Lassila Jonathan Kyle, Privett Heidi K, Allen Benjamin D, Mayo Stephen L
Biochemistry and Molecular Biophysics Option, Division of Chemistry and Chemical Engineering, California Institute of Technology, Pasadena, CA 91125, USA.
Proc Natl Acad Sci U S A. 2006 Nov 7;103(45):16710-5. doi: 10.1073/pnas.0607691103. Epub 2006 Oct 30.
The incorporation of small-molecule transition state structures into protein design calculations poses special challenges because of the need to represent the added translational, rotational, and conformational freedoms within an already difficult optimization problem. Successful approaches to computational enzyme design have focused on catalytic side-chain contacts to guide placement of small molecules in active sites. We describe a process for modeling small molecules in enzyme design calculations that extends previously described methods, allowing favorable small-molecule positions and conformations to be explored simultaneously with sequence optimization. Because all current computational enzyme design methods rely heavily on sampling of possible active site geometries from discrete conformational states, we tested the effects of discretization parameters on calculation results. Rotational and translational step sizes as well as side-chain library types were varied in a series of computational tests designed to identify native-like binding contacts in three natural systems. We find that conformational parameters, especially the type of rotamer library used, significantly affect the ability of design calculations to recover native binding-site geometries. We describe the construction and use of a crystallographic conformer library and find that it more reliably captures active-site geometries than traditional rotamer libraries in the systems tested.
将小分子过渡态结构纳入蛋白质设计计算带来了特殊挑战,因为在一个本就困难的优化问题中需要表示额外的平移、旋转和构象自由度。计算酶设计的成功方法集中在催化侧链接触上,以指导小分子在活性位点的放置。我们描述了一种在酶设计计算中对小分子进行建模的过程,该过程扩展了先前描述的方法,允许在序列优化的同时探索有利的小分子位置和构象。由于所有当前的计算酶设计方法都严重依赖于从离散构象状态对可能的活性位点几何结构进行采样,我们测试了离散化参数对计算结果的影响。在一系列旨在识别三个天然系统中类似天然结合接触的计算测试中,改变了旋转和平移步长以及侧链库类型。我们发现构象参数,尤其是所使用的旋转异构体库的类型,显著影响设计计算恢复天然结合位点几何结构的能力。我们描述了晶体构象异构体库的构建和使用,并发现它比测试系统中的传统旋转异构体库更可靠地捕捉活性位点几何结构。