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Plasma membrane localization signals in the light chain of botulinum neurotoxin

机译:肉毒杆菌神经毒素轻链中的质膜定位信号

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Botulinum neurotoxin (BoNT) is a potent biological substance used to treat neuromuscular and pain disorders. Both BoNT type A and BoNT type E display high-affinity uptake into motor neurons and inhibit exocytosis through cleavage of the synaptosome-associated protein of 25 kDa (SNAP25). The therapeutic effects of BoNT/A last from 3 to 12 months, whereas the effects of BoNT/E last less than 4 weeks. Using confocal microscopy and site-specific mutagenesis, we have determined that the protease domain of BoNT/A light chain (BoNT/ A-LC) localizes in a punctate manner to the plasma membrane, colocalizing with the cleaved product SNAP25_(197). In contrast, the short-duration BoNT/E serotype is cytoplasmic. Mutations in the BoNT/A-LC have revealed sequences at the N terminus necessary for plasma membrane localization, and an active dileucine motif in the C terminus that is likely involved in trafficking and interaction with adaptor proteins. These data support sequence-specific signals as determinants of intracellular localization and as a basis for the different durations of action in these two BoNT serotypes.
机译:肉毒杆菌神经毒素(BoNT)是一种有效的生物物质,可用于治疗神经肌肉和疼痛疾病。 BoNT A型和BoNT E型均显示出对运动神经元的高亲和力吸收,并通过裂解25kDa的突触体相关蛋白(SNAP25)来抑制胞吐作用。 BoNT / A的疗效持续3到12个月,而BoNT / E的疗效持续不到4周。使用共聚焦显微镜和位点特异性诱变,我们已确定BoNT / A轻链(BoNT / A-LC)的蛋白酶结构域以点状方式定位于质膜,与裂解产物SNAP25_(197)共定位。相反,短期BoNT / E血清型是细胞质的。 BoNT / A-LC中的突变已揭示了质膜定位所必需的N末端的序列,以及C末端的活跃的双亮氨酸基序,可能与转运和与衔接子蛋白相互作用有关。这些数据支持序列特异性信号,这些信号是细胞内定位的决定因素,并且是这两种BoNT血清型中不同作用时间的基础。

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