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DNA replication licensing proteins: Saints and sinners in cancer

机译:DNA复制许可蛋白:癌症中的圣徒和罪人

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DNA replication is all-or-none process in the cell, meaning, once the DNA replication begins it proceeds to completion. Hence, to achieve maximum control of DNA replication, eukaryotic cells employ a multi-subunit initiator protein complex known as "pre-replication complex or DNA replication licensing complex (DNA replication LC). This complex involves multiple proteins which are origin-recognition complex family proteins, cell division cycle-6, chromatin licensing and DNA replication factor 1, and minichromosome maintenance family proteins. Higher-expression of DNA replication LC proteins appears to be an early event during development of cancer since it has been a common hallmark observed in a wide variety of cancers such as oesophageal, laryngeal, pulmonary, mammary, colorectal, renal, urothelial etc. However, the exact mechanisms leading to the abnormally high expression of DNA replication LC have not been clearly deciphered. Increased expression of DNA replication LC leads to licensing and/or firing of multiple origins thereby inducing replication stress and genomic instability. Therapeutic approaches where the reduction in the activity of DNA replication LC was achieved either by siRNA or shRNA techniques, have shown increased sensitivity of cancer cell lines towards the anti-cancer drugs such as cisplatin, 5-Fluorouracil, hydroxyurea etc. Thus, the expression level of DNA replication LC within the cell determines a cell's fate thereby creating a paradox where DNA replication LC acts as both "Saint" and "Sinner". With a potential to increase sensitivity to chemotherapy drugs, DNA replication LC proteins have prospective clinical importance in fighting cancer. Hence, in this review, we will shed light on importance of DNA replication LC with an aim to use DNA replication LC in diagnosis and prognosis of cancer in patients as well as possible therapeutic targets for cancer therapy.
机译:DNA复制是细胞中的全部或无过程,意味着,一旦DNA复制开始,它就完成了完成。因此,为了实现DNA复制的最大控制,真核细胞使用称为“预复制复合物或DNA复制许可证综合体(DNA复制LC)的多亚基引发剂蛋白复合物。该综合体涉及多种蛋白质,这些蛋白质是起源识别复杂的家庭蛋白质,细胞分裂循环-6,染色质许可和DNA复制因子1,以及美学组织培养家族蛋白。DNA复制LC蛋白的较高表达似乎是癌症开发期间的早期事件,因为它是在a中观察到的共同标志各种各样的癌症如食管,喉,肺,乳腺,结直肠,肾,尿路上皮等,导致对DNA复制LC异常高表达的确切机制尚未明确破译。DNA复制LC引线的表达增加许多起源的许可和/或射击,从而诱导复制应力和基因组不稳定性。治疗性批准HESHER,其中DNA复制LC的活性的降低通过siRNA或shRNA技术实现,显示癌细胞系朝向抗癌药物如顺铂,5-氟尿嘧啶,羟基脲等的敏感性,因此表达水平细胞内的DNA复制LC确定一个小区的命运,从而创建一个悖论,其中DNA复制LC作为“圣徒”和“罪人”。随着对化疗药物敏感的潜力,DNA复制LC蛋白在癌症中具有前瞻性临床重要性。因此,在本次综述中,我们将阐明DNA复制LC的重要性,目的是在患者的癌症和可能治疗靶标的癌症治疗中使用DNA复制LC。

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