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首页> 外文期刊>Journal of Pathology: Journal of the Pathological Society of Great Britain and Ireland >Telomere-associated proteins: cross-talk between telomere maintenance and telomere-lengthening mechanisms.
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Telomere-associated proteins: cross-talk between telomere maintenance and telomere-lengthening mechanisms.

机译:端粒相关蛋白:端粒维持与端粒延长机制之间的串扰。

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摘要

Telomeres, the ends of eukaryotic chromosomes, have been the subject of intense investigation over the last decade. As telomere dysfunction has been associated with ageing and developing cancer, understanding the exact mechanisms regulating telomere structure and function is essential for the prevention and treatment of human cancers and age-related diseases. The mechanisms by which cells maintain telomere lengthening involve either telomerase or the alternative lengthening of the telomere pathway, although specific mechanisms of the latter and the relationship between the two are as yet unknown. Many cellular factors directly (TRF1/TRF2) and indirectly (shelterin-complex, PinX, Apollo and tankyrase) interact with telomeres, and their interplay influences telomere structure and function. One challenge comes from the observation that many DNA damage response proteins are stably associated with telomeres and contribute to several other aspects of telomere function. This review focuses on the different components involved in telomere maintenance and their role in telomere length homeostasis. Special attention is paid to understanding how these telomere-associated factors, and mainly those involved in double-strand break repair, perform their activities at the telomere ends.
机译:端粒是真核染色体的末端,在过去的十年中一直是研究的重点。由于端粒功能障碍与衰老和发展中的癌症有关,因此了解调节端粒结构和功能的确切机制对于预防和治疗人类癌症及与年龄有关的疾病至关重要。细胞维持端粒延长的机制涉及端粒酶或端粒途径的替代延长,尽管尚不清楚后者的具体机制以及两者之间的关系。许多细胞因子直接(TRF1 / TRF2)和间接(shelterin-complex,PinX,Apollo和tankyrase)间接与端粒相互作用,它们的相互作用影响端粒的结构和功能。一个挑战来自于观察到许多DNA损伤反应蛋白与端粒稳定相关,并有助于端粒功能的其他几个方面。这篇综述着重于端粒维持过程中涉及的不同成分及其在端粒长度稳态中的作用。要特别注意了解这些端粒相关因子(主要是那些参与双链断裂修复的因子)如何在端粒末端发挥作用。

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