Karle I L
Biopolymers. 1989 Jan;28(1):1-14. doi: 10.1002/bip.360280104.
Preferred conformation and types of molecular folding are some of the topics that can be addressed by structure analysis using x-ray diffraction of single crystals. The conformations of small linear peptide molecules with 2-6 residues are affected by polarity of solvent, presence of water molecules, hydrogen bonding with neighboring molecules, and other packing forces. Larger peptides, both cyclic and linear, have many intramolecular hydrogen bonds, the effect of which outweighs any intermolecular attractions. Numerous polymorphs of decapeptides grown from a variety of solvents, with different cocrystallized solvents, show a constant conformation for each peptide. Large conformational changes occur, however, upon complexation with metal ions. A new form of free valinomycin grown from DMSO exhibits near three-fold symmetry with only three intramolecular hydrogen bonds. The peptide is in the form of a shallow bowl with a hydrophobic exterior. Near the bottom of the interior of the bowl are three carbonyl oxygens, spaced and directed so that they are in position to form three ligands to a K+, e.g., complexation can be completed by the three lobes containing the beta-bends closing over and encapsulating the K+ ion. In another example, free antamanide and the biologically inactive perhydro analogue, in which four phenyl groups become cyclic hexyl groups, have essentially the same folding of backbone and side chains. The conformation changes drastically upon complexation with Li+ or Na+. However, the metal ion complex of natural antamanide has a hydrophobic globlar form whereas the metal ion complex of the inactive perhydro analogue has a polar band around the middle. The structure results indicate that the antamanide molecule is in a complexed form during its biological activity. Single crystal x-ray diffraction structure analyses have identified the manner in which water molecules are essential to creating minipolar areas on apolar helices. Completely apolar peptides, such as membrane-active peptides, can acquire amphiphilic character by insertion of a water molecule into the helical backbone of Boc-Aib-Ala-Leu-Aib-Ala-Leu-Aib-Ala-Leu-Aib-OMe, for example. The C-terminal half assumes an alpha-helix conformation, whereas the N-terminal half is distorted by an insertion of a water molecule W(1) between N(Ala5) and O(Ala2), forming hydrogen bonds N(5)H...W(1) and W(1)...O(2). The distortion of the helix exposes C = O(Aib1) and C = O(Aib4) to the outside environment with the consequence of attracting additional water molecules. The leucyl side chains are on the other side of the molecule. Thus a helix with an apolar sequence can mimic an amphiphilic helix.
优选的构象和分子折叠类型是可以通过使用单晶X射线衍射进行结构分析来解决的一些主题。具有2至6个残基的小线性肽分子的构象受溶剂极性、水分子的存在、与相邻分子的氢键以及其他堆积力的影响。较大的肽,包括环状和线性的,具有许多分子内氢键,其作用超过任何分子间吸引力。从多种溶剂中生长出来的、带有不同共结晶溶剂的十肽的众多多晶型物,对于每种肽都显示出恒定的构象。然而,与金属离子络合时会发生大的构象变化。从二甲基亚砜中生长出来的游离缬氨霉素的一种新形式表现出近乎三重对称性,只有三个分子内氢键。该肽呈浅碗状,外部具有疏水性。在碗内部底部附近有三个羰基氧,其间隔和方向使得它们能够形成与钾离子的三个配体,例如,络合可以通过包含β-转角的三个叶瓣闭合并包裹钾离子来完成。在另一个例子中,游离的抗霉素A和生物无活性的全氢类似物,其中四个苯基变成环状己基,其主链和侧链的折叠基本相同。与锂离子或钠离子络合时构象会发生剧烈变化。然而,天然抗霉素A的金属离子络合物具有疏水性球状形式,而无活性全氢类似物的金属离子络合物在中间有一个极性带。结构结果表明,抗霉素A分子在其生物活性期间处于络合形式。单晶X射线衍射结构分析已经确定了水分子对于在非极性螺旋上形成微极性区域至关重要的方式。例如,完全非极性的肽,如膜活性肽,可以通过将一个水分子插入到Boc-Aib-Ala-Leu-Aib-Ala-Leu-Aib-Ala-Leu-Aib-OMe的螺旋主链中来获得两亲性特征。C端的一半呈现α-螺旋构象,而N端的一半由于在N(Ala5)和O(Ala2)之间插入一个水分子W(1)而发生扭曲,形成氢键N(5)H...W(1)和W(···)O(2)。螺旋的扭曲使C = O(Aib1)和C = O(Aib4)暴露于外部环境,结果吸引了额外的水分子。亮氨酰侧链在分子的另一侧。因此,具有非极性序列的螺旋可以模拟两亲性螺旋。
