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首页> 外文期刊>Neoplasma: Journal of Experimental and Clinical Oncology >Targeting rictor inhibits mouse vascular tumor cell proliferation and invasion in vitro and tumor growth in vivo.
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Targeting rictor inhibits mouse vascular tumor cell proliferation and invasion in vitro and tumor growth in vivo.

机译:靶向rictor抑制小鼠血管肿瘤细胞的体外增殖和侵袭以及体内肿瘤的生长。

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摘要

Vascular tumor is an abnormal buildup of blood vessels in the skin or internal organs that can lead to disfigurement and/or life-threatening consequences. The mechanism of hemangiogenesis remains unknown. The aim of this study was to assess the role of rapamycin-insensitive companion of mTOR (Rictor) in control of vascular tumor malignant biological behavior and cell signaling mechanism in Mouse Hemangioendothelioma Endothelial Cells (EOMA cells) and nude mouse model. Knocking down rictor was mediated by lentivirus shRNA. The role and mechanism of rictor in vascular tumor were assessed by western blotting, wst-1 proliferation assay, matrigel invasion assay and xenograft vascular tumor growth. Our results in vitro showed that loss of rictor down-regulated phosphorylation of AKT and S6 by which EOMA cells growth and proliferation were greatly suppressed. Knock down of rictor also inhibited the invasion of EOMA cells. Furthermore, we demonstrated that knock down of rictor inhibited xenograft vascular tumor growth in nude mice. Taken together, we purpose that rictor contributed to vascular tumor growth and progression. Targeting rictor becomes an effective strategy in vascular tumor treatment. Keywords: AKT, mTOR2, rictor, vascular tumor, hemangioma.
机译:血管肿瘤是皮肤或内脏中血管的异常堆积,可能导致毁容和/或危及生命的后果。血管生成的机制仍然未知。这项研究的目的是评估雷帕霉素不敏感的同伴mTOR(Rictor)在控制小鼠血管内皮细胞瘤内皮细胞(EOMA细胞)和裸鼠模型中的血管肿瘤恶性生物学行为和细胞信号传导机制中的作用。敲除rictor是由慢病毒shRNA介导的。 rictor在血管肿瘤中的作用和机制通过蛋白质印迹,wst-1增殖测定,matrigel入侵测定和异种移植血管肿瘤生长进行评估。我们的体外研究结果表明,rictor的丢失下调了AKT和S6的磷酸化,从而大大抑制了EOMA细胞的生长和增殖。敲除rictor也抑制了EOMA细胞的侵袭。此外,我们证明敲除蓖麻油可以抑制裸鼠的异种移植血管肿瘤生长。综上所述,我们旨在使rictor促进血管肿瘤的生长和发展。靶向rictor成为治疗血管肿瘤的有效策略。关键词:AKT,mTOR2,rictor,血管瘤,血管瘤。

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