Franklin Joel, Koehl Patrice, Doniach Sebastian, Delarue Marc
Department of Physics, Reed College, Portland, OR 97202, USA.
Nucleic Acids Res. 2007 Jul;35(Web Server issue):W477-82. doi: 10.1093/nar/gkm342. Epub 2007 Jun 1.
The non-linear problem of simulating the structural transition between two known forms of a macromolecule still remains a challenge in structural biology. The problem is usually addressed in an approximate way using 'morphing' techniques, which are linear interpolations of either the Cartesian or the internal coordinates between the initial and end states, followed by energy minimization. Here we describe a web tool that implements a new method to calculate the most probable trajectory that is exact for harmonic potentials; as an illustration of the method, the classical Calpha-based Elastic Network Model (ENM) is used both for the initial and the final states but other variants of the ENM are also possible. The Langevin equation under this potential is solved analytically using the Onsager and Machlup action minimization formalism on each side of the transition, thus replacing the original non-linear problem by a pair of linear differential equations joined by a non-linear boundary matching condition. The crossover between the two multidimensional energy curves around each state is found numerically using an iterative approach, producing the most probable trajectory and fully characterizing the transition state and its energy. Jobs calculating such trajectories can be submitted on-line at: http://lorentz.dynstr.pasteur.fr/joel/index.php.
在结构生物学中,模拟大分子两种已知形式之间的结构转变这一非线性问题仍然是一项挑战。该问题通常使用“变形”技术以近似方式解决,“变形”技术是对初始状态和终态之间的笛卡尔坐标或内部坐标进行线性插值,然后进行能量最小化。在此,我们描述一种网络工具,它实现了一种新方法来计算对于简谐势精确的最可能轨迹;作为该方法的一个示例,初始态和终态均使用基于经典Cα的弹性网络模型(ENM),但ENM的其他变体也是可行的。利用昂萨格和马赫卢普作用最小化形式对转变两侧的该势下的朗之万方程进行解析求解,从而通过一对由非线性边界匹配条件连接的线性微分方程来取代原始的非线性问题。使用迭代方法通过数值计算找到围绕每个状态的两条多维能量曲线之间的交叉点,从而产生最可能轨迹并全面表征过渡态及其能量。计算此类轨迹的任务可在以下网址在线提交:http://lorentz.dynstr.pasteur.fr/joel/index.php 。
