HIV 诱导的肾细胞损伤:活性氧诱导的下调维生素 D 受体的作用。
HIV-induced kidney cell injury: role of ROS-induced downregulated vitamin D receptor.
机构信息
Immunology Center, Feinstein Institute for Medical Research, Hofstra North Shore LIJ Medical School, Great Neck, New York, USA.
出版信息
Am J Physiol Renal Physiol. 2012 Aug 15;303(4):F503-14. doi: 10.1152/ajprenal.00170.2012. Epub 2012 May 30.
Reactive oxygen species (ROS) have been demonstrated to contribute to HIV-induced tubular cell injury. We hypothesized that HIV-induced ROS generation may be causing tubular cell injury through downregulation of vitamin D receptor (VDR) and associated downstream effects. In the present study, HIV not only downregulated tubular cell VDR expression but also inflicted DNA injury. On the other hand, EB-1089, a VDR agonist (VD), inhibited both downregulation of VDR and tubular cell DNA injury in the HIV milieu. H(2)O(2) (an O(-) donor) directly downregulated tubular cell VDR, whereas catalase, a free radical scavenger, inhibited HIV-induced downregulation of tubular cell VDR expression. HIV also stimulated the tubular cell renin-angiotensin system (RAS) through downregulation of VDR. Because losartan (an ANG II blolcker) partially inhibited HIV-induced tubular cell ROS generation while ANG II directly stimulated tubular cell ROS generation, it appears that HIV-induced ROS production was partly contributed by the RAS activation. VD not only inhibited HIV-induced RAS activation but also attenuated tubular cell ROS generation. Tubular cells displayed double jeopardy in the HIV milieu induction of double-strand breaks and attenuated DNA repair; additionally, in the HIV milieu, tubular cells exhibited enhanced expression of phospho-p53 and associated downstream signaling. A VDR agonist and an ANG II blocker not only preserved expression of tubular cell DNA repair proteins but also inhibited induction of double-strand breaks. In in vivo studies, renal cortical sections of Tg26 mice displayed attenuated expression of VDR both in podocytes and tubular cells. In addition, renal cortical sections of Tg26 mice displayed enhanced oxidative stress-induced kidney cell DNA damage. These findings indicated that HIV-induced tubular cell downregulation of VDR contributed to the RAS activation and associated tubular cell DNA damage. However, both VD and RAS blockade provided protection against these effects of HIV.
活性氧(ROS)已被证明有助于 HIV 诱导的管状细胞损伤。我们假设 HIV 诱导的 ROS 生成可能通过下调维生素 D 受体(VDR)及其相关的下游效应导致管状细胞损伤。在本研究中,HIV 不仅下调了肾小管细胞 VDR 的表达,还造成了 DNA 损伤。另一方面,EB-1089,一种 VDR 激动剂(VD),抑制了 HIV 环境中 VDR 的下调和肾小管细胞 DNA 损伤。H2O2(O-的供体)直接下调肾小管细胞 VDR,而自由基清除剂过氧化氢酶抑制 HIV 诱导的肾小管细胞 VDR 表达下调。HIV 还通过下调 VDR 刺激肾小管细胞肾素-血管紧张素系统(RAS)。由于氯沙坦(一种 ANG II 阻滞剂)部分抑制了 HIV 诱导的肾小管细胞 ROS 生成,而 ANG II 直接刺激肾小管细胞 ROS 生成,因此 HIV 诱导的 ROS 生成部分归因于 RAS 的激活。VD 不仅抑制了 HIV 诱导的 RAS 激活,还减弱了肾小管细胞的 ROS 生成。在 HIV 环境中,肾小管细胞同时面临着双链断裂的诱导和减弱的 DNA 修复的双重危险;此外,在 HIV 环境中,肾小管细胞表现出磷酸化 p53 的增强表达及其相关的下游信号转导。VDR 激动剂和 ANG II 阻滞剂不仅保留了肾小管细胞 DNA 修复蛋白的表达,而且抑制了双链断裂的诱导。在体内研究中,Tg26 小鼠的肾皮质切片显示,足细胞和肾小管细胞中 VDR 的表达均减弱。此外,Tg26 小鼠的肾皮质切片显示,氧化应激诱导的肾细胞 DNA 损伤增强。这些发现表明,HIV 诱导的肾小管细胞下调 VDR 导致了 RAS 的激活及其相关的肾小管细胞 DNA 损伤。然而,VD 和 RAS 阻断都提供了对 HIV 这些影响的保护。
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