首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >PNAS Plus: Plasticity of the asialoglycoprotein receptor deciphered by ensemble FRET imaging and single-molecule counting PALM imaging
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PNAS Plus: Plasticity of the asialoglycoprotein receptor deciphered by ensemble FRET imaging and single-molecule counting PALM imaging

机译:PNAS Plus:通过整体FRET成像和单分子计数PALM成像破译的去唾液酸糖蛋白受体的可塑性

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摘要

The stoichiometry and composition of membrane protein receptors are critical to their function. However, the inability to assess receptor subunit stoichiometry in situ has hampered efforts to relate receptor structures to functional states. Here, we address this problem for the asialoglycoprotein receptor using ensemble FRET imaging, analytical modeling, and single-molecule counting with photoactivated localization microscopy (PALM). We show that the two subunits of asialoglycoprotein receptor [rat hepatic lectin 1 (RHL1) and RHL2] can assemble into both homo- and hetero-oligomeric complexes, displaying three forms with distinct ligand specificities that coexist on the plasma membrane: higher-order homo-oligomers of RHL1, higher-order hetero-oligomers of RHL1 and RHL2 with two-to-one stoichiometry, and the homo-dimer RHL2 with little tendency to further homo-oligomerize. Levels of these complexes can be modulated in the plasma membrane by exogenous ligands. Thus, even a simple two-subunit receptor can exhibit remarkable plasticity in structure, and consequently function, underscoring the importance of deciphering oligomerization in single cells at the single-molecule level.
机译:膜蛋白受体的化学计量和组成对其功能至关重要。但是,无法原位评估受体亚单位的化学计量,阻碍了将受体结构与功能状态相关联的努力。在这里,我们使用集成的FRET成像,分析模型和光活化定位显微镜(PALM)进行单分子计数来解决脱唾液酸糖蛋白受体的问题。我们显示去唾液酸糖蛋白受体的两个亚基[大鼠肝凝集素1(RHL1)和RHL2]可以组装成同型和异型寡聚复合物,显示出三种具有独特配体特异性并存在于质膜上的形式:高阶同型RHL1的低聚体,RHL1和RHL2的高阶异聚体(化学计量比为二比一)和均二聚体RHL2,几乎没有进一步的均聚趋势。这些复合物的水平可以通过外源性配体在质膜中调节。因此,即使是简单的二亚基受体也可以在结构上表现出显着的可塑性,并因此发挥功能,从而强调了在单分子水平上解密单细胞寡聚化的重要性。

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