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TRPM4阻断抗体可保护延迟性中风再灌注中的脑血管。

TRPM4 Blocking Antibody Protects Cerebral Vasculature in Delayed Stroke Reperfusion.

作者信息

Chen Bo, Wei Shunhui, Low See Wee, Poore Charlene Priscilla, Lee Andy Thiam-Huat, Nilius Bernd, Liao Ping

机构信息

Calcium Signalling Laboratory, Department of Research, National Neuroscience Institute, Singapore 308433, Singapore.

Health and Social Sciences, Singapore Institute of Technology, Singapore 138683, Singapore.

出版信息

Biomedicines. 2023 May 19;11(5):1480. doi: 10.3390/biomedicines11051480.

Abstract

Reperfusion therapy for acute ischemic stroke aims to restore the blood flow of occluded blood vessels. However, successful recanalization is often associated with disruption of the blood-brain barrier, leading to reperfusion injury. Delayed recanalization increases the risk of severe reperfusion injury, including severe cerebral edema and hemorrhagic transformation. The TRPM4-blocking antibody M4P has been shown to alleviate reperfusion injury and improve functional outcomes in animal models of early stroke reperfusion. In this study, we examined the role of M4P in a clinically relevant rat model of delayed stroke reperfusion in which the left middle cerebral artery was occluded for 7 h. To mimic the clinical scenario, M4P or control IgG was administered 1 h before recanalization. Immunostaining showed that M4P treatment improved vascular morphology after stroke. Evans blue extravasation demonstrated attenuated vascular leakage following M4P treatment. With better vascular integrity, cerebral perfusion was improved, leading to a reduction of infarct volume and animal mortality rate. Functional outcome was evaluated by the Rotarod test. As more animals with severe injuries died during the test in the control IgG group, we observed no difference in functional outcomes in the surviving animals. In conclusion, we identified the potential of TRPM4 blocking antibody M4P to ameliorate vascular injury during delayed stroke reperfusion. If combined with reperfusion therapy, M4P has the potential to improve current stroke management.

摘要

急性缺血性中风的再灌注治疗旨在恢复闭塞血管的血流。然而,成功再通往往伴随着血脑屏障的破坏,导致再灌注损伤。延迟再通会增加严重再灌注损伤的风险,包括严重脑水肿和出血性转化。在早期中风再灌注动物模型中,TRPM4阻断抗体M4P已被证明可减轻再灌注损伤并改善功能结局。在本研究中,我们在一个临床相关的延迟性中风再灌注大鼠模型中研究了M4P的作用,该模型中左大脑中动脉闭塞7小时。为模拟临床情况,在再通前1小时给予M4P或对照IgG。免疫染色显示,M4P治疗改善了中风后的血管形态。伊文思蓝外渗表明M4P治疗后血管渗漏减轻。随着血管完整性改善,脑灌注得到改善,导致梗死体积和动物死亡率降低。通过转棒试验评估功能结局。由于对照IgG组中更多重伤动物在试验期间死亡,我们在存活动物中未观察到功能结局的差异。总之,我们确定了TRPM4阻断抗体M4P在延迟性中风再灌注期间改善血管损伤的潜力。如果与再灌注治疗相结合,M4P有可能改善当前的中风治疗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3af5/10216476/35a62ab9f67f/biomedicines-11-01480-g001.jpg

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