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鞘氨醇激酶相互作用蛋白是一种蛋白激酶 A 锚定蛋白,特异性结合 I 型环腺苷酸依赖的蛋白激酶。

Sphingosine kinase interacting protein is an A-kinase anchoring protein specific for type I cAMP-dependent protein kinase.

机构信息

Biomolecular Mass Spectrometry and Proteomics Group, Bijvoet Center forBiomolecular Research and Utrecht Institute for Pharmaceutical Sciences, Utrecht University, Padualaan 8, 3584 CH, Utrecht, The Netherlands.

出版信息

Chembiochem. 2010 May 3;11(7):963-71. doi: 10.1002/cbic.201000058.

Abstract

The compartmentalization of kinases and phosphatases plays an important role in the specificity of second-messenger-mediated signaling events. Localization of the cAMP-dependent protein kinase is mediated by interaction of its regulatory subunit (PKA-R) with the versatile family of A-kinase-anchoring proteins (AKAPs). Most AKAPs bind avidly to PKA-RII, while some have dual specificity for both PKA-RI and PKA-RII; however, no mammalian PKA-RI-specific AKAPs have thus far been assigned. This has mainly been attributed to the observation that PKA-RI is more cytosolic than the more heavily compartmentalized PKA-RII. Chemical proteomics screens of the cAMP interactome in mammalian heart tissue recently identified sphingosine kinase type 1-interacting protein (SKIP, SPHKAP) as a putative novel AKAP. Biochemical characterization now shows that SPHKAP can be considered as the first mammalian AKAP that preferentially binds to PKA-RIalpha. Recombinant human SPHKAP functions as an RI-specific AKAP that utilizes the characteristic AKAP amphipathic helix for interaction. Further chemical proteomic screening utilizing differential binding characteristics of specific cAMP resins confirms SPHKAPs endogenous specificity for PKA-RI directly in mammalian heart and spleen tissue. Immunolocalization studies revealed that recombinant SPHKAP is expressed in the cytoplasm, where PKA-RIalpha also mainly resides. Alignment of SPHKAPs' amphipathic helix with peptide models of PKA-RI- or PKA-RII-specific anchoring domains shows that it has largely only PKA-RIalpha characteristics. Being the first mammalian PKA-RI-specific AKAP with cytosolic localization, SPHKAP is a very promising model for studying the function of the less explored cytosolic PKA-RI signaling nodes.

摘要

激酶和磷酸酶的区室化在第二信使介导的信号转导事件的特异性中发挥重要作用。cAMP 依赖性蛋白激酶的定位是通过其调节亚基(PKA-R)与多功能 AKAP 的相互作用介导的。大多数 AKAP 与 PKA-RII 结合紧密,而有些 AKAP 对 PKA-RI 和 PKA-RII 具有双重特异性;然而,迄今为止尚未指定哺乳动物 PKA-RI 特异性 AKAP。这主要归因于观察到 PKA-RI 比更具区室化的 PKA-RII 更多位于细胞质中。最近,对哺乳动物心脏组织中 cAMP 相互作用组的化学蛋白质组学筛选鉴定出鞘氨醇激酶 1 相互作用蛋白(SKIP,SPHKAP)作为一种潜在的新型 AKAP。生化特征现在表明,SPHKAP 可以被认为是第一个优先与 PKA-RIalpha 结合的哺乳动物 AKAP。重组人 SPHKAP 作为 RI 特异性 AKAP 起作用,利用特征性 AKAP 两亲性螺旋进行相互作用。利用特定 cAMP 树脂的差异结合特性进行进一步的化学蛋白质组筛选,直接在哺乳动物心脏和脾脏组织中证实了 SPHKAP 的内源性 PKA-RI 特异性。免疫定位研究表明,重组 SPHKAP 在细胞质中表达,PKA-RIalpha 也主要位于细胞质中。SPHKAP 的两亲性螺旋与 PKA-RI 或 PKA-RII 特异性锚定结构域的肽模型的比对表明,它主要具有 PKA-RIalpha 特征。作为第一个具有细胞质定位的哺乳动物 PKA-RI 特异性 AKAP,SPHKAP 是研究较少探索的细胞质 PKA-RI 信号节点功能的非常有前途的模型。

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