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Brain arachidonic acid uptake and turnover: implications for signaling and bipolar disorder.

机译:脑花生四烯酸的摄取和更新:对信号传导和双相情感障碍的影响。

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PURPOSE OF REVIEW: Arachidonic acid was first detected in the brain in 1922. Although earlier work examined the role of arachidonic acid in growth and development, more recent advancements have elucidated roles for arachidonic acid in brain health and disease. RECENT FINDINGS: In this review, we summarize evidence demonstrating that unesterified arachidonic acid in the plasma pool, which is supplied in part from adipose, is readily taken up and incorporated into brain phospholipids. By labeling plasma unesterified arachidonic acid, it is possible to trace the subsequent release of arachidonic acid from brain phospholipids upon neuroreceptor-mediated release by phospholipase A2 in response to drugs and neuroinflammation in rodents. With the synthesis of 11C labeled fatty acids, brain arachidonic acid signaling can now be measured in humans with position emission tomography. Arachidonic acid signals are known to regulate important biological functions, including neuroinflammation and excitotoxicity, and we focus on how the brain arachidonic acid cascade is a common target of drugs used to treat bipolar disorder (e.g. lithium, carbamazepine and valproate). SUMMARY: A better understanding of the regulation of arachidonic acid uptake into the brain and the brain arachidonic acid cascade could lead to new imaging techniques and the identification of novel therapeutic targets in excitotoxicity, neuroinflammation and bipolar disorder.
机译:审查目的:花生四烯酸于1922年首次在大脑中被发现。尽管较早的研究检查了花生四烯酸在生长和发育中的作用,但最近的进展阐明了花生四烯酸在脑健康和疾病中的作用。最近的发现:在这篇综述中,我们总结了证据,证明血浆中未酯化的花生四烯酸很容易吸收并掺入脑磷脂,血浆中的未酯化花生四烯酸部分由脂肪提供。通过标记血浆未酯化的花生四烯酸,有可能追踪随后花生四烯酸从脑磷脂中释放出来,这是由于磷脂酶A2响应药物和啮齿类动物神经炎症而由神经受体介导的释放。通过合成11C标记的脂肪酸,现在可以使用位置发射断层扫描技术在人体内测量脑花生四烯酸信号。花生四烯酸信号可调节重要的生物学功能,包括神经炎症和兴奋性毒性,我们将重点放在大脑花生四烯酸级联是如何用于治疗双相情感障碍的药物(例如锂,卡马西平和丙戊酸盐)的常见靶标上。摘要:更好地理解花生四烯酸摄取到大脑和大脑花生四烯酸级联的调节可能会导致新的成像技术和兴奋性毒性,神经炎症和躁郁症的新型治疗目标的确定。

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