Friedrich Miescher Institute for Biomedical Research, Basel, Switzerland.
Cell Cycle. 2011 Jun 15;10(12):1897-904. doi: 10.4161/cc.10.12.15826.
The mammalian genome encodes four members of the NDR/LATS kinase family: NDR1 (STK38), NDR2 (STK38L), LATS1 and LATS2, which are highly conserved from yeast to man. Members of the NDR/LATS kinase family have been implicated in a variety of biological processes ranging from cell division and morphology to apoptosis and tumor suppression. In mammals, LATS1/2 function as central parts of the HIPPO tumor suppressor pathway by restricting the activity of the YAP/TAZ proto-oncogenes. Recent evidence suggested that NDR1/2 are also part of an extended HIPPO tumor suppressor pathway. Apart from functions in apoptosis signaling and tumor suppression, NDR1/2 have been implicated in controlling centrosome duplication and mitotic chromosome alignment downstream of the HIPPO kinase homologs MST1 and MST2. Significantly, we also reported recently that NDR1/2 are controlling G 1/S transition downstream of a third MST family member MST3. Intriguingly, this newly described MST3-NDR1/2 axis promotes G 1 progression by stabilizing c-myc and preventing p21 accumulation, indicating a potential pro-tumorigenic role for NDR kinases. Here, we discuss these novel cell cycle functions of NDR kinases in a broader context and elaborate on possible explanations for the opposing functions of NDR kinases in normal and tumor biology.
哺乳动物基因组编码四个 NDR/LATS 激酶家族成员:NDR1(STK38)、NDR2(STK38L)、LATS1 和 LATS2,它们从酵母到人高度保守。NDR/LATS 激酶家族成员参与了从细胞分裂和形态到细胞凋亡和肿瘤抑制的各种生物学过程。在哺乳动物中,LATS1/2 通过限制 YAP/TAZ 原癌基因的活性,作为 HIPPO 肿瘤抑制途径的核心部分发挥作用。最近的证据表明,NDR1/2 也是扩展的 HIPPO 肿瘤抑制途径的一部分。除了在细胞凋亡信号和肿瘤抑制中的功能外,NDR1/2 还被认为控制着有丝分裂中心体复制和着丝粒染色体的排列,这是 HIPPO 激酶同源物 MST1 和 MST2 的下游作用。值得注意的是,我们最近还报道,NDR1/2 控制着第三个 MST 家族成员 MST3 的下游 G1/S 过渡。有趣的是,这个新描述的 MST3-NDR1/2 轴通过稳定 c-myc 和防止 p21 积累来促进 G1 期进展,表明 NDR 激酶具有潜在的促肿瘤作用。在这里,我们在更广泛的背景下讨论了 NDR 激酶的这些新的细胞周期功能,并详细阐述了 NDR 激酶在正常和肿瘤生物学中相反功能的可能解释。
