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饮食中的胆固醇和载脂蛋白 A-I 在内质网和溶酶体中在活体斑马鱼肠道中运输。

Dietary cholesterol and apolipoprotein A-I are trafficked in endosomes and lysosomes in the live zebrafish intestine.

机构信息

Department of Embryology, Carnegie Institution for Science , Baltimore, Maryland.

Department of Biology, Johns Hopkins University , Baltimore, Maryland.

出版信息

Am J Physiol Gastrointest Liver Physiol. 2019 Mar 1;316(3):G350-G365. doi: 10.1152/ajpgi.00080.2018. Epub 2019 Jan 10.

Abstract

Difficulty in imaging the vertebrate intestine in vivo has hindered our ability to model nutrient and protein trafficking from both the lumenal and basolateral aspects of enterocytes. Our goal was to use live confocal imaging to increase understanding of intestinal trafficking of dietary cholesterol and apolipoprotein A-I (APOA-I), the main structural component of high-density lipoproteins. We developed a novel assay to visualize live dietary cholesterol trafficking in the zebrafish intestine by feeding TopFluor-cholesterol (TF-cholesterol), a fluorescent cholesterol analog, in a lipid-rich, chicken egg yolk feed. Quantitative microscopy of transgenic zebrafish expressing fluorescently tagged protein markers of early, recycling, and late endosomes/lysosomes provided the first evidence, to our knowledge, of cholesterol transport in the intestinal endosomal-lysosomal trafficking system. To study APOA-I dynamics, transgenic zebrafish expressing an APOA-I fluorescent fusion protein (APOA-I-mCherry) from tissue-specific promoters were created. These zebrafish demonstrated that APOA-I-mCherry derived from the intestine accumulated in the liver and vice versa. Additionally, intracellular APOA-I-mCherry localized to endosomes and lysosomes in the intestine and liver. Moreover, live imaging demonstrated that APOA-I-mCherry colocalized with dietary TF-cholesterol in enterocytes, and this colocalization increased with feeding time. This study provides a new set of tools for the study of cellular lipid biology and elucidates a key role for endosomal-lysosomal trafficking of intestinal cholesterol and APOA-I. NEW & NOTEWORTHY A fluorescent cholesterol analog was fed to live, translucent larval zebrafish to visualize intracellular cholesterol and apolipoprotein A-I (APOA-I) trafficking. With this model intestinal endosomal-lysosomal cholesterol trafficking was observed for the first time. A new APOA-I fusion protein (APOA-I-mCherry) expressed from tissue-specific promoters was secreted into the circulation and revealed that liver-derived APOA-I-mCherry accumulates in the intestine and vice versa. Intestinal, intracellular APOA-I-mCherry was observed in endosomes and lysosomes and colocalized with dietary cholesterol.

摘要

在体内对脊椎动物肠道进行成像的困难阻碍了我们从肠细胞的腔侧和基底外侧方面来模拟营养物质和蛋白质转运的能力。我们的目标是使用活细胞共聚焦成像来增加对饮食胆固醇和载脂蛋白 A-I(APOA-I)(高密度脂蛋白的主要结构成分)在肠道中的转运的理解。我们开发了一种新的测定法,通过用富含脂质的鸡卵黄饲料喂养荧光胆固醇类似物 TopFluor-胆固醇(TF-cholesterol),来可视化斑马鱼肠道中饮食胆固醇的转运。对表达早期、回收和晚期内体/溶酶体荧光标记蛋白标记物的转基因斑马鱼的定量显微镜观察,为我们所知,首次提供了胆固醇在肠道内体-溶酶体转运系统中的转运证据。为了研究 APOA-I 的动力学,我们创建了表达组织特异性启动子的 APOA-I 荧光融合蛋白(APOA-I-mCherry)的转基因斑马鱼。这些斑马鱼表明,来自肠道的 APOA-I-mCherry 积累在肝脏中,反之亦然。此外,在肠道和肝脏中,细胞内 APOA-I-mCherry 定位于内体和溶酶体中。此外,活体成像显示,APOA-I-mCherry 与肠细胞中的饮食 TF-cholesterol 共定位,并且这种共定位随进食时间的增加而增加。这项研究为细胞脂质生物学的研究提供了一套新的工具,并阐明了肠道胆固醇和 APOA-I 的内体-溶酶体转运的关键作用。

新的和值得注意的是,给活体、半透明的幼虫斑马鱼喂食荧光胆固醇类似物,以可视化细胞内胆固醇和载脂蛋白 A-I(APOA-I)的转运。通过这种模型,首次观察到肠道内体-溶酶体胆固醇转运。一种从组织特异性启动子表达的新的 APOA-I 融合蛋白(APOA-I-mCherry)被分泌到循环中,并表明肝脏来源的 APOA-I-mCherry 在肠道中积累,反之亦然。在肠细胞内,观察到细胞内 APOA-I-mCherry 存在于内体和溶酶体中,并与饮食胆固醇共定位。

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