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口服避孕药和尼古丁协同作用加剧女性大脑的缺血性损伤。

Oral contraceptives and nicotine synergistically exacerbate cerebral ischemic injury in the female brain.

机构信息

Cerebral Vascular Disease Research Center, Department of Neurology, Leonard M. Miller School of Medicine, University of Miami, Two Story Lab (TSL), Room # 230A, 1420 NW 9th Avenue, Miami, FL, 33101, USA,

出版信息

Transl Stroke Res. 2013 Aug;4(4):402-12. doi: 10.1007/s12975-013-0253-6. Epub 2013 Feb 13.

Abstract

Oral contraceptives (OC) and smoking-derived nicotine (N) are known to synergistically increase the risk and severity of cerebral ischemia in women. Although it has been known for some time that long-term use of OC and nicotine will have an increased risk of peripheral thrombus formation, little is known about how the combination of OC and nicotine increases severity of brain ischemia. Recent laboratory studies simulating the conditions of nicotine exposure produced by cigarette smoking and OC regimen of women in female rats confirms that the severity of ischemic hippocampal damage is far greater in female rats simultaneously exposed to OC than to nicotine alone. These studies also demonstrated that the concurrent exposure of OC and nicotine reduces endogenous 17β-estradiol levels and inhibits estrogen signaling in the brain of female rats. The endogenous 17β-estradiol plays a key role in cerebrovascular protection in women during their pre-menopausal life and loss of circulating estrogen at reproductive senescence increases both the incidence and severity of cerebrovascular diseases. Therefore, OC and nicotine induced severe post-ischemic damage might be a consequence of lack of estrogen signaling in the brain. In the present review we highlight possible mechanisms by which OC and nicotine inhibits estrogen signaling that could be responsible for severe ischemic damage in females.

摘要

口服避孕药 (OC) 和吸烟衍生的尼古丁 (N) 已知会协同增加女性脑缺血的风险和严重程度。尽管长期使用 OC 和尼古丁会增加外周血栓形成的风险已为人所知一段时间,但对于 OC 和尼古丁的组合如何增加脑缺血的严重程度知之甚少。最近的实验室研究模拟了吸烟和女性服用 OC 方案产生的尼古丁暴露条件,证实同时暴露于 OC 的雌性大鼠的缺血性海马损伤严重程度远高于单独暴露于尼古丁的大鼠。这些研究还表明,OC 和尼古丁的同时暴露会降低雌性大鼠大脑中的内源性 17β-雌二醇水平并抑制大脑中的雌激素信号。内源性 17β-雌二醇在女性绝经前的脑血管保护中起着关键作用,生殖衰老时循环雌激素的丧失会增加脑血管疾病的发生率和严重程度。因此,OC 和尼古丁引起的严重缺血后损伤可能是大脑中雌激素信号缺失的结果。在本综述中,我们强调了 OC 和尼古丁抑制雌激素信号的可能机制,这些机制可能是女性严重缺血损伤的原因。

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