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首页> 外文期刊>Acta Histochemica: Zeitschrift fur Histologische Topochemie >The cell giveth and the cell taketh away: an overview of Notch pathway activation by endocytic trafficking of ligands and receptors.
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The cell giveth and the cell taketh away: an overview of Notch pathway activation by endocytic trafficking of ligands and receptors.

机译:细胞产生并被细胞带走:通过内吞运输配体和受体来激活Notch途径的概述。

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摘要

Notch signaling is firmly established as a form of cell-to-cell communication that is critical throughout development. Dysregulation of Notch has been linked to cancer and developmental disorders, making it an important target for therapeutic intervention. One aspect of this pathway that sets it apart from others is its apparent reliance on endocytosis by signal-sending and signal-receiving cells. The subtle details of endocytosis-mediated molecular processing within both ligand- and receptor-presenting cells that are required for the Notch signal to maintain fidelity remain unclear. The endosomal system has long been known to play an important role in terminating signal transduction by directing lysosomal trafficking and degradation of cell surface receptors. More recently, endocytic trafficking has also been shown to be critical for activation of signaling. This review highlights four models of endocytic processing in the context of the Notch pathway. In ligand-presenting cells, endocytosis may be required for pre-processing of ligands to make them competent for interaction with Notch receptors and/or for exerting a pulling force on the ligand/Notch complex. In receptor-presenting cells, endocytosis may be a prerequisite for Notch cleavage and thus activation and/or it could be a means of limiting ligand-independent Notch activation. Recent advances in our understanding of how and why endocytosis of Notch receptors and ligands is required for activation and termination of signaling during normal development and in disease states are discussed.
机译:陷波信号已被牢固地确立为在整个开发过程中至关重要的一种单元间通信形式。 Notch失调与癌症和发育异常有关,使其成为治疗干预的重要靶标。该途径与众不同的一个方面是其明显依赖信号发送和信号接收细胞的内吞作用。 Notch信号保持保真度所需的配体和受体呈递细胞内的内吞作用介导的分子加工的细微细节仍不清楚。早已知道内体系统通过指导溶酶体运输和细胞表面受体的降解在终止信号转导中起重要作用。最近,内吞运输也已被证明对于激活信号是至关重要的。这篇综述重点介绍了在Notch途径中内吞加工的四种模型。在存在配体的细胞中,可能需要胞吞作用来进行配体的预处理,以使其能够与Notch受体相互作用和/或对配体/ Notch复合体施加拉力。在受体呈递细胞中,内吞作用可能是Notch裂解并因此激活的先决条件,和/或它可能是限制不依赖配体的Notch激活的手段。讨论了我们对Notch受体和配体的内吞作用以及在正常发育过程中和疾病状态下激活和终止信号传导的要求的理解的最新进展。

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