SNPs), and urolithin metabotypes (UMs) influence are evaluated. Representative SNPs-GM associations after PE include Lactococcus and ClostridiumXIVa with rs5443-GNB3 (G-protein-β-polypeptide-3) and ClostridiumXIVa with rs7903146-TCF7L2 (transcription-factor-7-like-2) and rs1137101-LEPR (leptin-receptor). PE decreases sICAM-1 in LL-patients and the lipopolysaccharide-binding protein in all the patients. PE does not affect the other patients' markers as a group or stratifying by UMs. After PE, Lactococcus increases in AD-, LL-, and HP-patients, Bifidobacterium increases in LL- and AD-, while Clostridium XIVa decreases in non-LL- and non-HP-patients.

CONCLUSION

The prebiotic effect of PE depends on the medication, mainly on HP-treatments. Targeting GM can complement MetS therapy, but the patients' drug therapy should be considered individually.

摘要

范围

多药物治疗会改变代谢综合征(MetS)患者的肠道微生物群(GM)。多酚在多药物治疗 MetS 患者中的作用尚不清楚。

方法和结果

一项针对多药物治疗 MetS 患者(n=50)的随机、安慰剂对照、双盲、交叉试验,旨在探讨石榴提取物营养补充剂(PE,每天 320mg 多酚,持续 1 个月)的作用是否受药物治疗的影响。考虑到降脂(LL-)、降压(HP-)和/或降血糖(AD-)治疗:GM(16S rRNA 测序)、短链脂肪酸、40 种炎症代谢和内毒素血症相关生物标志物、生物标志物与 GM 与 53 种与心血管代谢功能障碍相关的单核苷酸多态性(SNP)之间的关联,以及尿石素代谢型(UM)的影响,进行了评估。PE 后代表性的 SNP-GM 关联包括 Lactococcus 和 ClostridiumXIVa 与 rs5443-GNB3(G 蛋白-β-多肽-3)和 ClostridiumXIVa 与 rs7903146-TCF7L2(转录因子-7 样-2)和 rs1137101-LEPR(瘦素受体)。PE 降低了 LL-患者的 sICAM-1 和所有患者的脂多糖结合蛋白。PE 作为一个组或按 UM 分层对其他患者的标志物没有影响。PE 后,AD-、LL-和 HP-患者的 Lactococcus 增加,LL-和 AD-患者的双歧杆菌增加,而非 LL-和非 HP-患者的 Clostridium XIVa 减少。

结论

PE 的益生元作用取决于药物治疗,主要取决于 HP 治疗。靶向 GM 可以补充 MetS 治疗,但应根据患者的药物治疗情况进行个体化考虑。

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