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首页> 外文期刊>The journal of sexual medicine >Hypercholesterolemia-induced erectile dysfunction: endothelial nitric oxide synthase (eNOS) uncoupling in the mouse penis by NAD(P)H oxidase.
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Hypercholesterolemia-induced erectile dysfunction: endothelial nitric oxide synthase (eNOS) uncoupling in the mouse penis by NAD(P)H oxidase.

机译:高胆固醇血症引起的勃起功能障碍:小鼠阴茎中的内皮一氧化氮合酶(eNOS)通过NAD(P)H氧化酶解偶联。

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INTRODUCTION: Hypercholesterolemia induces erectile dysfunction (ED) mostly by increasing oxidative stress and impairing endothelial function in the penis, but the mechanisms regulating reactive oxygen species (ROS) production in the penis are not understood. AIMS: We evaluated whether hypercholesterolemia activates nicotinamide adenine dinucleotide phosphate (NAD[P]H) oxidase in the penis, providing an initial source of ROS to induce endothelial nitric oxide synthase (eNOS) uncoupling and endothelial dysfunction resulting in ED. METHODS: Low-density-lipoprotein receptor (LDLR)-null mice were fed Western diet for 4 weeks to induce early-stage hyperlipidemia. Wild type (WT) mice fed regular chow served as controls. Mice received NAD(P)H oxidase inhibitor apocynin (10 mM in drinking water) or vehicle. Erectile function was assessed in response to cavernous nerve electrical stimulation. Markers of endothelial function (phospho [P]-vasodilator-stimulated-protein [VASP]-Ser-239), oxidative stress (4-hydroxy-2-nonenal [HNE]), sources of ROS (eNOS uncoupling and NAD[P]H oxidase subunits p67(phox) , p47(phox) , and gp91(phox) ), P-eNOS-Ser-1177, and eNOS were measured by Western blot in penes. MAIN OUTCOME MEASURES: The main outcome measures are the molecular mechanisms of ROS generation and endothelial dysfunction in hypercholesterolemia-induced ED. RESULTS: Erectile response was significantly (P<0.05) reduced in hypercholesterolemic LDLR-null mice compared with WT mice. Relative to WT mice, hypercholesterolemia increased (P<0.05) protein expressions of NAD(P)H oxidase subunits p67(phox) , p47(phox) and gp91(phox) , eNOS uncoupling, and 4-HNE-modified proteins, and reduced (P<0.05) P-VASP-Ser-239 expression in the penis. Apocynin treatment of LDLR-null mice preserved (P<0.05) maximal intracavernosal pressure, and reversed (P<0.05) the abnormalities in protein expressions of gp67(phox) and gp47(phox) , 4-HNE, P-VASP-Ser-239, and eNOS uncoupling in the penis. Apocynin treatment of WT mice did not affect any of these parameters. Protein expressions of P-eNOS-Ser-1177 and total eNOS were unaffected by hypercholesterolemia. CONCLUSION: Activated NAD(P)H oxidase in the penis is an initial source of oxidative stress resulting in eNOS uncoupling, thus providing a mechanism of eNOS uncoupling and endothelial dysfunction in hypercholesterolemia-induced ED.
机译:简介:高胆固醇血症主要通过增加阴茎的氧化应激和损害内皮功能来诱发勃起功能障碍(ED),但尚不清楚调节阴茎中活性氧(ROS)产生的机制。目的:我们评估了高胆固醇血症是否激活了阴茎中的烟酰胺腺嘌呤二核苷酸磷酸(NAD [P] H)氧化酶,提供了ROS的初始来源,以诱导内皮型一氧化氮合酶(eNOS)解偶联和内皮功能障碍,从而导致ED。方法:将低密度脂蛋白受体(LDLR)无效的小鼠喂食西方饮食4周,以诱导早期高脂血症。用常规食物喂养的野生型(WT)小鼠作为对照。小鼠接受了NAD(P)H氧化酶抑制剂Apocynin(在饮用水中为10 mM)或媒介物。响应于海绵体神经电刺激评估勃起功能。内皮功能的标志物(磷酸化[P]-血管扩张剂刺激的蛋白[VASP] -Ser-239),氧化应激(4-羟基-2-壬烯醛[HNE]),ROS的来源(eNOS解偶联和NAD [P]) H氧化酶亚基p67(phox),p47(phox)和gp91(phox)),P-eNOS-Ser-1177和eNOS通过Western blot在阴茎中进行测量。主要观察指标:主要观察指标是高胆固醇血症诱发的ED中ROS生成和内皮功能异常的分子机制。结果:与WT小鼠相比,高胆固醇血症的LDLR无效小鼠的勃起反应显着降低(P <0.05)。相对于WT小鼠,高胆固醇血症使NAD(P)H氧化酶亚基p67(phox),p47(phox)和gp91(phox),eNOS解偶联和4-HNE修饰的蛋白表达升高(P <0.05),并降低(P <0.05)P-VASP-Ser-239在阴茎中的表达。阿波西林对LDLR无效小鼠的最大腔内降压保持(P <0.05),逆转(P <0.05)gp67(phox)和gp47(phox),4-HNE,P-VASP-Ser-蛋白表达异常239,而eNOS在阴茎中解耦。 WT小鼠的Apocynin治疗不影响任何这些参数。 P-eNOS-Ser-1177和总eNOS的蛋白质表达不受高胆固醇血症的影响。结论:阴茎中活化的NAD(P)H氧化酶是导致eNOS解偶联的氧化应激的初始来源,从而为高胆固醇血症诱发的ED提供了eNOS解偶联和内皮功能障碍的机制。

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