中心体
有丝分裂
极光抑制剂
主轴检查点
PLK1
极光A激酶
细胞生物学
癌症研究
主轴装置
极光激酶B
生物
染色体不稳定性
极光激酶
细胞周期
细胞分裂
细胞
遗传学
染色体
基因
作者
Xiaoyang Lin,Xiaosong Xiang,Liping Hao,Ting Wang,Yongting Lai,Mubalake Abudoureyimu,Hao Zhou,Bing Feng,Xiaoyuan Chen,Rui Wang
出处
期刊:PubMed
日期:2020-01-01
卷期号:10 (9): 2705-2729
被引量:19
摘要
Aurora-A is a mitotic serine/threonine-protein kinase and an oncogene. In normal cells, Aurora-A appears from G2 phase and localizes at the centrosome, where it participates in centrosome replication, isolation and maturation. Aurora-A also maintains Golgi apparatus structure and spindle assembly. Aurora-A undergoes ubiquitination-mediated degradation after the cell division phase. Aurora-A is abnormally expressed in tumor cells and promotes cell proliferation by regulating mitotic substrates, such as PP1, PLK1, TPX2, and LAST2, and affects other molecules through a non-mitotic pathway to promote cell invasion and metastasis. Some molecules in tumor cells also indirectly act on Aurora-A to regulate tumor cells. Aurora-A also mediates resistance to chemotherapy and radiotherapy and is involved in tumor immunotherapy. Clinical trials of Aurora-A molecular inhibitors are currently underway, and clinical transformation is just around the corner.
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