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人组织激肽释放酶治疗急性缺血性脑卒中。

Human tissue kallikrein in the treatment of acute ischemic stroke.

作者信息

Alexander-Curtis Michelle, Pauls Rick, Chao Julie, Volpi John J, Bath Philip M, Verdoorn Todd A

机构信息

DiaMedica Therapeutics, 2 Carlson Parkway, Minneapolis, MN 55447, USA.

DiaMedica Therapeutics, Minneapolis, MN, USA.

出版信息

Ther Adv Neurol Disord. 2019 Jan 20;12:1756286418821918. doi: 10.1177/1756286418821918. eCollection 2019.

Abstract

Acute ischemic stroke (AIS) remains a major cause of death and disability throughout the world. The most severe form of stroke results from large vessel occlusion of the major branches of the Circle of Willis. The treatment strategies currently available in western countries for large vessel occlusion involve rapid restoration of blood flow through removal of the offending blood clot using mechanical or pharmacological means (e.g. tissue plasma activator; tPA). This review assesses prospects for a novel pharmacological approach to enhance the availability of the natural enzyme tissue kallikrein (KLK1), an important regulator of local blood flow. KLK1 is responsible for the generation of kinins (bradykinin and kallidin), which promote local vasodilation and long-term vascularization. Moreover, KLK1 has been used clinically as a direct treatment for multiple diseases associated with impaired local blood flow including AIS. A form of human KLK1 isolated from human urine is approved in the People's Republic of China for subacute treatment of AIS. Here we review the rationale for using KLK1 as an additional pharmacological treatment for AIS by providing the biochemical mechanism as well as the human clinical data that support this approach.

摘要

急性缺血性卒中(AIS)仍是全球范围内死亡和残疾的主要原因。最严重的卒中形式是由 Willis 环主要分支的大血管闭塞引起的。西方国家目前针对大血管闭塞的治疗策略包括通过机械或药物手段(如组织型纤溶酶原激活剂;tPA)清除致病血凝块来迅速恢复血流。本综述评估了一种新型药理学方法的前景,该方法旨在提高天然酶组织激肽释放酶(KLK1)的可用性,KLK1 是局部血流的重要调节因子。KLK1 负责激肽(缓激肽和胰激肽)的生成,激肽可促进局部血管舒张和长期血管生成。此外,KLK1 已在临床上用作多种与局部血流受损相关疾病(包括 AIS)的直接治疗药物。从人尿中分离出的一种人 KLK1 在中国被批准用于 AIS 的亚急性治疗。在此,我们通过提供支持该方法的生化机制以及人类临床数据,来综述将 KLK1 用作 AIS 额外药理学治疗方法的理论依据。

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