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.
Mol Nutr Food Res. 2021 Mar;65(6):e2001048. doi: 10.1002/mnfr.202001048. Epub 2021 Feb 11.
Poly-pharmacological therapy shapes the gut microbiota (GM) in metabolic syndrome (MetS) patients. The effects of polyphenols in poly-medicated MetS patients are unknown.
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.
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.
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。
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。
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。
