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Progesterone exerts neuroprotective effects and improves long-term neurologic outcome after intracerebral hemorrhage in middle-aged mice

机译:黄体酮在中年小鼠脑出血后发挥神经保护作用并改善长期神经系统结局

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摘要

In this study, we examined the effect of progesterone on histopathologic and functional outcomes of intracerebral hemorrhage (ICH) in 10–12-month-old mice. Progesterone or vehicle was administered by intraperitoneal injection 1 hour after collagenase-induced ICH and then by subcutaneous injections at 6, 24, and 48 hours. Oxidative and nitrosative stress were assayed at 12 hours post-ICH. Injury markers were examined on day 1, and lesion was examined on day 3. Neurologic deficits were examined for 28 days. Progesterone posttreatment reduced lesion volume, brain swelling, edema, and cell degeneration and improved long-term neurologic function. These protective effects were associated with reductions in protein carbonyl formation, protein nitrosylation, and MMP-9 activity and attenuated cellular and molecular inflammatory responses. Progesterone also reduced VEGF expression, increased neuronal-specific Na+/K+ ATPase α3 subunit expression, and reduced PKC-dependent Na+/K+ ATPase phosphorylation. Furthermore, progesterone reduced glial scar thickness, myelin loss, brain atrophy, and residual injury volume on day 28 after ICH. With multiple brain targets, progesterone warrants further investigation for its potential use in ICH therapy.
机译:在这项研究中,我们检查了孕酮对10-12个月大小鼠脑出血(ICH)的组织病理学和功能结局的影响。在胶原酶诱导的ICH后1小时腹膜内注射,然后在6、24和48小时皮下注射,给予孕酮或媒介物。在ICH后12小时测定氧化应激和亚硝化应激。在第1天检查损伤标记,在第3天检查病变。在28天内检查神经功能缺损。孕酮后处理可减少病变体积,脑肿胀,水肿和细胞变性,并改善长期神经功能。这些保护作用与蛋白质羰基形成减少,蛋白质亚硝基化和MMP-9活性降低以及细胞和分子炎症反应减弱有关。孕酮还降低VEGF表达,增加神经元特异性Na + / K + ATPaseα3亚基表达,并降低PKC依赖性Na + / K + ATPase磷酸化。此外,在ICH后第28天,孕酮减少了神经胶质瘢痕的厚度,髓磷脂的损失,脑萎缩和残余损伤量。黄体酮具有多个脑靶点,因此有必要进一步研究其在ICH治疗中的潜在用途。

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