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首页> 外文期刊>ACS nano >A Carbon Nanotube Optical Reporter Maps Endolysosomal Lipid Flux
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A Carbon Nanotube Optical Reporter Maps Endolysosomal Lipid Flux

机译:碳纳米管光学报告器地图底糖血清脂质通量

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摘要

Lipid accumulation within the lumen of endolysosomal vesicles is observed in various pathologies including atherosclerosis, liver disease, neurological disorders, lysosomal storage disorders, and cancer. Current methods cannot measure lipid flux specifically within the lysosomal lumen of live cells. We developed an optical reporter, composed of a photoluminescent carbon nanotube of a single chirality, that responds to lipid accumulation via modulation of the nanotube's optical band gap. The engineered nanomaterial, composed of short, single stranded DNA and a single nanotube chirality, localizes exclusively to the lumen of endolysosomal organelles without adversely affecting cell viability or proliferation or organelle morphology, integrity, or function. The emission wavelength of the reporter can be spatially resolved from within the endolysosomal lumen to generate quantitative maps of lipid content in live cells. Endolysosomal lipid accumulation in cell lines, an example of drug-induced phospholipidosis, was observed for multiple drugs in macrophages, and measurements of patient-derived Niemann Pick type C fibroblasts identified lipid accumulation and phenotypic reversal of this lysosomal storage disease. Single-cell measurements using the reporter discerned subcellular differences in equilibrium lipid content, illuminating significant intracellular heterogeneity among endolysosomal organelles of differentiating bone-marrow derived monocytes. Single-cell kinetics of lipoprotein-derived cholesterol accumulation within macrophages revealed rates that differed among cells by an order of magnitude. This carbon nanotube optical reporter of endolysosomal lipid content in live cells confers additional capabilities for drug development processes and the investigation of lipid-linked diseases.
机译:在包括动脉粥样硬化,肝病,神经病学疾病,溶酶体储存障碍和癌症的各种病理学中观察到底糖体囊泡内腔内的脂质积累。目前的方法不能在活细胞的溶酶体内腔内特异性测量脂质通量。我们开发了一种光学报告器,由单个手性的光致发光碳纳米管组成,其通过调制纳米管光带隙来响应脂质积累。工程化纳米材料,由短,单链DNA和单个纳米管肾手术组成,专门针对内溶血剂细胞器的内腔定位而不存在细胞活力或增殖或细胞器形态,完整性或功能。记者的发射波长可以从底糖瘤内部内部分解,以在活细胞中产生脂质含量的定量图。在巨噬细胞中的多种药物中观察到细胞系中细胞系中的内糖素脂质积聚,药物诱导的磷脂蛋白的实例,并测量患者衍生的Niemann挑选C成纤维细胞鉴定了这种溶酶体储存疾病的脂质积累和表型逆转。单细胞测量使用报道透明血细胞含量的亚细胞差异,在分化骨髓衍生的单核细胞中的底糖瘤细胞器中发出显着的细胞内异质性。巨噬细胞内脂蛋白衍生的胆固醇积聚的单细胞动力学揭示了细胞级不同的速率。这种碳纳米管光学报告者在活细胞中的内溶血素脂质含量赋予药物发育过程的额外能力和脂质关联疾病的调查。

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