| Literature DB >> 30957932 |
Yifei Lu1,2, Chao Li1, Qinjun Chen1, Peixin Liu1, Qin Guo1, Yu Zhang1, Xinli Chen1, Yujie Zhang1, Wenxi Zhou1, Donghui Liang1, Yiwen Zhang1, Tao Sun1, Weigen Lu2, Chen Jiang1.
Abstract
Reperfusion injury exists as the major obstacle to full recovery of neuron functions after ischemic stroke onset and clinical thrombolytic therapies. Complex cellular cascades including oxidative stress, neuroinflammation, and brain vascular impairment occur within neurovascular units, leading to microthrombus formation and ultimate neuron death. In this work, a multitarget micelle system is developed to simultaneously modulate various cell types involved in these events. Briefly, rapamycin is encapsulated in self-assembled micelles that are consisted of reactive oxygen species (ROS)-responsive and fibrin-binding polymers to achieve micelle retention and controlled drug release within the ischemic lesion. Neuron survival is reinforced by the combination of micelle facilitated ROS elimination and antistress signaling pathway interference under ischemia conditions. In vivo results demonstrate an overall remodeling of neurovascular unit through micelle polarized M2 microglia repair and blood-brain barrier preservation, leading to enhanced neuroprotection and blood perfusion. This strategy gives a proof of concept that neurovascular units can serve as an integrated target for ischemic stroke treatment with nanomedicines.Entities:
Keywords: ischemic stroke; microenvironment modulation; microglia polarization; neurovascular units; no-reflow
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Year: 2019 PMID: 30957932 DOI: 10.1002/adma.201808361
Source DB: PubMed Journal: Adv Mater ISSN: 0935-9648 Impact factor: 30.849