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Meeting report: ISN forefronts in nephrology on endothelial biology and renal disease: from bench to prevention

机译:会议报告:ISN在内皮生物学和肾脏疾病肾脏病学领域的前沿:从替补到预防

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摘要

This ISN-sponsored Forefront in Nephrology meeting, which has brought together 120 scientists from 21 countries, has been concerned with various aspects of endothelial function and dysfunction and their contribution to progression of chronic kidney disease and/or its cardiovascular complications. The following themes were discussed in great depth: (1) phenotypical changes in the vascular endothelium – permeability, senescence, and apoptosis; (2) regulation of endothelial nitric oxide (NO) synthase function – caveolar and shear stress mechanisms, epigenetic regulation, S-nitrosylation, and Rho-kinase regulation; (3) oxidative stress and hypoxia-induced changes; (4) organellar dysfunction – lysosomes, mitochondria, and endoplasmic reticulum; (5) NO-independent mechanisms of vasomotion – epoxides, heme oxygenase-1 and carbon monoxide, thromboxane, tumor necrosis factor-alpha, and uric acid; (6) endothelial crosstalk with podocytes, monocytes, smooth muscle cells, and platelets; (7) candidate clinical biomarkers of endothelial dysfunction – functional testing of macro- and micro-vascular functions, surrogate markers, circulating detached endothelial cells, and endothelial precursor cells; and culminated in Round Table discussion on the diagnosis of endothelial dysfunction and its treatment options. In conclusion, this meeting has focused on several key problems of endothelial cell pathobiology relevant to chronic kidney disease.
机译:这次由ISN赞助的前沿肾脏病会议汇集了来自21个国家/地区的120位科学家,他们关注内皮功能和功能障碍的各个方面,以及它们对慢性肾脏疾病和/或其心血管并发症的进展的贡献。对以下主题进行了深入讨论:(1)血管内皮的表型变化–通透性,衰老和凋亡; (2)调节内皮一氧化氮(NO)合酶的功能–肾小球和切应力机制,表观遗传调控,S-亚硝基化和Rho激酶调控; (3)氧化应激和缺氧引起的变化; (4)细胞器功能障碍–溶酶体,线粒体和内质网; (5)不依赖于NO的血管运动机制-环氧化物,血红素加氧酶-1和一氧化碳,血栓烷,肿瘤坏死因子-α和尿酸; (6)与足细胞,单核细胞,平滑肌细胞和血小板的内皮串扰; (7)内皮功能障碍的候选临床生物标志物–大血管和微血管功能的功能测试,替代标志物,循环分离的内皮细胞和内皮前体细胞;最后在圆桌会议上讨论了内皮功能障碍的诊断及其治疗选择。总之,本次会议的重点是与慢性肾脏疾病有关的内皮细胞病理生物学的几个关键问题。

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