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Fluorescence study on transmembrane Ca2+ gradient-mediated conformation changes of sarcoplasmic reticulum Ca2+-ATPase

机译:跨膜Ca2 +梯度介导的肌浆网C​​a2 + -ATPase构象变化的荧光研究

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摘要

The conformational states of Ca2+-ATPase in sarcoplasmic reticulum (SR) vesicles with or without a thousand-fold transmembrane Ca2+ gradient have been studied by fluorescence spectroscopy and fluorescence quenching. In consequence of the establishment of the transmembrane Ca2+ gradient, the steady-state fluorescence results revealed a reproducible 8% decrease in the intrinsic fluorescence while time-resolved fluorescence measurements showed that 13 tryptophan residues in SR · Ca2+-ATPase could be divided into three groups. The fluorescence lifetime of one of these groups increased from 5.5 ns to 5.95 ns in the presence of a Ca2+ gradient. Using KI and hypocrellin B (a photosensitive pigment obtained from a parasitic fungus, growing in Yunnan, China), the fluorescence quenching further indicated that the dynamic change of this tryptophan group, located at the protein-lipid interface, is a characteristic of transmembrane Ca2+ gradient-mediated conformational changes in SR · Ca2+-ATPase.
机译:通过荧光光谱和荧光猝灭研究了有或无千倍跨膜Ca2 +梯度的肌浆网(SR)囊泡中Ca2 + -ATPase的构象状态。建立跨膜Ca2 +梯度的结果是,稳态荧光结果显示固有荧光降低了8%,而时间分辨荧光测量表明SR·Ca2 + -ATPase中的13个色氨酸残基可分为三类。在存在Ca2 +梯度的情况下,这些组之一的荧光寿命从5.5 ns增加到5.95 ns。使用KI和hypercrellin B(一种从寄生真菌获得的光敏色素,在中国云南生长),荧光猝灭进一步表明,位于蛋白-脂质界面的色氨酸基团的动态变化是跨膜Ca2 +的特征。梯度介导的SR·Ca2 + -ATPase构象变化。

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