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Protein Fluctuations as the Possible Origin of the Thermal Activation of Rod Photoreceptors in the Dark

机译:蛋白质波动是黑暗中棒感光细胞热激活的可能起源

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摘要

Efficient retinal photoisomerization, signal transduction, and amplification contribute to single-photon electrical responses in vertebrates visual cells. However, spontaneous discrete electrical signals arising in the dark, with identical intensity and time profiles as those generated by genuine single photons (dark events), limit the potential capability of the rod visual system to discern single photons from thermal noise. It is accepted that the light and the thermal activation of the rod photoreceptor rhodopsin (Rho) triggers the light and the dark events, respectively. However the activation barrier for the dark events (80-110 kJ/mol) appears to be only half of the barrier for light-dependent activation of Rho (≥180 kJ/mol). On the basis of these observations, it has been postulated that both processes should follow different pathways, but the molecular mechanism for the thermal activation process still remains an open question and subject of debate. Here, performing infrared difference spectroscopy measurements, we found that the -OH group of Thr118 from bovine Rho exhibits a slow but measurable hydrogen/deuterium exchange (HDX) under native conditions. Given the location of Thr118 in the X-ray structures, isolated from the aqueous phase and in steric contact with the buried retinal chromophore, we assume that a protein structural fluctuation must drive the retinal binding pocket (RBP) transiently open. We characterized the kinetics (rate and activation enthalpy) and thermodynamics (equilibrium constant and enthalpy) of this fluctuation from the global analysis of the HDX of Thr118-OH as a function of the temperature and pH. In parallel, using HPLC chromatography, we determined the kinetics of the thermal isomerization of the protonated 11 -cis retinal in solution, as a model for retinal thermal isomerization in an open RBP. Finally, we propose a quantitative two-step model in which the dark activation of Rho is triggered by thermal isomerization of the retinal in a transiently opened RBP, which accurately reproduced both the experimental activation barrier and the rate of the dark events. We conclude that the absolute sensitivity threshold of our visual system is limited by structural fluctuations of the chromophore binding pocket rather than in the chromophore itself.
机译:高效的视网膜光异构化,信号转导和扩增有助于脊椎动物视觉细胞中的单光子电反应。但是,在黑暗中产生的自发离散电信号具有与真正的单个光子(黑暗事件)所产生的强度和时间分布相同的强度和时间分布,这限制了棒状视觉系统识别单个光子与热噪声的潜在能力。棒状光感受器视紫红质(Rho)的光激活和热激活分别触发了亮事件和暗事件。但是,黑暗事件的激活势垒(80-110 kJ / mol)似乎只是光依赖的Rho激活(≥180kJ / mol)的一半。根据这些观察结果,假定两个过程都应遵循不同的途径,但是热活化过程的分子机理仍然是一个悬而未决的问题,并且尚需争论。在这里,通过进行红外差光谱测量,我们发现来自牛Rho的Thr118的-OH基团在自然条件下表现出缓慢但可测量的氢/氘交换(HDX)。给定Thr118在X射线结构中的位置(与水相隔离并与掩埋的视网膜生色团发生空间接触),我们认为蛋白质结构波动必须驱动视网膜结合袋(RBP)暂时打开。我们根据Thr118-OH HDX随温度和pH值的全局分析来表征了这种波动的动力学(速率和活化焓)和热力学(平衡常数和焓)。平行地,使用HPLC色谱,我们确定了溶液中质子化的11-顺式视网膜的热异构化动力学,作为开放RBP中的视网膜热异构化的模型。最后,我们提出了一个定量的两步模型,其中Rho的暗激活是由短暂打开的RBP中视网膜的热异构化触发的,该RBP准确地再现了实验激活屏障和暗事件的发生率。我们得出结论,我们视觉系统的绝对灵敏度阈值受发色团结合袋的结构波动限制,而不是受发色团本身的限制。

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  • 来源
    《Journal of the American Chemical Society》 |2010年第16期|p.5693-5703|共11页
  • 作者单位

    Department of Frontier Materials, Nagoya Institute of Technology, Showa-ku, Nagoya 466-8555, Japan Unitat de Biofisica, Departament de Bioquimica i de Biologia Molecular, and Centre d'Estudis en Bioflsica, Universitat Autonoma de Barcelona, Barcelona 08193, Spain;

    Department of Frontier Materials, Nagoya Institute of Technology, Showa-ku, Nagoya 466-8555, Japan Department of Life and Coordination-Complex Molecular Science, Institute for Molecular Science, 38 Nishigo-Naka, Myodaiji, Okazaki 444-8585, Japan;

    Department of Frontier Materials, Nagoya Institute of Technology, Showa-ku, Nagoya 466-8555, Japan;

    Department of Frontier Materials, Nagoya Institute of Technology, Showa-ku, Nagoya 466-8555, Japan;

    Department of Frontier Materials, Nagoya Institute of Technology, Showa-ku, Nagoya 466-8555, Japan;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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  • 正文语种 eng
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  • 入库时间 2022-08-18 03:15:32

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