端粒和端粒酶在神经退行性疾病中的潜在作用

Jun Shao, Jing Wang, Bo Li, Chuanbin Liu
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引用次数: 0

摘要

端粒是位于染色体末端的重要 DNA 蛋白复合物,在防止染色体融合、重组和降解方面发挥着关键作用,从而确保基因组的稳定性。当端粒达到极限缩短长度时,就会激活DNA损伤检查点,停止细胞分裂,引发复制衰老。端粒酶由核糖核酸(RNA)和蛋白质组成,可以合成端粒重复序列,延长端粒。研究表明,端粒长度(TL)和端粒酶活性与衰老、与衰老相关的退行性疾病和肿瘤密切相关。神经退行性疾病(NDDs)是由遗传和环境因素引起的主要衰老相关疾病之一,具有起病隐匿、诊断困难、疾病进展不可逆、缺乏有效治疗等特点,给社会和家庭带来沉重负担。目前,许多研究都注意到了NDD中白细胞端粒长度(LTL)和端粒酶活性的变化,这表明端粒和端粒酶在NDD发病机制中起着至关重要的作用。本综述探讨了端粒长度与 NDD 之间的关系,研究了作为潜在治疗靶点的端粒酶,并讨论了用于 NDD 诊断和治疗的新兴生物标记物和干预策略。
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Potential roles of telomeres and telomerase in neurodegenerative diseases
Telomeres, essential DNA-protein complexes located at chromosome ends, play a critical role in preventing chromosome fusion, recombination, and degradation, thus ensuring genomic stability. When telomeres reach a limiting shortened length, they will activate DNA damage checkpoints, stop cell division and trigger replicative senescence. Telomerase is composed of RNA and protein, which can synthesize telomeres repeat sequences, and elongate telomeres. Studies have shown that telomere length (TL) and telomerase activity are closely involved in aging, aging-related degenerative diseases, and tumors. Neurodegenerative diseases (NDDs) are one of the major aging-related diseases caused by both genetic and environmental factors, characterized by insidious onset, difficult diagnosis, irreversible disease progression, and lack of effective treatments, which brings a heavy burden to society and families. Currently, many studies have noted variations in leukocyte telomere length (LTL) and telomerase activity in NDDs, suggesting a vital role for telomeres and telomerase in NDD pathogenesis. This review explores the relationship between TL and NDDs, examines telomerase as a potential therapeutic target, and discusses emerging biomarkers and intervention strategies for NDD diagnosis and treatment.
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