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脊椎动物和箱形水母视蛋白中视黄醛的三级结构的趋同进化。

Convergent evolution of tertiary structure in rhodopsin visual proteins from vertebrates and box jellyfish.

机构信息

Faculty of Biology Medicine and Health, University of Manchester, Manchester M13 9PL, United Kingdom.

Paul Scherrer Institute, 5232 Villigen PSI, Switzerland.

出版信息

Proc Natl Acad Sci U S A. 2018 Jun 12;115(24):6201-6206. doi: 10.1073/pnas.1721333115. Epub 2018 May 23.

Abstract

Box jellyfish and vertebrates are separated by >500 million years of evolution yet have structurally analogous lens eyes that employ rhodopsin photopigments for vision. All opsins possess a negatively charged residue-the counterion-to maintain visible-light sensitivity and facilitate photoisomerization of their retinaldehyde chromophore. In vertebrate rhodopsins, the molecular evolution of the counterion position-from a highly conserved distal location in the second extracellular loop (E181) to a proximal location in the third transmembrane helix (E113)-is established as a key driver of higher fidelity photoreception. Here, we use computational biology and heterologous action spectroscopy to determine whether the appearance of the advanced visual apparatus in box jellyfish was also accompanied by changes in the opsin tertiary structure. We found that the counterion in an opsin from the lens eye of the box jellyfish (JellyOp) has also moved to a unique proximal location within the transmembrane bundle-E94 in TM2. Furthermore, we reveal that this Schiff base/counterion system includes an additional positive charge-R186-that has coevolved with E94 to functionally separate E94 and E181 in the chromophore-binding pocket of JellyOp. By engineering this pocket-neutralizing R186 and E94, or swapping E94 with the vertebrate counterion E113-we can recreate versions of the invertebrate and vertebrate counterion systems, respectively, supporting a relatively similar overall architecture in this region of animal opsins. In summary, our data establish the third only counterion site in animal opsins and reveal convergent evolution of tertiary structure in opsins from distantly related species with advanced visual systems.

摘要

箱形水母和脊椎动物在进化上相隔超过 5 亿年,但它们具有结构相似的晶状体眼睛,这些眼睛使用视紫红质光色素进行视觉。所有视蛋白都带有一个带负电荷的残基——抗衡离子,以维持可见光敏感性并促进视黄醛发色团的光异构化。在脊椎动物视蛋白中,抗衡离子位置的分子进化——从第二细胞外环 (E181) 的高度保守的远端位置到第三跨膜螺旋 (E113) 的近端位置——已被确立为提高光感受器保真度的关键驱动因素。在这里,我们使用计算生物学和异源作用光谱学来确定箱形水母中先进视觉器官的出现是否也伴随着视蛋白三级结构的变化。我们发现,来自箱形水母晶状体眼的视蛋白中的抗衡离子也移动到了跨膜束内的独特近端位置-TM2 中的 E94。此外,我们揭示了这个席夫碱/抗衡离子系统包括一个额外的正电荷-R186-它与 E94 共同进化,在 JellyOp 的发色团结合口袋中功能上分离了 E94 和 E181。通过工程化这个口袋中和 R186 和 E94,或用脊椎动物抗衡离子 E113 替换 E94-我们可以分别重建无脊椎动物和脊椎动物抗衡离子系统的版本,支持动物视蛋白这一区域具有相对相似的整体结构。总之,我们的数据确定了动物视蛋白中的第三个抗衡离子位点,并揭示了具有先进视觉系统的远缘物种的视蛋白三级结构的趋同进化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eb45/6004467/4b2674365ac7/pnas.1721333115fig01.jpg

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