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HMGNs, DNA repair and cancer.

机译:HMGN,DNA修复和癌症。

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摘要

DNA lesions threaten the integrity of the genome and are a major factor in cancer formation and progression. Eukaryotic DNA is organized in nucleosome-based higher order structures, which form the chromatin fiber. In recent years, considerable knowledge has been gained on the importance of chromatin dynamics for the cellular response to DNA damage and for the ability to repair DNA lesions. High Mobility Group N1 (HMGN1) protein is an emerging factor that is important for chromatin alterations in response to DNA damage originated from both ultra violet light (UV) and ionizing irradiation (IR). HMGN1 is a member in the HMGN family of chromatin architectural proteins. HMGNs bind directly to nucleosomes and modulate the structure of the chromatin fiber in a highly dynamic manner. This review focuses mainly on the roles of HMGN1 in the cellular response pathways to different types of DNA lesions and in transcriptional regulation of cancer-related genes. In addition, emerging roles for HMGN5 in cancer progression and for HMGN2 as a potential tool in cancer therapy will be discussed.
机译:DNA损伤威胁基因组的完整性,并且是癌症形成和进展的主要因素。真核DNA以基于核小体的高级结构组织,形成染色质纤维。近年来,已经获得了关于染色质动力学对于细胞对DNA损伤的反应和修复DNA损伤的能力的重要性的大量知识。 N1高迁移率族蛋白(HMGN1)是新兴的因子,对于响应源自紫外线(UV)和电离辐射(IR)的DNA损伤的染色质变化非常重要。 HMGN1是染色质建筑蛋白HMGN家族的成员。 HMGNs直接与核小体结合,并以高度动态的方式调节染色质纤维的结构。这篇综述主要侧重于HMGN1在细胞对不同类型的DNA损伤的反应途径中的作用以及在癌症相关基因的转录调控中的作用。另外,将讨论HMGN5在癌症进展中的新兴作用以及HMGN2作为癌症治疗中潜在的工具。

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