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Synthetic self-assembling clostridial chimera for modulation of sensory functions.

机译:合成自组装梭菌嵌合体,可调节感觉功能。

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摘要

Clostridial neurotoxins reversibly block neuronal communication for weeks and months. While these proteolytic neurotoxins hold great promise for clinical applications and the investigation of brain function, their paralytic activity at neuromuscular junctions is a stumbling block. To redirect the clostridial activity to neuronal populations other than motor neurons, we used a new self-assembling method to combine the botulinum type A protease with the tetanus binding domain, which natively targets central neurons. The two parts were produced separately and then assembled in a site-specific way using a newly introduced 'protein stapling' technology. Atomic force microscopy imaging revealed dumbbell shaped particles which measure ∼23 nm. The stapled chimera inhibited mechanical hypersensitivity in a rat model of inflammatory pain without causing either flaccid or spastic paralysis. Moreover, the synthetic clostridial molecule was able to block neuronal activity in a defined area of visual cortex. Overall, we provide the first evidence that the protein stapling technology allows assembly of distinct proteins yielding new biomedical properties.
机译:梭菌神经毒素可逆地阻断神经元的交流长达数周和数月。虽然这些蛋白水解神经毒素在临床应用和脑功能研究方面具有广阔的前景,但它们在神经肌肉接头处的麻痹活性却是绊脚石。为了将梭菌活性重定向到运动神经元以外的神经元群体,我们使用了一种新的自组装方法,将A型肉毒杆菌蛋白酶与破伤风结合域结合在一起,后者天然靶向中枢神经元。这两部分分别生产,然后使用新近引入的“蛋白质钉合”技术以特定位置的方式组装。原子力显微镜成像显示哑铃形颗粒,尺寸约为23 nm。装订的嵌合体在炎性疼痛的大鼠模型中抑制了机械性超敏反应,而不会引起松弛或痉挛性麻痹。此外,合成的梭菌分子能够在视觉皮层的限定区域内阻断神经元活动。总体而言,我们提供了第一个证据,即蛋白质钉合技术可以组装独特的蛋白质,从而产生新的生物医学特性。

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