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首页> 外文期刊>Frontiers in Oncology >Intercellular Vesicular Transfer by Exosomes, Microparticles and Oncosomes - Implications for Cancer Biology and Treatments
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Intercellular Vesicular Transfer by Exosomes, Microparticles and Oncosomes - Implications for Cancer Biology and Treatments

机译:外来体,微粒和癌体的细胞间囊泡转移-对癌症生物学和治疗的意义

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Intercellular communication is a normal feature of most physiological interactions between cells in healthy organisms. While cells communicate directly through intimate physiology contact, other mechanisms of communication exist, such as through the influence of soluble mediators such as growth factors, cytokines and chemokines. There is, however, yet another mechanism of intercellular communication that permits the exchange of information between cells through extracellular vesicles (EVs). EVs are microscopic (50 nm?10 μM) phospholipid bilayer enclosed entities produced by virtually all eukaryotic cells. EVs are abundant in the intracellular space and are present at a cells' normal microenvironment. Irrespective of the EV “donor” cell type, or the mechanism of EV biogenesis and production, or the size and EV composition, cancer cells have the potential to utilize EVs in a manner that enhances their survival. For example, cancer cell EV overproduction confers benefits to tumor growth, and tumor metastasis, compared with neighboring healthy cells. Herein, we summarize the current status of knowledge on different populations of EVs. We review the situations that regulate EV release, and the factors that instruct differential packaging or sorting of EV content. We then highlight the functions of cancer-cell derived EVs as they impact on cancer outcomes, promoting tumor progression, metastases, and the mechanisms by which they facilitate the creation of a pre-metastatic niche. The review finishes by focusing on the beneficial (and challenging) features of tumor-derived EVs that can be adapted and utilized for cancer treatments, including those already being investigated in human clinical trials.
机译:细胞间通讯是健康生物体内细胞之间大多数生理相互作用的正常特征。当细胞通过紧密的生理接触直接交流时,存在其他的交流机制,例如通过可溶性介质(例如生长因子,细胞因子和趋化因子)的影响。但是,还有另一种细胞间通讯机制,该机制允许通过细胞外囊泡(EVs)在细胞之间交换信息。电动汽车是由几乎所有真核细胞产生的微观(50 nm?10μM)磷脂双层包裹的实体。电动汽车在细胞内空间中很丰富,并存在于细胞的正常微环境中。不论EV“供体”细胞的类型,EV生源和产生的机制,或EV的大小和组成如何,癌细胞都有可能以提高其存活率的方式利用EV。例如,与邻近的健康细胞相比,癌细胞电动汽车的过量生产可为肿瘤生长和肿瘤转移带来益处。在此,我们总结了不同电动汽车人群的知识现状。我们回顾了规范EV释放的情况,以及指示差异包装或EV内容分类的因素。然后,我们重点介绍了源自癌细胞的电动汽车的功能,因为它们影响癌症结局,促进肿瘤进展,转移以及它们促进转移前利基形成的机制。这篇综述的重点是肿瘤电动汽车的有益(和具有挑战性)特征,这些电动汽车可以适应并用于癌症治疗,包括那些已经在人类临床试验中进行研究的电动汽车。

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