Department of Materials and Interfaces, Weizmann Institute of Science, Rehovot 76100, Israel.
Proc Natl Acad Sci U S A. 2013 Jan 8;110(2):507-12. doi: 10.1073/pnas.1210457110. Epub 2012 Dec 24.
Measuring solid-state electron transport (ETp) across proteins allows studying electron transfer (ET) mechanism(s), while minimizing solvation effects on the process. ETp is, however, sensitive to any static (conformational) or dynamic (vibrational) changes in the protein. Our macroscopic measurements allow extending ETp studies to low temperatures, with the concomitant resolution of lower current densities, because of the larger electrode contact areas. Thus, earlier we reported temperature-independent ETp via the copper protein azurin (Az), from 80 K until denaturation, whereas for apo-Az ETp was temperature dependent above 180 K. Deuteration (H/D substitution) may provide mechanistic information on the question of whether the ETp involves H-bonds in the solid state. Here we report results of kinetic deuterium isotope effect (KIE) measurements on ETp through holo-Az as a function of temperature (30-340 K). Strikingly, deuteration changed ETp from temperature independent to temperature dependent above 180 K. This H/D effect is expressed in KIE values between 1.8 (340 K) and 9.1 (≤ 180 K). These values are remarkable in light of the previously reported inverse KIE on ET in Az in solution. We ascribe the difference between our KIE results and those observed in solution to the dominance of solvent effects in the latter (larger thermal expansion in H(2)O than in D(2)O), whereas in our case the KIE is primarily due to intramolecular changes, mainly in the low-frequency structural modes of the protein caused by H/D exchange. The observed high KIE values are consistent with a transport mechanism that involves through-H-bonds of the β-sheet structure of Az, likely also those in the Cu coordination sphere.
测量蛋白质中固态电子输运(ETp)可以研究电子转移(ET)机制,同时最小化过程中的溶剂化效应。然而,ETp 对蛋白质中的任何静态(构象)或动态(振动)变化都很敏感。我们的宏观测量允许将 ETp 研究扩展到低温,同时由于电极接触面积较大,分辨率也较低。因此,我们之前报道了通过铜蛋白蓝铜蛋白(Az)的温度独立 ETp,从 80 K 到变性,而对于 apo-Az,ETp 在 180 K 以上的温度下是温度依赖的。氘代(H/D 取代)可以为固态中是否涉及氢键的 ETp 提供关于机制的信息。在这里,我们报告了作为温度函数的通过 holo-Az 的 ETp 的动力学氘同位素效应(KIE)测量结果(30-340 K)。令人惊讶的是,氘代作用使 ETp 在 180 K 以上从温度独立变为温度依赖。这种 H/D 效应在 1.8(340 K)和 9.1(≤180 K)之间的 KIE 值中得到了体现。这些值在 Az 在溶液中的 ET 的先前报道的反 KIE 下是显著的。我们将我们的 KIE 结果与在溶液中观察到的结果之间的差异归因于后者溶剂效应的主导地位(H2O 的热膨胀比 D2O 大),而在我们的情况下,KIE 主要是由于分子内变化,主要是蛋白质的低频结构模式由 H/D 交换引起的。观察到的高 KIE 值与涉及 Az 的β-折叠结构的通过氢键的输运机制一致,可能还涉及 Cu 配位球中的氢键。