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与嗜酸乳杆菌R-26的脱氧腺苷激酶异源激活有关的顺式活性Ras G2样序列。

cis-Active Ras G2-like sequence implicated in the heterotropic activation of the deoxyadenosine kinase of Lactobacillus acidophilus R-26.

作者信息

Guo S, Ma N, Ives D H

机构信息

Department of Biochemistry, The Ohio State University, Columbus, Ohio 43210-1292, USA.

出版信息

J Biol Chem. 1997 Mar 14;272(11):6890-7. doi: 10.1074/jbc.272.11.6890.

Abstract

Deoxyadenosine kinase (dAK) forms a heterodimer with either deoxyguanosine kinase (dGK) or deoxycytidine kinase (dCK), and is heterotropically activated 3-5 times by dGuo or dCyd. Expressed alone, dAK is inactive and exhibits no response to dGuo or dCyd; activity and heterotropic response are fully restored upon reassociation with dGK or dCK. However, turnover of independently expressed dGK or dCK is nearly maximal, being further activated only 50-100% upon reassociation with dAK. In neither case is the heterotropic activation due to ligand-induced heterodimer formation. A proline/alanine substitution within a dAK segment homologous to loop G2 of Ras proteins yielded a heterodimer with dAK permanently cis-activated 2-fold, with a corresponding reduction in heterotropic activation by dGuo. A chimeric dAK, with 25% of its C terminus substituted by the homologous sequence from dGK, was inactive alone, and its characteristics were unchanged in the reconstituted heterodimer. Superimposing the Pro/Ala substitution on this chimera also reduced heterotropic activation by half. Cross-linking the dimer by 1,5-difluoro-2,4-dinitrobenzene was inhibited by ATP, dATP, dGTP, and dAdo, suggesting the proximity of the active site(s) to the interface. These data suggest that dAK depends on dGK or dCK in a manner resembling the reliance of Ras upon GTPase activating protein.

摘要

脱氧腺苷激酶(dAK)与脱氧鸟苷激酶(dGK)或脱氧胞苷激酶(dCK)形成异源二聚体,并被dGuo或dCyd异向激活3至5倍。单独表达时,dAK无活性,对dGuo或dCyd无反应;与dGK或dCK重新结合后,活性和异向反应完全恢复。然而,独立表达的dGK或dCK的周转率几乎达到最大值,与dAK重新结合后仅进一步激活50%至100%。在这两种情况下,异向激活都不是由于配体诱导的异源二聚体形成。在与Ras蛋白的环G2同源的dAK片段内的脯氨酸/丙氨酸取代产生了一种异源二聚体,其中dAK永久顺式激活2倍,同时dGuo的异向激活相应降低。一种嵌合dAK,其C末端的25%被来自dGK的同源序列取代,单独时无活性,在重组异源二聚体中其特性不变。在这种嵌合体上叠加脯氨酸/丙氨酸取代也使异向激活降低了一半。1,5-二氟-2,4-二硝基苯对二聚体的交联被ATP、dATP、dGTP和dAdo抑制,表明活性位点靠近界面。这些数据表明,dAK对dGK或dCK的依赖方式类似于Ras对GTP酶激活蛋白的依赖。

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