Notch signalling pathway as an oncogenic factor involved in cancer development

M. Brzozowa-Zasada, A. Piecuch, Anna Dittfeld, Ł. Mielańczyk, M. Michalski, G. Wyrobiec, M. Harabin-Słowińska, J. Kurek, R. Wojnicz
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引用次数: 37

Abstract

Notch signalling is an evolutionarily conserved signalling pathway, which plays a significant role in a wide array of cellular processes including proliferation, differentiation, and apoptosis. Nevertheless, it must be noted that Notch is a binary cell fate determinant, and its overexpression has been described as oncogenic in a broad range of human malignancies. This finding led to interest in therapeutically targeting this pathway especially by the use of GSIs, which block the cleavage of Notch at the cell membrane and inhibit release of the transcriptionally active NotchIC subunit. Preclinical cancer models have clearly demonstrated that GSIs suppress the growth of such malignancies as pancreatic, breast, and lung cancer; however, GSI treatment in vivo is associated with side effects, especially those within the gastrointestinal tract. Although intensive studies are associated with the role of γ-secretase in pathological states, it should be pointed out that this complex impacts on proteolytic cleavages of around 55 membrane proteins. Therefore, it is clear that GSIs are highly non-specific and additional drugs must be designed, which will more specifically target components of the Notch signalling.
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Notch信号通路作为致癌因子参与癌症发展
Notch信号是一种进化上保守的信号通路,在包括增殖、分化和凋亡在内的一系列细胞过程中起着重要作用。然而,必须指出的是,Notch是一个二元细胞的命运决定因素,其过表达已被描述为在广泛的人类恶性肿瘤中致癌。这一发现引起了人们对治疗这一途径的兴趣,特别是通过使用gsi, gsi可以阻断Notch在细胞膜上的切割并抑制转录活性NotchIC亚基的释放。临床前癌症模型清楚地表明,gsi抑制胰腺癌、乳腺癌和肺癌等恶性肿瘤的生长;然而,体内GSI治疗与副作用有关,特别是胃肠道内的副作用。尽管大量研究与病理状态下γ-分泌酶的作用有关,但应该指出的是,这种复合物影响约55种膜蛋白的蛋白水解裂解。因此,很明显gsi是高度非特异性的,必须设计额外的药物,这些药物将更特异性地靶向Notch信号的成分。
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