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Integrins and heparan sulfate proteoglycans on hepatic stellate cells (HSC) are novel receptors for HSC-derived exosomes

机译:肝星状细胞(HSC)上的整合素和硫酸乙酰肝素蛋白聚糖是HSC衍生外泌体的新型受体

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摘要

Exosomes mediate intercellular microRNA delivery between hepatic stellate cells (HSC), the principal fibrosis-producing cells in the liver. The purpose of this study was to identify receptors on HSC for HSC-derived exosomes, which bind to HSC rather than to hepatocytes. Our findings indicate that exosome binding to HSC is blocked by treating HSC with RGD, EDTA, integrin v or 1 siRNAs, integrin v3 or 51 neutralizing antibodies, heparin, or sodium chlorate. Furthermore, exosome cargo delivery and exosome-regulated functions in HSC, including expression of fibrosis- or activation-associated genes and/or miR-214 target gene regulation, are dependent on cellular integrin v3, integrin 51, or heparan sulfate proteolgycans (HSPG). Thus, integrins and HSPG mediate the binding of HSC-derived exosomes to HSC as well as the delivery and intracellular action of the exosomal payload.
机译:外泌体介导肝星状细胞(HSC)(肝脏中主要的纤维化产生细胞)之间的细胞间微小RNA传递。这项研究的目的是鉴定HSC衍生的HSC的外泌体受体,该受体与HSC而非肝细胞结合。我们的发现表明,通过用RGD,EDTA,整联蛋白v或1个siRNA,整联蛋白v3或51种中和抗体,肝素或氯酸钠处理HSC,可以阻止外来体与HSC的结合。此外,HSC中的外泌体货物递送和外泌体调节的功能(包括纤维化或激活相关基因的表达和/或miR-214靶基因的调节)取决于细胞整联蛋白v3,整联蛋白51或硫酸乙酰肝素蛋白聚糖(HSPG) 。因此,整联蛋白和HSPG介导HSC衍生的外来体与HSC的结合以及外体有效载荷的递送和细胞内作用。

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