硒
冲程(发动机)
医学
神经科学
纳米点
药理学
化学
心理学
纳米技术
材料科学
工程类
机械工程
有机化学
作者
Qian Zhang,Xiaoyu Wang,Xuegang Niu,Haojie Wang,Yi Wu,Chunwang Li,Huimin Wang,Lin Shen,D. Y. Wang,Fuxin Lin,Pei‐Sen Yao,Yuanxiang Lin,Dezhi Kang,Fei Gao
标识
DOI:10.1186/s12951-024-02847-0
摘要
Intracerebral hemorrhage is a lethal cerebrovascular disease, and the inevitable secondary brain injury (SBI) is responsible for serious disability and death. Perfect therapeutic goal is to minimize SBI and restore neurobehavioral functions. Recently, neuroprotection is highlighted to reduce SBI, but it still faces "Neuronal survival but impaired functions" dilemma. Herein, this work further proposes a novel combinational therapeutic strategy of neuroprotection and neurogenesis toward this goal. However, appropriate therapeutic agents are rarely reported, and their discovery and development are urgently needed. Selenium participates in various physiological/pathological processes, which is hypothesized as a potential targeting molecule. To explore this effect, this work formulates an ultra-small selenium nanodot with a seleno-amino acid derived carbon dot domain and a hydrophilic PEG layer, surprisingly finding that it increases various selenoproteins levels at perihematomal region, to not only exert multiple neuroprotective roles at acute phase but promote neurogenesis and inhibit glial scar formation at recovery phase. At a safe dose, this combinational strategy effectively prevents SBI and recovers neurobehavioral functions to a normal level. Furthermore, its molecular mechanisms are revealed to broaden application scopes in other complex diseases.
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