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QUANTUM DOT SINGLE MOLECULE TRACKING REVEALS A WIDE RANGE OF DIFFUSIVE MOTIONS OF MEMBRANE TRANSPORT PROTEINS

机译:量子点单分子示踪揭示了膜运输蛋白的扩散运动的广泛范围

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Single particle tracking (SPT) provides information about the microscopic motions of individual particles in live cells. We applied SPT to study the diffusion of membrane transport proteins in cell plasma membranes in which individual proteins are labeled with quantum dots at engineered extracellular epitopes. Software was created to deduce particle diffusive modes from quantum dot trajectories. SPT of aquaporin (AQP) water channels and cystic fibrosis transmembrane conductance regulator (CFTR) chloride channels revealed several types of diffusion. AQP1 was freely mobile in cell membranes, showing rapid, Brownian-type diffusion. The full-length (M1) isoform of AQP4 also diffused rapidly, though the diffusion of a shorter (M23) isoform of AQP4 was highly restricted due to its supermolecular assembly in raft-like orthogonal arrays. CFTR mobility was also highly restricted, in a spring-like potential, due to its tethering to the actin cytoskeleton through PDZ-domain C-terminus interactions. The biological significance of regulated diffusion of membrane transport proteins is a subject of active investigation.
机译:单粒子跟踪(SPT)提供有关活细胞中单个粒子的微观运动的信息。我们应用SPT研究了细胞质膜中膜转运蛋白的扩散,其中单个蛋白在工程化的细胞外表位上被量子点标记。创建了从量子点轨迹推断粒子扩散模式的软件。水通道蛋白(AQP)水通道的SPT和囊性纤维化跨膜电导调节剂(CFTR)氯化物通道的SPT显示出几种扩散类型。 AQP1在细胞膜中自由移动,显示出快速的布朗型扩散。 AQP4的全长(M1)异构体也迅速扩散,尽管较短的(M23)异构体的扩散由于其在筏状正交阵列中的超分子组装而受到高度限制。由于CFTR通过PDZ域C末端相互作用与肌动蛋白细胞骨架束缚,因此它在春季的潜力中也受到极大限制。膜转运蛋白的调节扩散的生物学意义是积极研究的主题。

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