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Localization and retention of p90 ribosomal S6 kinase 1 in the nucleus: implications for its function

机译:p90核糖体S6激酶1在细胞核中的定位和保留:对其功能的影响

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Ribosomal S6 kinase 1 (RSK1) belongs to a family of proteins with two kinase domains. Following activation in the cytoplasm by extracellular signal-regulated kinases (ERK1/2), it mediates the cell-proliferative, cell-growth, and survival-promoting actions of a number of growth factors and other agonists. These diverse biological actions of RSK1 involve regulation of both cytoplasmic and nuclear events. However, the mechanisms that permit nuclear accumulation of RSK1 remain unknown. Here, we show that phosphorylation of RSK1 on S221 is important for its dissociation from the type Iα regulatory subunit of protein kinase A (PKA) in the cytoplasm and that RSK1 contains a bipartite nuclear localization sequence that is necessary for its nuclear entry. Once inside, the active RSK1 is retained in the nucleus via its interactions with PKA catalytic subunit and AKAP95. Mutations of RSK1 that do not affect its activity but disrupt its entry into the nucleus or expression of AKAP95 forms that do not enter the nucleus inhibit the ability of active RSK1 to stimulate DNA synthesis. Our findings identify novel mechanisms by which active RSK1 accumulates in the nucleus and also provide new insights into how AKAP95 orchestrates cell cycle progression.
机译:核糖体S6激酶1(RSK1)属于具有两个激酶结构域的蛋白质家族。通过细胞外信号调节激酶(ERK1 / 2)在细胞质中激活后,它介导许多生长因子和其他激动剂的细胞增殖,细胞生长和存活促进作用。 RSK1的这些多样的生物学作用涉及细胞质和核事件的调节。但是,允许RSK1核积累的机制仍然未知。在这里,我们显示S221上的RSK1磷酸化对于其与细胞质中蛋白激酶A(PKA)的Iα型调节亚基的解离非常重要,并且RSK1包含其核进入所必需的两部分核定位序列。进入内部后,活性RSK1通过与PKA催化亚基和AKAP95的相互作用而保留在细胞核中。 RSK1突变不会影响其活性,但会破坏其进入细胞核或不进入细胞核的AKAP95形式的表达,会抑制活性RSK1刺激DNA合成的能力。我们的发现确定了活性RSK1在细胞核中积累的新机制,也为AKAP95如何协调细胞周期进程提供了新见解。

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