小胶质细胞膜伪装的纳米粒用于缺血性脑卒中的治疗

目的:制备一款由小胶质细胞膜(microglia cell membrane,MiCM)伪装和装载相变材料全氟己烷(perfluorohexane,PFH)的多功能脂质体(liposome,Lipid)纳米粒(MiCM@PFH@Lipid),并研究其基本性质,检测特异性靶向卒中后的损伤部位和实现栓塞部位血管再通的能力。方法:采用旋蒸法制备脂质体球载体,通过超声融合法将PFH和MiCM融合至脂质体形成MiCM@PFH@Lipid,透射电镜(transmission electron microscope,TEM)观察纳米粒的形样貌,马尔文粒径分析仪检测纳米粒第1天的粒径分布,和其在第1、3、5、7 d的电位分布,检测其稳定性。Western blot和考马斯亮蓝染色检测MiCM的包被情况,通过2,3,5-三苯基氯化四氮唑(2,3,5-triphenyltetrazolium chloride,TTC)、动物行为学测试检测小鼠脑功能状态。结果:表征结果显示,MiCM@PFH@Lipid呈球形,粒径为(234.800±3.143)nm,平均电位为(-33.433±1.550)mV,具有良好的分散性,在7 d内具有较好的稳定性,MiCM成功包被在纳米粒上。小鼠离体荧光结果显示,纳米粒可以快速地在损伤部位蓄积,并且与非靶向组比较差异有统计学意义(P<0.05)。动物行为学实验和脑TTC染色结果显示,MiCM@PFH@Lipid纳米粒可以实现血管再通,恢复部分神经功能(P<0.05)。病理学检查显示,纳米粒治疗后没有对重要脏器造成明显损伤,而血常规检测与正常对照组并未见明显异常(P<0.05)。结论:本实验成功制备了多功能纳米粒MiCM@PFH@Lipid,其可以靶向至缺血性卒中后脑损伤区域并破坏血栓,用于缺血性卒中疾病的治疗。

Role of microglial polarization in age-related macular degeneration

Microglia,originating from primitive macrophages in the yolk sac,serves as both immune system defenders and regulators of homeostasis.These cells exhibit two primary polarization states:conventionally activated(M1)and alternatively activated(M2).The polarization of microglia plays a crucial role in influencing inflammatory disorders,metabolic imbalances,and neural degeneration.This process is implicated in various aspects of ocular diseases,especially age-related macular degeneration(AMD),including inflammation,oxidative stress and pathological angiogenesis.The distinct functional phenotypes of microglia impact disease progression and prognosis.Thus,regulating the polarization or functional phenotype of microglia at different stages of AMD holds promise for personalized therapeutic approaches.This comprehensive review outlines the involvement of microglia polarization in both physiological and pathological conditions,emphasizing its relevance in AMD.The discussion underscores the potential of polarization as a foundation for personalized treatment strategies for AMD.