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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >A regulatory role of scavenger receptor class B type 1 in endocytosis and lipid droplet formation induced by liposomes containing phosphatidylethanolamine in HEK293T cells
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A regulatory role of scavenger receptor class B type 1 in endocytosis and lipid droplet formation induced by liposomes containing phosphatidylethanolamine in HEK293T cells

机译:清除剂受体B型调节作用1在HEK293T细胞中脂质体诱导的脂质体诱导的内吞作用和脂质液滴形成

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We have recently reported that phosphatidylethanolamine (PE)-containing liposomes are endocytosed and then induce lipid droplets (LDs) in HEK293T cells. In this study, we elucidated a mechanism responsible for endocytosis of PE-containing liposomes and induction of LDs. By using fluorescence-labeled liposomes and flow cytometry, we found that PE-containing liposomes were very efficiently internalized in HEK293T cells. However, Block lipid transporter-1 (BLT-1) only marginally suppressed the uptake of these liposomes, indicating that entire liposomes were mostly taken up in these cells. They were therefore inferred to express abundant PE receptors responsible for endocytosis of PE-containing liposomes. We examined the expression of 52 candidate genes through transcriptomic analyses and eventually narrowed it down to four candidate genes, which were abundantly expressed in HEK293T cells. Among siRNAs targeting these candidates, scavenger receptor class B type 1 (SR-B1) siRNA showed the most profound reduction in PE liposomal uptake. Conversely, the expression of SR-B1 by transfection of an expression plasmid enhanced the uptake of PE-containing liposomes. After the internalization of PE-containing liposomes, they were colocalized with endosomes/lysosomes and SR-B1, which indicates that these liposomes are taken up in HEK293T cells at least partially through the endosomal/lysosomal pathway. A specific anti-SR-B1-antibody blocked the uptake of PE-containing liposomes in HEK293T cells while LD formation in these cells induced by PE-containing liposomes was suppressed by treatment with SR-B1 siRNA. These results demonstrate that SR-B1 functions as a receptor for the endocytosis of PE-containing liposomes and regulates the formation of LDs induced by PE-containing liposomes in HEK293T cells.
机译:我们最近报道了磷脂酰乙醇胺(PE) - 致脂质体是内核细胞的,然后在HEK293T细胞中诱导脂液滴(LDS)。在这项研究中,我们阐明了负责含有体积脂质体的内吞作用的机制和LDS的诱导。通过使用荧光标记的脂质体和流式细胞术,我们发现在HEK293T细胞中非常有效地内化了含有体积的脂质体。然而,嵌段脂质转运蛋白-1(BLT-1)仅略微抑制了这些脂质体的吸收,表明整个脂质体主要溶于这些细胞中。因此,推断它们以表达负责含有脂质体的细胞增多症的丰富的体积受体。我们通过转录组分析检查了52个候选基因的表达,最终将其缩小到四种候选基因,其在HEK293T细胞中大量表达。在靶向这些候选者的SIRNA中,清除剂受体B型(SR-B1)siRNA表现出pE脂质体摄取最深入的降低。相反,通过转染表达质粒的SR-B1的表达增强了含有体积脂质体的摄取。在含有体积脂质体的内化之后,它们用胚乳/溶酶体和SR-B1分成了分致纳米,表明这些脂质体至少部分地通过内体/溶酶体途径溶于HEK293T细胞中。特定的抗SR-B1-抗体阻断了HEK293T细胞中含有体积脂质体的摄取,同时通过用SR-B1 siRNA处理抑制了通过含有体积脂质体诱导的这些细胞中的LD形成。这些结果表明,SR-B1用作含PE脂质体的内吞作用的受体,并调节通过HEK293T细胞中含有体积脂质体诱导的LDS的形成。

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