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Oncoprotein stabilization in brain tumors

机译:脑肿瘤中癌蛋白的稳定化

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摘要

Proteins involved in promoting cell proliferation and viability need to be timely expressed and carefully controlled for the proper development of the brain but also efficiently degraded in order to prevent cells from becoming brain cancer cells. A major pathway for targeted protein degradation in cells is the ubiquitin–proteasome system (UPS). Oncoproteins that drive tumor development and tumor maintenance are often deregulated and stabilized in malignant cells. This can occur when oncoproteins escape degradation by the UPS because of mutations in either the oncoprotein itself or in the UPS components responsible for recognition and ubiquitylation of the oncoprotein. As the pathogenic accumulation of an oncoprotein can lead to effectively sustained cell growth, viability and tumor progression, it is an indisputable target for cancer treatment. The most common types of malignant brain tumors in children and adults are medulloblastoma and glioma, respectively. Here, we review different ways of how deregulated proteolysis of oncoproteins involved in major signaling cancer pathways contributes to medulloblastoma and glioma development. We also describe means of targeting relevant oncoproteins in brain tumors with treatments affecting their stability or therapeutic strategies directed against the UPS itself.
机译:为了促进脑的正常发育,需要及时表达和仔细控制参与促进细胞增殖和活力的蛋白质,但为了防止细胞变成脑癌细胞,它们也需要有效降解。细胞中靶向蛋白质降解的主要途径是泛素-蛋白酶体系统(UPS)。驱动肿瘤发展和肿瘤维持的癌蛋白通常在恶性细胞中被失调和稳定。当由于癌蛋白本身或负责癌蛋白识别和泛素化的UPS组件中的突变而使癌蛋白无法通过UPS降解时,就会发生这种情况。由于癌蛋白的致病性积累可导致有效持续的细胞生长,生存能力和肿瘤进展,因此它是癌症治疗不可争议的目标。儿童和成人中最常见的恶性脑肿瘤类型分别是髓母细胞瘤和神经胶质瘤。在这里,我们审查了不同的方式,涉及主要信号通路的癌蛋白的蛋白水解失调如何促成髓母细胞瘤和神经胶质瘤的发展。我们还描述了针对脑肿瘤中相关癌蛋白的治疗手段,这些手段会影响其稳定性或针对UPS本身的治疗策略。

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