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Monitoring of lipid storage in Caenorhabditis elegans using coherent anti-Stokes Raman scattering (CARS) microscopy

机译:使用相干抗斯托克斯拉曼散射(CARS)显微镜监测秀丽隐杆线虫的脂质存储

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Better understanding of the fundamental mechanisms behind metabolic diseases requires methods to monitor lipid stores on single-cell level in vivo. We have used Caenorhabditis elegans as a model organism to demonstrate the limitations of fluorescence microscopy for imaging of lipids compared with coherent anti-Stokes Raman scattering (CARS) microscopy, the latter allowing chemically specific and label-free imaging in living organisms. CARS microscopy was used to quantitatively monitor the impact of genetic variations in metabolic pathways on lipid storage in 60 specimens of C. elegans. We found that the feeding-defective mutant pha-3 contained a lipid volume fraction one-third of that found in control worms. In contrast, mutants (daf-2, daf-4 dauer) with deficiencies in the insulin and transforming growth factors (IGF and TGF-β) signaling pathways had lipid volume fractions that were 1.4 and 2 times larger than controls, respectively. This was observed as an accumulation of small-sized lipid droplets in the hypodermal cells, hosting as much as 40% of the total lipid volume in contrast to the 9% for the wild-type larvae. Spectral CARS microscopy measurements indicated that this is accompanied by a shift in the ordering of the lipids from gel to liquid phase. We conclude that the degree of hypodermal lipid storage and the lipid phase can be used as a marker of lipid metabolism shift. This study shows that CARS microscopy has the potential to become a sensitive and important tool for studies of lipid storage mechanisms, improving our understanding of phenomena underlying metabolic disorders.
机译:更好地了解代谢性疾病背后的基本机制,需要在体内监测单细胞水平脂质存储的方法。我们已经使用秀丽隐杆线虫作为模型生物,与相干抗斯托克斯拉曼散射(CARS)显微镜相比,证明了荧光显微镜在脂质成像方面的局限性,后者可以在活生物体中进行化学特异性和无标记成像。 CARS显微镜用于定量监测代谢途径中遗传变异对60条秀丽隐杆线虫脂质存储的影响。我们发现,具有进食缺陷的突变体pha-3的脂质体积分数为对照蠕虫中的三分之一。相比之下,胰岛素和转化生长因子(IGF和TGF-β)信号通路缺乏的突变体(daf-2,daf-4 dauer)的脂质体积分数分别是对照的1.4和2倍。观察到这是皮下细胞中小脂质滴的堆积,占总脂质体积的40%,而野生型幼虫为9%。光谱CARS显微镜测量表明,这伴随着脂质从凝胶到液相的顺序改变。我们得出的结论是,皮下脂质存储的程度和脂质相可以用作脂质代谢变化的标志。这项研究表明,CARS显微镜有可能成为研究脂质存储机制的敏感而重要的工具,从而加深了我们对代谢异常现象的理解。

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