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Gadolinium-containing phosphatidylserine liposomes for molecular imaging of atherosclerosis

机译:含d磷脂酰丝氨酸脂质体的动脉粥样硬化分子成像

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摘要

Exteriorized phosphatidylserine (PS) residues in apoptotic cells trigger rapid phagocytosis by macrophage scavenger receptor pathways. Mimicking apoptosis with liposomes containing PS may represent an attractive approach for molecular imaging of atherosclerosis. We investigated the utility of paramagnetic gadolinium liposomes enriched with PS (Gd-PS) in imaging atherosclerotic plaque. Gd-PS-containing Gd-conjugated lipids, fluorescent rhodamine, and PS were prepared and characterized. Cellular uptake in RAW macrophages (fluorescent uptake of rhodamine) was studied on a fluorescence plate reader, while Gd-PS-induced alteration in T1 relaxivity was evaluated using a 1.5 T MRI scanner. RAW cells demonstrate PS-dependent uptake of across a range of concentrations (2, 6, 12, and 20%) in comparison to control liposomes with no PS (0%). In vivo performance of Gd-PS was evaluated in the ApoE−/− mouse model by collection of serial T1 weighted gradient echo MR images using an 11.7 T MRI system and revealed rapid and significant enhancement of the aortic wall that was seen for at least 4 h after injection. Gd-PS-enriched liposomes enhance atherosclerotic plaque and colocalize with macrophages in experimental atherosclerosis.
机译:凋亡细胞中外部化的磷脂酰丝氨酸(PS)残基通过巨噬细胞清除剂受体途径触发快速吞噬作用。用含PS的脂质体模仿细胞凋亡可能代表一种用于动脉粥样硬化分子成像的有吸引力的方法。我们调查了富含PS(Gd-PS)的顺磁性ado脂质体在成像动脉粥样硬化斑块中的效用。制备并表征了含Gd-PS的Gd共轭脂质,荧光若丹明和PS。在荧光板读数器上研究了RAW巨噬细胞的细胞摄取(若丹明的荧光摄取),而使用1.5 T MRI扫描仪评估了Gd-PS诱导的T1弛豫性改变。与没有PS的对照脂质体(0​​%)相比,RAW细胞在一系列浓度范围(2、6、12和20%)表现出PS依赖性摄取。通过使用11.7 T MRI系统收集一系列T1加权梯度回波MR图像,在ApoE -/-小鼠模型中评估了Gd-PS的体内性能,并揭示了主动脉壁的快速而明显的增强注射后至少4小时内观察到。富含Gd-PS的脂质体可增强动脉粥样硬化斑块,并在实验性动脉粥样硬化中与巨噬细胞共定位。

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