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视觉色素的分子生物学

Molecular biology of the visual pigments.

作者信息

Applebury M L, Hargrave P A

出版信息

Vision Res. 1986;26(12):1881-95. doi: 10.1016/0042-6989(86)90115-x.

Abstract

With the identification and structural characterization of several visual pigments has come a new era of investigation. The above comparisons of amino acids sequences predict specific functional domains that may be tested to tell us how visual pigments function to absorb light and transform this "signal" to trigger a neural response. The details of how rod and cone pigments differ are now known for human pigments. The striking similarities between vertebrate and invertebrate pigments are remarkable for pigments that have been subject to divergence for over 500 million years. There are yet challenges ahead of us. The true tertiary structure of visual pigments must be obtained from a 3-dimensional crystal structure. The predictions for functional domains of interaction with the GTP binding protein must be confirmed or redefined. A rigorous definition of the chromophore environment and the properties that control the wavelength of absorption of 11-cis retinal chromophore are certainly still on the drawing boards. Specific genetic alteration through in vitro mutagenesis promises much insight, but the technology for expressing these membrane proteins in functional form has yet to be achieved. We may expect, however, these problems will be addressed and in the next few years facts should replace what are now speculations. Finally, it is a delightful observation that nature has capitalized on a general biochemical mechanism for control of second messengers in the cytoplasm of cells. Protein structural data deduced from genetic information now document the hypothesis that the structure and function of receptors for the catecholamines and that of visual pigments are similar. The receptors for serotonin, leukotrienes, prostaglandins, histamine and acetylcholine (muscarinic) are expected to belong to this same family. The lessons learned about visual pigments can be applied broadly to a general set of membrane receptors.

摘要

随着几种视觉色素的鉴定和结构表征,一个新的研究时代已经到来。上述氨基酸序列的比较预测了特定的功能域,这些功能域可以通过测试来告诉我们视觉色素如何发挥作用以吸收光线并将这种“信号”转化为触发神经反应。现在已知人类色素中视杆和视锥色素的差异细节。脊椎动物和无脊椎动物色素之间惊人的相似性对于已经分化了超过5亿年的色素来说是非常显著的。我们面前仍然存在挑战。视觉色素的真正三级结构必须从三维晶体结构中获得。与GTP结合蛋白相互作用的功能域的预测必须得到证实或重新定义。对发色团环境以及控制11-顺式视黄醛发色团吸收波长的特性的严格定义肯定仍在规划之中。通过体外诱变进行的特定基因改变有望带来很多见解,但以功能形式表达这些膜蛋白的技术尚未实现。然而,我们可以期待这些问题将得到解决,在未来几年,事实将取代现在的推测。最后,令人高兴的是,大自然利用了一种控制细胞胞质中第二信使的一般生化机制。从遗传信息推导得出的蛋白质结构数据现在证明了这样一个假设,即儿茶酚胺受体和视觉色素的结构与功能相似。血清素、白三烯、前列腺素、组胺和乙酰胆碱(毒蕈碱型)的受体预计也属于同一个家族。从视觉色素中学到的经验教训可以广泛应用于一组通用的膜受体。

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