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Gamma secretase inhibitors of Notch signaling

机译:Notch信号的γ分泌酶抑制剂

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摘要

The numerous processes involved in the etiology of breast cancer such as cell survival, metabolism, proliferation, differentiation, and angiogenesis are currently being elucidated. However, underlying mechanisms that drive breast cancer progression and drug resistance are still poorly understood. As we discuss here in detail, the Notch signaling pathway is an important regulatory component of normal breast development, cell fate of normal breast stem cells, and proliferation and survival of breast cancer initiating cells. Notch exerts a wide range of critical effects through a canonical pathway where it is expressed as a type I membrane precursor heterodimer followed by at least two subsequent cleavages induced by ligand engagement to ultimately release an intracellular form to function as a transcriptional activator. Notch and its ligands are overexpressed in breast cancer, and one method of effectively blocking Notch activity is preventing its cleavage at the cell surface with γ-secretase inhibitors. In the context of Notch signaling, the application of clinically relevant anti-Notch drugs in treatment regimens may contribute to novel therapeutic interventions and promote more effective clinical response in women with breast cancer.
机译:当前正在阐明与乳腺癌的病因有关的许多过程,例如细胞存活,代谢,增殖,分化和血管生成。但是,驱动乳腺癌进展和耐药性的基本机制仍知之甚少。正如我们在此处详细讨论的那样,Notch信号通路是正常乳腺发育,正常乳腺干细胞的细胞命运以及乳腺癌起始细胞的增殖和存活的重要调控成分。 Notch通过经典途径发挥广泛的关键作用,在经典途径中,Notch被表达为I型膜前体异二聚体,随后通过配体结合而诱导的至少两次后续裂解,最终释放出细胞内形式以充当转录激活因子。 Notch及其配体在乳腺癌中过表达,有效阻断Notch活性的一种方法是用γ-分泌酶抑制剂阻止其在细胞表面的裂解。在Notch信号转导的背景下,临床上相关的Notch药物在治疗方案中的应用可能有助于新型治疗手段,并促进乳腺癌女性的更有效临床反应。

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