Department of Food and Drugs, University of Parma, Parco Area delle Scienze 27/A, 43124, Parma, Italy.
Department of Chemistry, Life Sciences and Environmental Sustainability, University of Parma, Parco Area delle Scienze 11/A, 43124, Parma, Italy.
Cardiovasc Diabetol. 2017 Jul 6;16(1):80. doi: 10.1186/s12933-017-0561-3.
Emerging evidence suggests that specific (poly)phenols may constitute new preventative strategies to counteract cell oxidative stress and myocardial tissue inflammation, which have a key role in the patho-physiology of diabetic cardiomyopathy. In a rat model of early diabetes, we evaluated whether in vivo administration of urolithin A (UA) or urolithin B (UB), the main gut microbiota phenolic metabolites of ellagitannin-rich foods, can reduce diabetes-induced microenvironmental changes in myocardial tissue, preventing cardiac functional impairment.
Adult Wistar rats with streptozotocin-induced type-1 diabetes (n = 29) were studied in comparison with 10 control animals. Diabetic rats were either untreated (n = 9) or subjected to daily i.p. injection of UA (n = 10) or UB (n = 10). After 3 weeks of hyperglycaemia, hemodynamics, cardiomyocyte contractile properties and calcium transients were measured to assess cardiac performance. The myocardial expression of the pro-inflammatory cytokine fractalkine and proteins involved in calcium dynamics (sarcoplasmic reticulum calcium ATPase, phospholamban and phosphorylated phospholamban) were evaluated by immunoblotting. Plasma, urine and tissue distribution of UA, UB and their phase II metabolites were determined.
In vivo urolithin treatment reduced by approximately 30% the myocardial expression of the pro-inflammatory cytokine fractalkine, preventing the early inflammatory response of cardiac cells to hyperglycaemia. The improvement in myocardial microenvironment had a functional counterpart, as documented by the increase in the maximal rate of ventricular pressure rise compared to diabetic group (+18% and +31% in UA and UB treated rats, respectively), and the parallel reduction in the isovolumic contraction time (-12%). In line with hemodynamic data, both urolithins induced a recovery of cardiomyocyte contractility and calcium dynamics, leading to a higher re-lengthening rate (+21%, on average), lower re-lengthening times (-56%), and a more efficient cytosolic calcium clearing (-32% in tau values). UB treatment also increased the velocity of shortening (+27%). Urolithin metabolites accumulated in the myocardium, with a higher concentration of UB and UB-sulphate, potentially explaining the slightly higher efficacy of UB administration.
In vivo urolithin administration may be able to prevent the initial inflammatory response of myocardial tissue to hyperglycaemia and the negative impact of the altered diabetic milieu on cardiac performance.
新出现的证据表明,特定的(多)酚类化合物可能成为新的预防策略,以对抗细胞氧化应激和心肌组织炎症,这些在糖尿病心肌病的病理生理学中起着关键作用。在早期糖尿病大鼠模型中,我们评估了体内给予尿石素 A(UA)或尿石素 B(UB),即富含鞣花单宁的食物的主要肠道微生物酚代谢物,是否可以减少糖尿病引起的心肌组织微环境变化,从而防止心脏功能障碍。
用链脲佐菌素诱导的 1 型糖尿病大鼠(n=29)与 10 只对照动物进行比较。糖尿病大鼠分为未治疗组(n=9)或每天腹腔注射 UA(n=10)或 UB(n=10)。在高血糖 3 周后,测量血流动力学、心肌细胞收缩性能和钙瞬变,以评估心脏功能。通过免疫印迹法评估促炎细胞因子 fractalkine 以及钙动态相关蛋白(肌浆网钙 ATP 酶、磷酸化肌浆网钙结合蛋白和磷酸化肌浆网钙结合蛋白)的心肌表达。测定 UA、UB 及其相 II 代谢物在血浆、尿液和组织中的分布。
体内给予尿石素治疗可使促炎细胞因子 fractalkine 的心肌表达减少约 30%,从而防止心脏细胞对高血糖的早期炎症反应。心肌微环境的改善有一个功能对应物,这体现在与糖尿病组相比,心室压上升的最大速率增加(UA 和 UB 治疗组分别增加+18%和+31%),以及等容收缩时间平行减少(-12%)。与血流动力学数据一致,两种尿石素均诱导心肌收缩力和钙动力学恢复,导致再伸长率增加(平均增加+21%),再伸长时间减少(-56%),细胞浆钙清除效率更高(tau 值减少-32%)。UB 治疗还增加了缩短速度(+27%)。尿石素代谢物在心内积聚,UB 和 UB-硫酸盐浓度较高,这可能解释了 UB 给药的效果略高。
体内给予尿石素治疗可能能够预防心肌组织对高血糖的初始炎症反应,以及改变的糖尿病环境对心脏功能的负面影响。
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