Zhou Ruhong, Huang Xuhui, Margulis Claudio J, Berne Bruce J
Computational Biology Center, IBM Thomas J. Watson Research Center, 1101 Kitchawan Road, Yorktown Heights, NY 10598, USA.
Science. 2004 Sep 10;305(5690):1605-9. doi: 10.1126/science.1101176.
We performed molecular dynamics simulations of the collapse of a two-domain protein, the BphC enzyme, into a globular structure to examine how water molecules mediate hydrophobic collapse of proteins. In the interdomain region, liquid water persists with a density 10 to 15% lower than in the bulk, even at small domain separations. Water depletion and hydrophobic collapse occur on a nanosecond time scale, which is two orders of magnitude slower than that found in the collapse of idealized paraffin-like plates. When the electrostatic protein-water forces are turned off, a dewetting transition occurs in the interdomain region and the collapse speeds up by more than an order of magnitude. When attractive van der Waals forces are turned off as well, the dewetting in the interdomain region is more profound, and the collapse is even faster.
我们对双结构域蛋白BphC酶折叠成球状结构进行了分子动力学模拟,以研究水分子如何介导蛋白质的疏水折叠。在结构域间区域,即使结构域间距很小,液态水依然存在,其密度比本体水低10%至15%。水的耗尽和疏水折叠发生在纳秒时间尺度上,这比理想化的类石蜡板折叠慢两个数量级。当蛋白质与水之间的静电力关闭时,结构域间区域会发生去湿转变,折叠速度加快一个多数量级以上。当吸引性范德华力也关闭时,结构域间区域的去湿更显著,折叠速度更快。