Allosteric proteins after thirty years: the binding and state functions of the neuronal alpha 7 nicotinic acetylcholine receptors.

Experientia Pub Date : 1996-12-15 DOI:10.1007/BF01952106
S J Edelstein, J P Changeux
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引用次数: 20

Abstract

A key statement of the 1965 Monod-Wyman-Changeux (MWC) model for allosteric proteins concerns the distinction between the ligand-binding function (Y) and the relevant state function (R). Sequential models predict overlapping behavior of the two functions. In contrast, a straightforward experimental consequence of the MWC model is that for an oligomeric protein the parameters which characterize the two functions should differ significantly. Two situations, where R > Y and the system is hyper-responsive or where R < Y and the system is hypo-responsive, have been encountered. Indeed, the hyper-responsive pattern was first observed for the enzyme aspartate transcarbamoylase, by comparing Y with R monitored by a change in sedimentation. Extensions of the theory to ligand-gated channels led to the suggestion that, on the one hand, hyper-responsive properties also occur with high-affinity mutants. On the other hand, native channels of the acetylcholine neuronal alpha 7 receptor and low-affinity mutants of the glycine receptor can be interpreted in terms of the hypo-responsive pattern. For the ligand-gated channels, whereas R is detected directly by ion flux, ligand binding has rarely been measured and the formation of desensitized states may complicate the analysis. However, stochastic models incorporating both binding and channel opening for single molecules predict differences that should be measurable with new experimental approaches, particularly fluorescence correlation spectroscopy.

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三十年后的变构蛋白:神经元α - 7烟碱乙酰胆碱受体的结合和状态功能。
1965年Monod-Wyman-Changeux (MWC)变构蛋白模型的一个关键陈述涉及配体结合功能(Y)和相关状态功能(R)之间的区别。序列模型预测了这两种功能的重叠行为。相反,MWC模型的一个直接的实验结果是,对于一个寡聚蛋白,表征这两种功能的参数应该有很大的不同。遇到了两种情况:R > Y,系统响应超快;R < Y,系统响应慢。事实上,通过比较Y和R的沉降变化,首次观察到天冬氨酸转甲氨基酰基酶的超反应模式。将这一理论扩展到配体门控通道,表明一方面,高亲和突变体也具有超响应特性。另一方面,乙酰胆碱神经元α 7受体的天然通道和甘氨酸受体的低亲和力突变体可以根据低反应模式来解释。对于配体门控通道,R是通过离子通量直接检测的,而配体结合很少被测量,并且脱敏状态的形成可能使分析复杂化。然而,结合单分子结合和通道打开的随机模型预测了应该用新的实验方法,特别是荧光相关光谱学来测量的差异。
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Immunogenetics. Cytosolic factors in mitochondrial protein import. Regulated protein degradation in mitochondria. The mitochondrial processing peptidase: function and specificity. Allosteric proteins after thirty years: the binding and state functions of the neuronal alpha 7 nicotinic acetylcholine receptors.
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