Modular photostable fluorescent DNA blocks dissect the effects of pathogenic mutant kinesin on collective transport

Tomoki Kita, Ryota Sugie, Yuki Suzuki, Shinsuke Niwa
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Abstract

Intracellular transport is driven by teams of various motor proteins. Advances in DNA nanotechnology have enabled the programmable linkage of different types of motor proteins. In this study, we developed a modular, photostable, fluorescence-labeled tiny DNA origami block (FTOB) for extended observation of collective transport by selected motor combinations. The FTOB is designed as a 4-helix bundle (~8.4 nm) with densely accumulated fluorescent dyes, minimizing blinking and photobleaching. By designing a pair of connector DNAs, FTOBs are heterodimerized following motor protein attachment using the ALFA-tag/nanobody system. Our system examined the impact of a pathogenic mutant kinesin on its collective movement with wild-type kinesin, clearly observing two distinct behaviors: the team's velocity was generally governed by the slower mutant but occasionally surged to levels comparable to that of a single wild-type motor. Our photostable, robust, modular FTOB system could serve as a versatile tool for precisely dissecting cooperative cargo transport.
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模块化光稳定荧光 DNA 块剖析致病突变驱动蛋白对集体运输的影响
细胞内运输由各种运动蛋白组成的团队驱动。DNA 纳米技术的进步实现了不同类型的运动蛋白的可编程连接。在这项研究中,我们开发了一种模块化、光稳定、荧光标记的微小 DNA 折纸块(FTOB),用于扩展观察选定马达组合的集体运输。FTOB 被设计成一个 4 螺旋束(约 8.4 nm),上面密集地积聚着荧光染料,从而最大程度地减少了闪烁和光漂白。通过设计一对连接 DNA,FTOB 在使用 ALFA-tag/nanobody 系统连接马达蛋白后被异源二聚化。我们的系统检测了致病突变驱动蛋白对其与野生型驱动蛋白集体运动的影响,清楚地观察到两种截然不同的行为:团队的速度一般由较慢的突变体控制,但偶尔也会激增到与单个野生型马达相当的水平。我们的FTOB系统具有光稳定性、稳健性和模块化,可以作为精确剖析合作货物运输的多功能工具。
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