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作 者:李彦萍[1] 苏雅娴 林克椿[1] 张煦[1] 翁诗甫[1] 许振华[1]
出 处:《生物物理学报》1995年第4期490-496,共7页Acta Biophysica Sinica
基 金:国家自然科学基金
摘 要:用FTIR光谱研究了短杆菌肽A(GA)在固态,组装入DPPC脂持体,以及Na+结合状态的构象变化。固态时酰胺Ⅰ带峰位于163cm-1左右,且在1685cm-1处有一肩峰;酰胺Ⅱ带位于1530cm1左右,整个分子为反平行的β螺旋结构,为非通道构象。当GA组装入脂质体后,酰胺Ⅰ带仍位于1633cm-1,但1685cm-1的肩峰消失,酰胺Ⅱ带移至1550cm-1,分子间氢键转变为分子内氢键,二聚体从原来的双股螺旋变为头-头相连的单股螺旋,是GA的膜内通道构象。Na+的结合并不改变GA的骨架结构,但通过对酰胺Ⅰ带的拟合分析发现:加Na+后位于1644cm-1的无规结构含量减少10%,而有序结构增加,提示部分无视结构可能有一种“门”的作用:当无离子通过时为“关闭”状态,当与离子结合后即“打开”,这样通过构象的改变来实现其通道功能。FTIR was used to examine the seconda ry structural changes of GA in solid state,phospholipid bilayer and in the presence of sodium cation. In solid state a strong amide Iband Was observed at-1630cm-1 accompanied by a shoulder at-1685cm-1. Thestrongest amide Ⅱ band was at-1530cm-1. The predominant structure of GA was doub le-stranded anti-panalle helix. This is the non-channal conformation of GA. Thereconstitution of GA in DPPC did not change its 1633cm-1 band but the shoulder at1685cm-1 disappeared. The amide Ⅱ band also shifted to 1550cm-1. These data suggestedthat GA had undertaken a conformational change: from the double-stranded β helix to asingle-stranded β helix consisting of the head-to-head dimer. This is the channel.conformation of GA. Binding of Na+ to the GA channel did not change the main βbelical conformtion in the hydrophobic area. But a ed-quantitative analysis indicated thatthe unordered structure of the peptide decreased from 22% to 11% in the presence of Na+.The result suggested that the sodium binding caused a partial change in the unordered structure, which probably acts as a " door" of the GA channel. The "door" is "closed"when there is no ion binding but can be "opened" by adding of Na+.
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