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血脑屏障是脑全缺血后类前列腺素迅速且显著增加的主要部位。

Blood-Brain Barrier Is the Major Site for a Rapid and Dramatic Prostanoid Increase upon Brain Global Ischemia.

作者信息

Seeger Drew R, Golovko Svetlana A, Golovko Mikhail Y

机构信息

Department of Biomedical Sciences, School of Medicine and Health Sciences, University of North Dakota, 1301 N. Columbia Rd., Grand Forks, ND, 58202-9037, USA.

出版信息

Lipids. 2020 Jan;55(1):79-85. doi: 10.1002/lipd.12205. Epub 2019 Dec 8.

Abstract

We and others have demonstrated a rapid and dramatic increase in brain prostanoids upon decapitation-induced brain global ischemia and injury. However, the mechanism for this induction, including the cell types involved, are unknown. In the present study, we have validated and applied a pharmacological approach to inhibit prostanoid synthesis in the blood-brain barrier including endothelial cells. Our results indicate that a nonspecific cyclooxygenase (COX) inhibitor, ketorolac, does not pass the blood-brain barrier and does not enter red blood cells but penetrates endothelial cells. Ketorolac treatment did not affect basal prostanoid levels but completely prevented prostanoid induction upon global ischemia. These data indicate that basal prostanoids are synthesized in brain parenchyma cells, while inducible prostanoids are synthesized in the blood-brain barrier, most likely in endothelial cells. However, future studies with cell and COX isoform-specific gene ablation are needed to further validate this conclusion. These findings identify endothelial cells as a possible target for the development of pharmacological approaches to selectively attenuate inducible prostanoid pools without affecting basal levels under brain ischemia, trauma, surgery, and other related conditions.

摘要

我们及其他研究人员已证实,断头诱导的全脑缺血和损伤会使脑内前列腺素迅速且显著增加。然而,这种诱导的机制,包括涉及的细胞类型,尚不清楚。在本研究中,我们验证并应用了一种药理学方法来抑制血脑屏障(包括内皮细胞)中的前列腺素合成。我们的结果表明,非特异性环氧化酶(COX)抑制剂酮咯酸不能通过血脑屏障,也不会进入红细胞,但能穿透内皮细胞。酮咯酸治疗不影响基础前列腺素水平,但能完全阻止全脑缺血时前列腺素的诱导。这些数据表明,基础前列腺素在脑实质细胞中合成,而诱导性前列腺素在血脑屏障中合成,最有可能是在内皮细胞中。然而,需要进一步开展细胞和COX同工型特异性基因敲除研究来进一步验证这一结论。这些发现确定内皮细胞是开发药理学方法的一个可能靶点,该方法可在脑缺血、创伤、手术及其他相关情况下选择性地减少诱导性前列腺素池,而不影响基础水平。

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