Department of Chemistry, Texas A&M University, P.O. Box 30012, College Station, Texas 77843, USA.
J Am Chem Soc. 2011 Nov 23;133(46):18707-12. doi: 10.1021/ja205106e. Epub 2011 Oct 27.
The molecular orientation of trimethylamine N-oxide (TMAO), a powerful protein stabilizer, was explored at aqueous/hydrophobic interfaces using vibrational sum frequency spectroscopy (VSFS). The systems studied included the octadecyltrichlorosilane (OTS)/water interface, which represents an aqueous solution in direct contact with a hydrophobic medium. Surprisingly, the measurements revealed that the methyl groups of TMAO pointed into the aqueous phase and away from the OTS. This orientation may arise from the more hydrophilic nature of methyl groups attached to a strongly electron-withdrawing atom such as a quaternary nitrogen. Additional studies were performed at the air/water interface. This interface showed a high degree of TMAO alignment, but the dangling OH from water was present even at 5 M TAMO. Moreover, the addition of this osmolyte modestly increased the surface tension of the interface. This meant that this species was somewhat depleted at the interface compared to the bulk solution. These findings may have implications for the stabilizing effect of TMAO on proteins. Specifically, the strong hydration required for the methyl groups as well as the oxide moiety should be responsible for the osmolyte's depletion from hydrophobic/aqueous interfaces. Such depletion effects should help stabilize proteins in their folded and native conformations on entropic grounds, although orientational effects may play an additional role.
采用振动和频光谱(VSFS)技术研究了三甲基氧化胺(TMAO)在水/疏水性界面处的分子取向,TMAO 是一种强大的蛋白质稳定剂。研究的体系包括十八烷基三氯硅烷(OTS)/水界面,它代表了直接与疏水性介质接触的水溶液。令人惊讶的是,测量结果表明 TMAO 的甲基基团指向水相,远离 OTS。这种取向可能源于与强吸电子原子(如季氮)相连的甲基基团具有更高的亲水性。在空气/水界面也进行了进一步的研究。该界面显示出高度的 TMAO 取向,但即使在 5 M TAMO 时,水中的悬挂 OH 仍然存在。此外,这种渗透物的添加适度增加了界面的表面张力。这意味着与本体溶液相比,该物质在界面处略有消耗。这些发现可能对 TMAO 对蛋白质的稳定作用具有启示意义。具体来说,甲基基团以及氧化物部分所需的强烈水合作用应负责从疏水性/水界面消耗渗透物。这种消耗效应应该有助于在熵的基础上稳定蛋白质的折叠和天然构象,尽管取向效应可能会发挥额外的作用。
