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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >(15)N Solid-state NMR spectroscopic studies on phospholamban at its phosphorylated form at Ser-16 in aligned phospholipid bilayers.
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(15)N Solid-state NMR spectroscopic studies on phospholamban at its phosphorylated form at Ser-16 in aligned phospholipid bilayers.

机译:(15)N固态NMR光谱研究在对准的磷脂双层中以Ser-16磷酸化形式的磷lamban。

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Wild-type phospholamban (WT-PLB) is a pentameric transmembrane protein that regulates the cardiac cycle (contraction and relaxation). From a physiological prospective, unphosphorylated WT-PLB inhibits sarcoplasmic reticulum ATPase activity; whereas, its phosphorylated form relieves the inhibition in a mechanism that is not completely understood. In this study, site-specifically (15)N-Ala-11- and (15)N-Leu-7-labeled WT-PLB and the corresponding phosphorylated forms (P-PLB) were incorporated into 1,2-dioleoyl-sn-glycero-3-phosphocholine/2-dioleoyl-sn-glycero-3-phosphoethanolam ine (DOPC/DOPE) mechanically oriented lipid bilayers. The aligned (15)N-labeled Ala-11 and Leu-7 WT-PLB samples show (15)N resonance peaks at approximately 71ppm and 75ppm, respectively, while the corresponding phosphorylated forms P-PLB show (15)N peaks at 92ppm and 99ppm, respectively. These (15)N chemical shift changes upon phosphorylation are significant and in agreement with previous reports, which indicate that phosphorylation of WT-PLB at Ser-16 alters the structural properties of the cytoplasmic domain with respect to the lipid bilayers.
机译:野生型磷酸lamban(WT-PLB)是一种五聚体跨膜蛋白,可调节心脏周期(收缩和舒张)。从生理学角度来看,未磷酸化的WT-PLB抑制了肌质网ATPase的活性;然而,其磷酸化形式以一种尚不完全了解的机制减轻了抑制作用。在这项研究中,将位点特异性(15)N-Ala-11-和(15)N-Leu-7标记的WT-PLB及其相应的磷酸化形式(P-PLB)掺入1,2-二油酰基-sn中-甘油-3-磷酸胆碱/ 2-油酰基-sn-甘油-3-磷酸乙醇胺(DOPC / DOPE)机械定向的脂质双层。对齐的(15)N标记的Ala-11和Leu-7 WT-PLB样品分别在大约71ppm和75ppm处显示(15)N共振峰,而相应的磷酸化形式P-PLB在92ppm处显示(15)N峰。和99ppm。这些(15)N化学位移在磷酸化时的变化是显着的,并且与先前的报道一致,这表明WT-PLB在Ser-16上的磷酸化改变了相对于脂质双层的细胞质结构域的结构性质。

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