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长期膳食中富含槲皮素作为mdx小鼠心脏保护对策。

Long-term dietary quercetin enrichment as a cardioprotective countermeasure in mdx mice.

作者信息

Ballmann Christopher, Denney Thomas, Beyers Ronald J, Quindry Tiffany, Romero Matthew, Selsby Joshua T, Quindry John C

机构信息

School of Kinesiology, Auburn University, Auburn, AL, USA.

MRI Research Center, Auburn University, Auburn, AL, USA.

出版信息

Exp Physiol. 2017 Jun 1;102(6):635-649. doi: 10.1113/EP086091. Epub 2017 Mar 30.

Abstract

What is the central question of this study? The central question of this study is to understand whether dietary quercetin enrichment attenuates physiologic, histological, and biochemical indices of cardiac pathology. What is the main finding and its importance? Novel findings from this investigation, in comparison to prior published studies, suggest that mouse strain-dependent cardiac outcomes in performance and remodelling exist. Unlike Mdx/Utrn mice, mdx mice receiving lifelong quercetin treatment did not exhibit improvements cardiac function. Similar to prior work in Mdx/Utrn mice, histological evidence of remodelling suggests that quercetin consumption may have benefited hearts of mdx mice. Positive outcomes may be related to indirect markers that suggest improved mitochondrial wellbeing and to selected indices of inflammation that were lower in hearts from quercetin-fed mice. Duchenne muscular dystrophy causes a decline in cardiac health, resulting in premature mortality. As a potential countermeasure, quercetin is a polyphenol possessing inherent anti-inflammatory and antioxidant effects that activate proliferator-activated γ coactivator 1α (PGC-1α), increasing the abundance of mitochondrial biogenesis proteins. We investigated the extent to which lifelong 0.2% dietary quercetin enrichment attenuates dystrophic cardiopathology in mdx mice. Dystrophic animals were fed a quercetin-enriched or control diet for 12 months, while control C57 mice were fed a control diet. Cardiac function was assessed via 7 T magnetic resonance imaging at 2, 10 and 14 months. At 14 months, hearts were harvested for histology and Western blotting. The results indicated an mdx strain-dependent decline in cardiac performance at 14 months and that dietary quercetin enrichment did not attenuate functional losses. In contrast, histological analyses provided evidence that quercetin feeding was associated with decreased fibronectin and indirect damage indices (Haematoxylin and Eosin) compared with untreated mdx mice. Dietary quercetin enrichment increased cardiac protein abundance of PGC-1α, cytochrome c, electron transport chain complexes I-V, citrate synthase, superoxide dismutase 2 and glutathione peroxidase (GPX) versus untreated mdx mice. The protein abundance of the inflammatory markers nuclear factor-κB, phosphorylated nuclear factor kappa beta (P-NFκB) and phosphorylated nuclear factor of kappa light polypeptide gene enhancer in B-cells inhibitor alpha (P-IKBα) was decreased by quercetin compared with untreated mdx mice, while preserving nuclear factor of kappa light polypeptide gene enhancer in B-cells inhibitor alpha( IKBα) compared with mdx mice. Furthermore, quercetin decreased transforming growth factor-β1, cyclooxygenase-2 (COX2) and macrophage-restricted F4/80 protein (F4/80) versus untreated mdx mice. The data suggest that long-term quercetin enrichment does not impact physiological parameters of cardiac function but improves indices of mitochondrial biogenesis and antioxidant enzymes, facilitates dystrophin-associated glycoprotein complex (DGC) assembly and decreases inflammation in dystrophic hearts.

摘要

本研究的核心问题是什么?本研究的核心问题是了解膳食中槲皮素的富集是否能减轻心脏病理的生理、组织学和生化指标。主要发现及其重要性是什么?与先前发表的研究相比,本调查的新发现表明,在心脏性能和重塑方面存在小鼠品系依赖性的心脏结果。与Mdx/Utrn小鼠不同,接受终身槲皮素治疗的mdx小鼠心脏功能并未改善。与先前在Mdx/Utrn小鼠中的研究相似,重塑的组织学证据表明,食用槲皮素可能对mdx小鼠的心脏有益。积极结果可能与提示线粒体健康状况改善的间接标志物以及槲皮素喂养小鼠心脏中较低的选定炎症指标有关。杜氏肌营养不良会导致心脏健康下降,从而导致过早死亡。作为一种潜在的对策,槲皮素是一种具有内在抗炎和抗氧化作用的多酚,可激活增殖激活γ共激活因子1α(PGC-1α),增加线粒体生物发生蛋白的丰度。我们研究了终身0.2%膳食槲皮素富集在多大程度上减轻mdx小鼠的营养不良性心脏病理。给营养不良的动物喂食富含槲皮素的饮食或对照饮食12个月,而对照C57小鼠喂食对照饮食。在2个月、10个月和14个月时通过7T磁共振成像评估心脏功能。在14个月时,采集心脏进行组织学和蛋白质印迹分析。结果表明,在14个月时mdx品系存在心脏性能下降,且膳食中槲皮素的富集并未减轻功能损失。相比之下,组织学分析提供的证据表明,与未治疗的mdx小鼠相比,喂食槲皮素与纤连蛋白减少和间接损伤指标(苏木精和伊红)降低有关。与未治疗的mdx小鼠相比,膳食中槲皮素的富集增加了PGC-1α、细胞色素c、电子传递链复合物I-V、柠檬酸合酶、超氧化物歧化酶2和谷胱甘肽过氧化物酶(GPX)的心脏蛋白丰度。与未治疗的mdx小鼠相比,槲皮素降低了炎症标志物核因子-κB、磷酸化核因子κB(P-NFκB)和B细胞抑制剂α中κ轻链多肽基因增强子的磷酸化核因子(P-IKBα)的蛋白丰度,而与mdx小鼠相比保留了B细胞抑制剂α(IKBα)中κ轻链多肽基因增强子的核因子。此外,与未治疗的mdx小鼠相比,槲皮素降低了转化生长因子-β1、环氧合酶-2(COX2)和巨噬细胞特异性F4/80蛋白(F4/80)。数据表明,长期的槲皮素富集不会影响心脏功能的生理参数,但会改善线粒体生物发生和抗氧化酶指标,促进肌营养不良蛋白相关糖蛋白复合物(DGC)组装,并减少营养不良心脏中的炎症。

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