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Phosphatidylserine: A Novel Target for Ischemic Stroke Treatment

机译:磷脂酰丝氨酸:缺血性卒中治疗的新靶点

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摘要

Over the past 40 years, research has heavily emphasized stroke treatments that directly target ischemic cascades after stroke onset. Much attention has focused on studying neuroprotective drugs targeting one aspect of the ischemic cascade. However, the single-target therapeutic approach resulted in minimal clinical benefit and poor outcomes in patients. Considering the ischemic cascade is a multifaceted and complex pathophysiological process with many interrelated pathways, the spotlight is now shifting towards the development of neuroprotective drugs that affect multiple aspects of the ischemic cascade. Phosphatidylserine (PS), known as the “eat-me” signal, is a promising candidate. PS is involved in many pathophysiological changes in the central nervous system after stroke onset, including apoptosis, inflammation, coagulation, and neuronal regeneration. Moreover, PS might also exert various roles in different phases after stroke onset. In this review, we describe the synthesis, regulation, and function of PS under physiological conditions. Furthermore, we also summarize the different roles of PS after stroke onset. More importantly, we also discuss several treatment strategies that target PS. We aim to advocate a novel stroke care strategy by targeting PS through a translational perspective.
机译:在过去的 40 年里,研究一直非常强调直接针对中风发作后缺血级联反应的中风治疗。许多注意力都集中在研究针对缺血级联反应的一个方面的神经保护药物上。然而,单靶点治疗方法对患者的临床获益最小,预后较差。考虑到缺血级联反应是一个多方面且复杂的病理生理过程,具有许多相互关联的途径,现在的焦点正在转向影响缺血级联反应多个方面的神经保护药物的开发。磷脂酰丝氨酸 (PS),被称为“吃我”信号,是一个很有前途的候选者。PS 参与中风发作后中枢神经系统的许多病理生理变化,包括细胞凋亡、炎症、凝血和神经元再生。此外,PS 也可能在中风发作后的不同阶段发挥各种作用。在这篇综述中,我们描述了 PS 在生理条件下的合成、调节和功能。此外,我们还总结了 PS 在中风发作后的不同作用。更重要的是,我们还讨论了几种针对 PS 的治疗策略。我们的目标是通过转化视角靶向 PS 来倡导一种新的中风护理策略。

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