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MicroRNAs are exported from malignant cells in customized particles

机译:MicroRNA从恶性细胞以定制颗粒形式输出

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MicroRNAs (miRNAs) are released from cells in association with proteins or microvesicles. We previously reported that malignant transformation changes the assortment of released miRNAs by affecting whether a particular miRNA species is released or retained by the cell. How this selectivity occurs is unclear. Here we report that selectively exported miRNAs, whose release is increased in malignant cells, are packaged in structures that are different from those that carry neutrally released miRNAs (n-miRNAs), whose release is not affected by malignancy. By separating breast cancer cell microvesicles, we find that selectively released miRNAs associate with exosomes and nucleosomes. However, n-miRNAs of breast cancer cells associate with unconventional exosomes, which are larger than conventional exosomes and enriched in CD44, a protein relevant to breast cancer metastasis. Based on their large size, we call these vesicles L-exosomes. Contrary to the distribution of miRNAs among different microvesicles of breast cancer cells, normal cells release all measured miRNAs in a single type of vesicle. Our results suggest that malignant transformation alters the pathways through which specific miRNAs are exported from cells. These changes in the particles and their miRNA cargo could be used to detect the presence of malignant cells in the body.
机译:MicroRNA(miRNA)与蛋白质或微泡一起从细胞中释放出来。我们先前曾报道恶性转化通过影响细胞是否释放或保留特定的miRNA种类来改变释放的miRNA的种类。选择性如何发生尚不清楚。在这里,我们报道了选择性输出的在恶性细胞中释放增加的miRNA,其包装结构与携带中性释放的miRNA(n-miRNA)的结构不同,后者的释放不受恶性影响。通过分离乳腺癌细胞微泡,我们发现选择性释放的miRNA与外泌体和核小体相关。然而,乳腺癌细胞的n-miRNA与非常规外泌体相关,非常规外泌体比常规外泌体更大,并富含CD44(一种与乳腺癌转移相关的蛋白质)。基于它们的大尺寸,我们称这些囊泡为L-外泌体。与miRNA在乳腺癌细胞不同微泡中的分布相反,正常细胞会在一种囊泡中释放所有测得的miRNA。我们的结果表明,恶性转化会改变特定miRNA从细胞输出的途径。颗粒及其miRNA货物中的这些变化可用于检测体内恶性细胞的存在。

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