Lee K H, Benson D R, Kuczera K
Department of Chemistry, University of Kansas, 2010 Malott Hall, Lawrence, Kansas 66045, USA.
Biochemistry. 2000 Nov 14;39(45):13737-47. doi: 10.1021/bi001126b.
Molecular dynamics simulations were carried out for three 13-residue peptides of the form AcNH-A-A-E-X-A-E-A-H-A-A-E-K-A-CONH(2) with X = A, F, and W. All three peptides exhibited unexpected dynamical behavior, undergoing a transition from an alpha-helical to a pi-helical structure in the course of 5-ns trajectories in aqueous solution. Analysis of peptide length, accessible surface, interaction energies, hydrogen bonding, and dihedral angles was consistent with alpha --> pi transitions at 2800, 500, and 800 ps for X = A, F and W, respectively. The transitions occurred sequentially and cooperatively, propagating from the C- to the N-terminus for X = A and W and from the center toward both termini for X = F. The time scale of the overall transition ranged from 300 to 500 ps. For all three peptides the backbone structural transition was accompanied by a concerted rearrangement of the charged side chains, including a 3 A increase in the distance between carboxylate groups of Glu-3 and Glu-6. During the transition the peptide backbone hydrogen-bonding patterns were disrupted at the interface between the alpha-helical and nascent pi-helical regions, with peptide groups forming water-bridged hydrogen bonds. The peptide structures exhibited significant fluidity, with individual residues sampling alpha-, pi-, and 3(10)-helical conformations, as well as a "coil" state, without any intramolecular hydrogen bonds. The studied peptides have been designed to form alpha-helices when incorporated in novel hemoprotein model compounds, peptide-sandwiched mesohemes, which consist of two identical peptides covalently attached to an Fe(III) mesoporphyrin [Liu, D., Williamson, D. A., Kennedy, M. L., Williams, T. D., Morton, M. M., and Benson, D. R. (1999) J. Am. Chem. Soc. 121, 11798-11812]. The possibility of adopting pi-helical structures by the constituent peptides may influence the properties of the hemoprotein models.
对三种形式为AcNH-A-A-E-X-A-E-A-H-A-A-E-K-A-CONH(2)的13残基肽进行了分子动力学模拟,其中X = A、F和W。所有这三种肽都表现出意想不到的动力学行为,在水溶液中5纳秒的轨迹过程中从α-螺旋结构转变为π-螺旋结构。对肽长度、可及表面积、相互作用能、氢键和二面角的分析与X分别为A、F和W时在2800、500和800皮秒发生的α→π转变一致。转变依次协同发生,对于X = A和W从C端向N端传播,对于X = F从中心向两端传播。整体转变的时间尺度为300至500皮秒。对于所有这三种肽,主链结构转变伴随着带电侧链的协同重排,包括Glu-3和Glu-6的羧基之间的距离增加3埃。在转变过程中,肽主链的氢键模式在α-螺旋和新生π-螺旋区域之间的界面处被破坏,肽基团形成水桥氢键。肽结构表现出显著的流动性,单个残基呈现α-、π-和3(10)-螺旋构象以及“卷曲”状态,没有任何分子内氢键。所研究的肽被设计成在掺入新型血红蛋白模型化合物(肽夹合的中卟啉)时形成α-螺旋,该化合物由两个共价连接到Fe(III)中卟啉的相同肽组成[刘,D.,威廉姆森,D. A.,肯尼迪,M. L.,威廉姆斯,T. D.,莫顿,M. M.,和本森,D. R. (1999) J. Am. Chem. Soc. 121, 11,798 - 11,812]。组成肽采用π-螺旋结构的可能性可能会影响血红蛋白模型的性质。
