During oncogenesis,the hyper-activation of proto-oncogenes and defection of tumor suppressor genes(Zhao et al.,2012,2016a)can regulate cell proliferation,differentiation,apoptosis,and cell-to-cell communication(Bal...During oncogenesis,the hyper-activation of proto-oncogenes and defection of tumor suppressor genes(Zhao et al.,2012,2016a)can regulate cell proliferation,differentiation,apoptosis,and cell-to-cell communication(Balmain et al.,2003;Haber and Settleman,2007).Recent evidence has shown that non-coding RNAs, such as microRNAs (miRNAs) (Chen, 2005), and long non- coding RNAs (lncRNAs), can also act as oncogenes to initiate and promote cancer progression.展开更多
文摘During oncogenesis,the hyper-activation of proto-oncogenes and defection of tumor suppressor genes(Zhao et al.,2012,2016a)can regulate cell proliferation,differentiation,apoptosis,and cell-to-cell communication(Balmain et al.,2003;Haber and Settleman,2007).Recent evidence has shown that non-coding RNAs, such as microRNAs (miRNAs) (Chen, 2005), and long non- coding RNAs (lncRNAs), can also act as oncogenes to initiate and promote cancer progression.
