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Melanoma Affects the Composition of Blood Cell-Derived Extracellular Vesicles

机译:黑色素瘤影响血细胞衍生的细胞外囊泡的组成。

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摘要

Extracellular vesicles (EVs) are specifically loaded with nucleic acids, lipids, and proteins from their parental cell. Therefore, the constitution of EVs reflects the type and status of the originating cell and EVs in melanoma patient’s plasma could be indicative for the tumor. Likewise, EVs might influence tumor progression by regulating immune responses. We performed a broad protein characterization of EVs from plasma of melanoma patients and healthy donors as well as from T cells, B cells, natural killer (NK) cells, monocytes, monocyte-derived dendritic cells (moDCs), and platelets using a multiplex bead-based platform. Using this method, we succeeded in analyzing 58 proteins that were differentially displayed on EVs. Hierarchical clustering of protein intensity patterns grouped EVs according to their originating cell type. The analysis of EVs from stimulated B cells and moDCs revealed the transfer of surface proteins to vesicles depending on the cell status. The protein profiles of plasma vesicles resembled the protein profiles of EVs from platelets, antigen-presenting cells and NK cells as shown by platelet markers, co-stimulatory proteins, and a NK cell subpopulation marker. In comparison to healthy plasma vesicles, melanoma plasma vesicles showed altered signals for platelet markers, indicating a changed vesicle secretion or protein loading of EVs by platelets and a lower CD8 signal that might be associated with a diminished activity of NK cells or T cells. As we hardly detected melanoma-derived vesicles in patient’s plasma, we concluded that blood cells induced the observed differences. In summary, our results question a direct effect of melanoma cells on the composition of EVs in melanoma plasma, but rather argue for an indirect influence of melanoma cells on the vesicle secretion or vesicle protein loading by blood cells.
机译:细胞外囊泡(EV)特异地从其亲代细胞中装载了核酸,脂质和蛋白质。因此,EV的构成反映了原始细胞的类型和状态,黑色素瘤患者血浆中的EV可能指示肿瘤。同样,电动汽车可能会通过调节免疫反应来影响肿瘤的进展。我们使用多重磁珠对黑色素瘤患者血浆和健康供体以及T细胞,B细胞,自然杀伤(NK)细胞,单核细胞,单核细胞衍生的树突状细胞(moDC)和血小板的EV进行了广泛的蛋白质表征基于平台。使用这种方法,我们成功地分析了在电动汽车上差异显示的58种蛋白质。蛋白质强度模式的分层聚类根据其原始细胞类型将电动汽车分组。对受刺激的B细胞和moDC的EV的分析表明,取决于细胞状态,表面蛋白向囊泡的转移。血浆囊泡的蛋白质谱类似于血小板,抗原呈递细胞和NK细胞的EV的蛋白质谱,如血小板标记,共刺激蛋白和NK细胞亚群标记所示。与健康血浆囊泡相比,黑色素瘤血浆囊泡显示血小板标志物信号改变,表明血小板分泌的囊泡分泌改变或EV的蛋白质负载增加,而CD8信号降低,这可能与NK细胞或T细胞活性降低有关。由于我们几乎没有检测到患者血浆中黑色素瘤衍生的囊泡,因此我们得出结论,血细胞可引起观察到的差异。总而言之,我们的结果质疑黑色素瘤细胞对黑色素瘤血浆中EV组成的直接影响,而是主张黑色素瘤细胞对血细胞分泌的囊泡或囊泡蛋白负载有间接影响。

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