Kiss R S, Ryan R O, Hicks L D, Oikawa K, Kay C M
Department of Biochemistry, University of Alberta, Edmonton, Canada.
Biochemistry. 1993 Aug 10;32(31):7872-8. doi: 10.1021/bi00082a006.
The amphipathic alpha-helices of exchangeable apolipoproteins (apo) function to simultaneously facilitate interaction with lipid surfaces and the aqueous environment. In contrast to mammalian apoA-I's, which self-associate in the absence of lipid, chicken apoA-I, which shares 66% sequence homology with human apoA-I, exists as a monomeric protein when dissociated from high-density lipoprotein (HDL). Sedimentation equilibrium studies conducted in the analytical ultracentrifuge yielded a weight-average molecular weight of 28,170. Corresponding sedimentation velocity and diffusion experiments gave rise to s0(20,w) = 2.23 S and D0(20,w) = 6.39 x 10(-7) cm2/s. A translational frictional ratio (f/fmin) of 1.18 and an axial ratio of 4.0 were also determined from this data. The Stokes radius (Rs,sed = 2.80 nm) and translational frictional ratio were subsequently used to calculate estimated molecular dimensions of 25.2 x 100.8 A for chicken apoA-I. Circular dichroism (CD) studies revealed a highly alpha-helical structure predicted to be 74% by Provencher-Glöckner analysis. Denaturation studies performed on lipid-free apoA-I and monitored by CD revealed a midpoint of denaturation of 0.64 M guanidine hydrochloride. From plots of delta G(app) versus guanidine hydrochloride concentration, a delta GDH2O of 1.86 kcal/mol was determined. In other studies, a midpoint of temperature-induced denaturation for apoA-I of 57 degrees C was obtained. The effect of solvent pH on the secondary structure content of apoA-I revealed a significant loss of alpha-helix below pH 4.0 and above pH 10, suggesting that lipid-free apoA-I may by partially stabilized by the formation of intra- or interhelix salt bridges between oppositely charged amino acid side chains.(ABSTRACT TRUNCATED AT 250 WORDS)
可交换载脂蛋白(apo)的两亲性α-螺旋具有同时促进与脂质表面和水性环境相互作用的功能。与在无脂质时会自我缔合的哺乳动物载脂蛋白A-I不同,与人载脂蛋白A-I具有66%序列同源性的鸡载脂蛋白A-I,从高密度脂蛋白(HDL)解离后以单体蛋白形式存在。在分析超速离心机中进行的沉降平衡研究得出重均分子量为28,170。相应的沉降速度和扩散实验得出s0(20,w) = 2.23 S和D0(20,w) = 6.39×10(-7) cm2/s。还根据该数据确定了平移摩擦比(f/fmin)为1.18,轴比为4.0。斯托克斯半径(Rs,sed = 2.80 nm)和平移摩擦比随后用于计算鸡载脂蛋白A-I的估计分子尺寸为25.2×100.8 Å。圆二色性(CD)研究表明,通过普罗文彻 - 格洛克纳分析预测其具有高度α-螺旋结构,占比74%。对无脂质载脂蛋白A-I进行的变性研究并通过CD监测,得出变性中点为0.64 M盐酸胍。根据ΔG(app)与盐酸胍浓度的关系图,确定ΔGDH2O为1.86 kcal/mol。在其他研究中,获得了载脂蛋白A-I温度诱导变性的中点为57℃。溶剂pH对载脂蛋白A-I二级结构含量的影响表明,在pH 4.0以下和pH 10以上α-螺旋显著丧失,这表明无脂质载脂蛋白A-I可能通过相反电荷氨基酸侧链之间形成的螺旋内或螺旋间盐桥而部分稳定。(摘要截断于250字)
