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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Solid-state (2)H and (15)N NMR studies of side-chain and backbone dynamics of phospholamban in lipid bilayers: investigation of the N27A mutation.
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Solid-state (2)H and (15)N NMR studies of side-chain and backbone dynamics of phospholamban in lipid bilayers: investigation of the N27A mutation.

机译:固态(2)H和(15)N NMR研究脂质双层中磷脂酰肌醇的侧链和主链动力学:N27A突变的研究。

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摘要

Phospholamban (PLB) is an integral membrane protein regulating Ca(2+) transport through inhibitory interaction with sarco(endo)plasmic reticulum calcium ATPase (SERCA). The Asn27 to Ala (N27A) mutation of PLB has been shown to function as a superinhibitor of the affinity of SERCA for Ca(2+) and of cardiac contractility in vivo. The effects of this N27A mutation on the side-chain and backbone dynamics of PLB were investigated with (2)H and (15)N solid-state NMR spectroscopy in phospholipid multilamellar vesicles (MLVs). (2)H and (15)N NMR spectra indicate that the N27A mutation does not significantly change the side-chain or backbone dynamics of the transmembrane and cytoplasmic domains when compared to wild-type PLB. However, dynamic changes are observed for the hinge region, in which greater mobility is observed for the CD(3)-labeled Ala24 N27A-PLB. The increased dynamics in the hinge region of PLB upon N27A mutation may allow the cytoplasmic helix to more easily interact with the Ca(2+)-ATPase; thus, showing increased inhibition of Ca(2+)-ATPase.
机译:Phospholamban(PLB)是通过与肌(内)质网钙ATPase(SERCA)的抑制性相互作用调节Ca(2+)转运的完整膜蛋白。 PLB的Asn27至Ala(N27A)突变已显示出可作为SERCA对Ca(2+)的亲和力和体内心脏收缩力的超级抑制剂。使用磷脂多层囊泡(MLV)中的(2)H和(15)N固态NMR光谱研究了此N27A突变对PLB的侧链和主链动力学的影响。 (2)H和(15)N NMR光谱表明,与野生型PLB相比,N27A突变不会显着改变跨膜和胞质域的侧链或主链动力学。但是,动态变化观察到的铰链区域,其中CD(3)标记的Ala24 N27A-PLB观察到更大的迁移率。 N27A突变后,PLB的铰链区动力学的增加可能使胞质螺旋更容易与Ca(2 +)-ATPase相互作用;因此,显示出增加的Ca(2 +)-ATPase抑制作用。

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