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首页> 外文期刊>Journal of Extracellular Vesicles >Extensive surface protein profiles of extracellular vesicles from cancer cells may provide diagnostic signatures from blood samples
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Extensive surface protein profiles of extracellular vesicles from cancer cells may provide diagnostic signatures from blood samples

机译:癌细胞胞外囊泡的广泛表面蛋白谱可提供血样的诊断特征

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Extracellular vesicles (EV) are membranous particles (30–1,000 nm in diameter) secreted by cells. Important biological functions have been attributed to 2 subsets of EV, the exosomes (bud from endosomal membranes) and the microvesicles (MV; bud from plasma membranes). Since both types of particles contain surface proteins derived from their cell of origin, their detection in blood may enable diagnosis and prognosis of disease. We have used an antibody microarray (DotScan) to compare the surface protein profiles of live cancer cells with those of their EV, based on their binding patterns to immobilized antibodies. Initially, EV derived from the cancer cell lines, LIM1215 (colorectal cancer) and MEC1 (B-cell chronic lymphocytic leukaemia; CLL), were used for assay optimization. Biotinylated antibodies specific for EpCAM (CD326) and CD19, respectively, were used to detect captured particles by enhanced chemiluminescence. Subsequently, this approach was used to profile CD19~(+)EV from the plasma of CLL patients. These EV expressed a subset (~40%) of the proteins detected on CLL cells from the same patients: moderate or high levels of CD5, CD19, CD31, CD44, CD55, CD62L, CD82, HLA-A,B,C, HLA-DR; low levels of CD21, CD49c, CD63. None of these proteins was detected on EV from the plasma of age- and gender-matched healthy individuals.
机译:细胞外囊泡(EV)是细胞分泌的膜状颗粒(直径为30-1,000 nm)。重要的生物学功能归因于EV的2个子集,即外泌体(来自内体膜的芽)和微囊泡(MV;来自质膜的芽)。由于两种类型的颗粒均包含源自其起源细胞的表面蛋白,因此在血液中对其进行检测可以实现疾病的诊断和预后。我们已经使用抗体微阵列(DotScan),根据其与固定抗体的结合模式,比较了活癌细胞和其EV的表面蛋白谱。最初,将源自癌细胞系LIM1215(结肠直肠癌)和MEC1(B细胞慢性淋巴细胞性白血病; CLL)的EV用于分析优化。分别对EpCAM(CD326)和CD19特异的生物素化抗体被用于通过增强的化学发光来检测捕获的颗粒。随后,该方法用于分析CLL患者血浆中的CD19〜(+)EV。这些EV表达了在同一患者的CLL细胞上检测到的蛋白质的一部分(〜40%):中度或高水平的CD5,CD19,CD31,CD44,CD55,CD62L,CD82,HLA-A,B,C,HLA -DR;低水平的CD21,CD49c,CD63。在年龄和性别匹配的健康个体血浆中,在EV上均未检测到这些蛋白质。

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