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Exosomes and immune surveillance of neoplastic lesions: A review

机译:外瘤和免疫监测肿瘤病变:综述

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The immune system has been reported to suppress the development and progression of neoplastic lesions; however, the exact mechanisms by which neoplastic lesions and the immune system interact are not well understood. Within the last decade, tiny membrane bound particles, approximately 30-100 nm in diameter, have been observed in the blood and other body fluids. These particles, currently called exosomes, are released from many types of tissues including tumors, and they contain and carry many proteins, and mRNAs and microRNA species. We review here how tumors suppress the immune system, especially by the formation of exosomes. Exosomes released from tumors are carried in part by the vascular system to distant cells, which phagocytose them. Depending on the proteins, mRNAs or microRNAs in the exosomes and the cell type, phagocytosis of exosomes may provide a modulating signal to the cell. In the case of exosomes from tumors, uptake of the exosomes by cells of the immune system has been reported to have three main effects: 1) suppression of the number and activity of natural killer cells, 2) suppression of the activity of T cells and 3) suppression of the number and maturation of mature dendritic cells.
机译:据报道,免疫系统抑制了肿瘤病变的发展和进展;然而,肿瘤病变和免疫系统相互作用的确切机制尚不清楚。在过去的十年内,在血液和其他体液中观察到血液和直径约30-100nm的微小膜结合颗粒。目前被称为外泌体的这些颗粒从包括肿瘤的许多类型的组织中释放,它们含有并携带许多蛋白质和MRNA和MICRRNA物种。我们在此审查肿瘤如何抑制免疫系统,特别是通过形成外来体。从肿瘤中释放的外泌体部分地由血管系统携带到远处细胞,其吞噬它们。根据蛋白质,MRNA或微小RNA和细胞型,外泌体的吞噬作用可以向细胞提供调节信号。在来自肿瘤外来的情况下,据报道,免疫系统细胞的摄取是具有三个主要影响:1)抑制自然杀伤细胞的数量和活性,2)抑制T细胞的活性和3)抑制成熟树突细胞的数量和成熟。

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