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Accessing neuroinflammation sites: Monocyteeutrophil-mediated drug delivery for cerebral ischemia

机译:进入神经炎症部位:单核细胞/中性粒细胞介导的药物输送,用于脑缺血

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Cerebral ischemia (CI) results from inadequate blood flow to the brain. The difficulty of delivering therapeutic molecules to lesions resulting from CI hinders the effective treatment of this disease. The inflammatory response following CI offers a unique opportunity for drug delivery to the ischemic brain and targeted cells because of the recruitment of leukocytes to the stroke core and penumbra. In the present study, neutrophils and monocytes were explored as cell carriers after selectively carrying cRGD liposomes, which effectively transmigrated the blood-brain barrier, infiltrated the cerebral parenchyma, and delivered therapeutic molecules to the injured sites and target cells. Our results showed the successful comigration of liposomes with neutrophils/monocytes and that both monocytes and neutrophils were important for successful delivery. Enhanced protection against ischemic injury was achieved in the CI/reperfusion model. The strategy presented here shows potential in the treatment of CI and other diseases related to inflammation.
机译:脑缺血(CI)是由于流向大脑的血液不足引起的。将治疗分子递送至由CI引起的损伤的困难阻碍了对该疾病的有效治疗。由于白细胞募集到中风核心和半影,CI后的炎症反应为将药物输送到缺血性脑和靶向细胞提供了独特的机会。在本研究中,嗜中性粒细胞和单核细胞在选择性地携带cRGD脂质体后被探索为细胞载体,该脂质体有效地转移了血脑屏障,渗透到脑实质中,并将治疗性分子递送至受伤部位和靶细胞。我们的结果表明脂质体与嗜中性粒细胞/单核细胞的成功迁移,并且单核细胞和嗜中性粒细胞对于成功分娩都很重要。在CI /再灌注模型中,增强了针对缺血性损伤的保护。本文介绍的策略显示了在CI和其他与炎症有关的疾病中的治疗潜力。

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