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首页> 外文期刊>The Journal of Comparative Neurology >Alterations in the Subcellular Distribution of NADPH Oxidase p47(phox) in Hypothalamic Paraventricular Neurons Following Slow-Pressor Angiotensin II Hypertension in Female Mice With Accelerated Ovarian Failure
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Alterations in the Subcellular Distribution of NADPH Oxidase p47(phox) in Hypothalamic Paraventricular Neurons Following Slow-Pressor Angiotensin II Hypertension in Female Mice With Accelerated Ovarian Failure

机译:在加速卵巢衰竭的雌性小鼠慢压血管紧张素II高血压后下丘脑肺腺疽(PHOX)亚细胞氧化酶P47(PHOX)的改变

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摘要

At younger ages, women have a lower risk for hypertension than men, but this sexual dimorphism declines with the onset of menopause. These differences are paralleled in rodents following "slow-pressor" angiotensin II (AngII) administration: young male and aged female mice, but not young females, develop hypertension. There is also an established sexual dimorphism both in the cardiovascular response to the neurohypophyseal hormone arginine vasopressin (AVP) and in the expression of oxidative stress. We examined the relationship between AngII-mediated hypertension and the cellular distribution of the superoxide generating NADPH oxidase (NOX) in AVP-expressing hypothalamic paraventricular nucleus (PVN) neurons in "menopausal" female mice. Dual-labeling immunoelectron microscopy was used to determine whether the subcellular distribution of the organizer/adapter NOX p47(phox) subunit is altered in PVN dendrites following AngII administered (14 days) during the "postmenopausal" stage of accelerated ovarian failure (AOF) in young female mice treated with 4-vinylcyclohexene diepoxide. Slow-pressor AngII elevated blood pressure in AOF females and induced a significant increase in near plasmalemmal p47(phox) and a decrease in cytoplasmic p47(phox) in PVN AVP dendrites. These changes are the opposite of those observed in AngII-induced hypertensive male mice (Coleman et al. [2013] J. Neurosci. 33:4308-4316) and may be ascribed in part to baseline differences between young females and males in the near plasmalemmal p47(phox) on AVP dendrites seen in the present study. These findings highlight fundamental differences in the neural substrates of oxidative stress in the PVN associated with AngII hypertension in postmenopausal females compared with males. (C) 2015 Wiley Periodicals, Inc.
机译:在较年轻的年龄,女性的风险低于男性,但这种性别二态性随更年期的发病而下降。这些差异在“慢压”血管紧张素II(Angii)施用之后在啮齿动物中并联:年轻男性和老年女性小鼠,但非女性,雌性幼年,发展高血压。在心血管反应中也存在既定的性二态,对神经骨骺激素精氨酸加压素(AVP)和氧化应激的表达。我们研究了Angii介导的高血压与超氧化物在“更年期”女小鼠中的丘脑中核(PVN)神经元中的超氧化物产生NADPH氧化酶(NOx)之间的关系。使用双标记免疫电解显微镜检查组织者/适配器NOx P47(PHOX)亚基的亚细胞分布是否在Angii(14天)在加速卵巢衰竭(AOF)中的“绝经后”阶段施用(14天)中改变了PVN树枝状用4-乙烯基环己烯用枯牛盐治疗的幼小母小鼠。缓慢压力机Angii在AOF女性中升高了血压,并诱导PVN AVP树突中近极性肿瘤P47(PHOX)附近的近似增加的细胞质P47(PHOX)减少。这些变化与在血管诱导的高血压雄性小鼠中观察到的变化相反(Coleman等人[2013] J. neurosci。33:4308-4316),并且可以部分地归因于近乎幼年的年轻女性和男性之间的基线差异在本研究中观察到的AVP树枝状体P47(PHOX)。与男性相比,这些发现突出了与血管后期血管的PVN中氧化应激的神经底物的基本差异亮起。 (c)2015 Wiley期刊,Inc。

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