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Early ischemic blood brain barrier damage: A potential indicator for hemorrhagic transformation following tissue plasminogen activator (tpa) thrombolysis?

机译:早期缺血性血脑屏障损害:组织纤溶酶原激活物(tpa)溶栓后出血性转化的潜在指标吗?

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摘要

Tissue plasminogen activator (tPA) thrombolysis, remains to be the only United States Food and Drug Administration (FDA) approved treatment for acute ischemia stroke. However, the use of tPA has been profoundly constrained due to its narrow therapeutic time window and the increased risk of potentially deadly hemorrhagic complications. TPA-Associated hemorrhagic transformation (HT) often occurs as a result of catastrophic failure of the blood brain barrier (BBB), wherein the affected cerebral capillaries can no longer hold blood constituents. Due to its direct contribution to edema and HT, reperfusion-Associated BBB damage has been extensively studied, while BBB damage that occurs within the thrombolytic time window is largely neglected. Of note, ischemia-induced BBB damage in the early stroke stages is increasingly appreciated to negatively affect the safety and efficacy profiles of thrombolytic therapy for ischemic stroke. In this review, we discussed the recent findings of spatio-temporal evolution of BBB injury in the early stages of cerebral ischemia and its association with intracerebral hemorrhage following tPA thrombolysis. The increased understanding of early ischemic BBB damage and its close link to tPA-Associated HT is of particular importance for developing new preventive and therapeutic strategies to reduce the hemorrhagic complications in stroke thrombolysis.
机译:组织纤溶酶原激活剂(tPA)溶栓仍是唯一获得美国食品和药物管理局(FDA)批准的急性缺血性中风的治疗方法。然而,由于tPA的治疗时间范围狭窄以及潜在致命的出血并发症的风险增加,因此tPA的使用受到了严重的限制。 TPA相关的出血性转化(HT)通常是由于血脑屏障(BBB)的灾难性故障而发生的,其中受影响的脑毛细血管不再能容纳血液成分。由于其对水肿和HT的直接贡献,已经广泛研究了与再灌注相关的BBB损伤,而在血栓溶解时间窗内发生的BBB损伤则被忽略了。值得注意的是,在卒中早期缺血引起的血脑屏障损害日益受到人们的关注,它会对溶栓治疗缺血性卒中的安全性和疗效产生负面影响。在这篇综述中,我们讨论了脑缺血早期BBB损伤时空演变的最新发现及其与tPA溶栓后脑出血的相关性。对于早期缺血性BBB损伤及其与tPA相关性HT的密切联系的进一步了解对于开发新的预防和治疗策略以减少中风血栓溶解中的出血并发症特别重要。

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