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CSE1L, a novel microvesicle membrane protein, mediates Ras-triggered microvesicle generation and metastasis of tumor cells

机译:CSE1L,一种新型的微泡膜蛋白,介导Ras触发的微泡生成和肿瘤细胞转移

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Tumor-derived microvesicles are rich in metastasis-related proteases and play a role in the interactions between tumor cells and tumor microenvironment in tumor metastasis. Because shed microvesicles may remain in the extracellular environment around tumor cells, the microvesicle membrane protein may be the potential target for cancer therapy. Here we report that chromosome segregation 1-like (CSE1L) protein is a microvesicle membrane protein and is a potential target for cancer therapy. v-H-Ras expression induced extracellular signal-regulated kinase (ERK)-dependent CSE1L phosphorylation and microvesicle biogenesis in various cancer cells. CSE1L overexpression also triggered microvesicle generation, and CSE1L knockdown diminished v-H-Ras-induced microvesicle generation, matrix metalloproteinase (MMP)-2 and MMP-9 secretion and metastasis of B16F10 melanoma cells. CSE1L was preferentially accumulated in microvesicles and was located in the microvesicle membrane. Furthermore, anti-CSE1L antibody-conjugated quantum dots could target tumors in animal models. Our findings highlight a novel role of Ras-ERK signaling in tumor progression and suggest that CSE1L may be involved in the "early" and "late" metastasis of tumor cells in tumorigenesis. Furthermore, the novel microvesicle membrane protein, CSE1L, may have clinical utility in cancer diagnosis and targeted cancer therapy.
机译:肿瘤来源的微泡富含转移相关的蛋白酶,并在肿瘤转移中在肿瘤细胞与肿瘤微环境之间的相互作用中发挥作用。由于脱落的微泡可能保留在肿瘤细胞周围的细胞外环境中,因此微泡膜蛋白可能是癌症治疗的潜在靶标。在这里我们报告染色体分离1样(CSE1L)蛋白是一种微泡膜蛋白,是癌症治疗的潜在目标。 v-H-Ras表达诱导各种癌细胞中的细胞外信号调节激酶(ERK)依赖性CSE1L磷酸化和微泡生物发生。 CSE1L的过表达也触发了微囊泡的产生,而CSE1L的敲低则减少了v-H-Ras诱导的微囊泡的产生,基质金属蛋白酶(MMP)-2和MMP-9的分泌以及B16F10黑色素瘤细胞的转移。 CSE1L优先积聚在微泡中,并位于微泡膜中。此外,抗CSE1L抗体缀合的量子点可以靶向动物模型中的肿瘤。我们的发现突出了Ras-ERK信号传导在肿瘤进展中的新作用,并暗示CSE1L可能参与肿瘤发生过程中肿瘤细胞的“早期”和“晚期”转移。此外,新型微囊泡膜蛋白CSE1L在癌症诊断和靶向癌症治疗中可能具有临床效用。

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