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MAP4K4 is a Threonine Kinase that Phosphorylates FARP1

机译:MAP4K4是磷酸化Farp1的苏氨酸激酶

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Mitogen-activated protein kinase 4 (MAP4K4) regulates the MEK kinase cascade and governs cytoskeletal rearrangement, however identifying MAP4K4 substrates has remained a challenge. To ascertain MAP4K4-dependent phosphorylation events, we combined phosphoproteomic studies of MAP4K4 inhibition with in vitro assessment of its kinase specificity. We identified 235 phosphosites affected by MAP4K4 inhibition in cells and found that pTP and pSP motifs were predominant amongst them. In contrast, in vitro assessment of kinase specificity showed that MAP4K4 favors a pTL motif. We showed that MAP4K4 directly phosphorylates and coimmunoprecipitates with FERM, RhoGEF and pleckstrin domain-containing protein 1 (FARP1). MAP4K4 inhibition in SH-SY5Y cells increases neurite outgrowth, a process known to involve FARP1. As FARP1 and MAP4K4 both contribute to cytoskeletal rearrangement, the results suggest that MAP4K4 exerts some of its effects on the cytoskeleton via phosphorylation of FARP1.
机译:丝裂原激活的蛋白激酶4(MAP4K4)调节MEK激酶级联并治理细胞骨骼重排,然而识别MAP4K4基材仍然是挑战。为了确定MAP4K4依赖性磷酸化事件,我们将MAP4K4抑制的磷蛋白酶研究与其激酶特异性的体外评估组合。我们鉴定了由MAP4K4在细胞中影响的335种磷酸水,发现PTP和PSP基序在它们之间是主要的。相反,对激酶特异性的体外评估表明,MAP4K4有利于PTL基序。我们展示MAP4K4直接用FERM,RHOGEF和PLeckstrin结构域蛋白1(Farp1)直接磷酸化和携带含有Fermunoplectates。 MAP4K4在SH-SY5Y细胞中的抑制增加了神经突的过度,一种涉及FARP1的过程。由于Farp1和Map4k4都有助于细胞骨架重排,结果表明MAP4K4通过Farp1的磷酸化对其对细胞骨架的一些影响。

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