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Function, replication and structure of the mammalian telomere

机译:哺乳动物端粒的功能,复制和结构

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Telomeres are specialized structures at the ends of linear chromosomes that were originally defined functionally based on observations first by Muller (1938) and subsequently by McClintock (1941) that naturally occurring chromosome ends do not behave as double-stranded DNA breaks, in spite of the fact that they are the physical end of a linear, duplex DNA molecule. Double-stranded DNA breaks are highly unstable entities, being susceptible to nucleolytic attack and giving rise to chromosome rearrangements through end-to-end fusions and recombination events. In contrast, telomeres confer stability upon chromosome termini, as evidenced by the fact that chromosomes are extraordinarily stable through multiple cell divisions and even across evolutionary time. This protective function of telomeres is due to the formation of a nucleoprotein complex that sequesters the end of the DNA molecule, rendering it inaccessible to nucleases and recombinases as well as preventing the telomere from activating the DNA damage checkpoint pathways. The capacity of a functional end-protective complex to form is dependent upon maintenance of sufficient telomeric DNA. We have learned a great deal about telomere structure and how this specialized nucleoprotein complex confers stability on chromosome ends since the original observations that defined telomeres were made. This review summarizes our current understanding of mammalian telomere replication, structure and function.
机译:端粒是线性染色体末端的特殊结构,最初是根据穆勒(1938)和麦克林托克(1941)的观察在功能上进行定义的,尽管观察到的是,天然存在的染色体末端并不表现为双链DNA断裂。事实上,它们是线性双链DNA分子的物理末端。双链DNA断裂是高度不稳定的实体,易受溶核攻击,并通过端对端融合和重组事件引起染色体重排。相比之下,端粒赋予染色体末端以稳定性,这一事实证明了染色体通过多个细胞分裂甚至在整个进化时间内都非常稳定。端粒的这种保护功能是由于形成了一种核蛋白复合物,该复合物螯合了DNA分子的末端,使核酸酶和重组酶难以接近,并阻止了端粒激活DNA损伤检查点途径。功能性末端保护复合物形成的能力取决于维持足够的端粒DNA。自从进行了定义端粒的原始观察以来,我们已经学到了很多有关端粒结构以及这种专门的核蛋白复合物如何赋予染色体末端稳定性的知识。这篇综述总结了我们目前对哺乳动物端粒复制,结构和功能的理解。

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