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Engineering Botulinum Toxins to Improve and Expand Targeting and SNARE Cleavage Activity

机译:工程肉毒杆菌毒素,以改善和扩大针对性和网罗切割活动。

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摘要

Botulinum neurotoxins (BoNTs) are highly successful protein therapeutics. Over 40 naturally occurring BoNTs have been described thus far and, of those, only 2 are commercially available for clinical use. Different members of the BoNT family present different biological properties but share a similar multi-domain structure at the molecular level. In nature, BoNTs are encoded by DNA in producing clostridial bacteria and, as such, are amenable to recombinant production through insertion of the coding DNA into other bacterial species. This, in turn, creates possibilities for protein engineering. Here, we review the production of BoNTs by the natural host and also recombinant production approaches utilised in the field. Applications of recombinant BoNT-production include the generation of BoNT-derived domain fragments, the creation of novel BoNTs with improved performance and enhanced therapeutic potential, as well as the advancement of BoNT vaccines. In this article, we discuss site directed mutagenesis, used to affect the biological properties of BoNTs, including approaches to alter their binding to neurons and to alter the specificity and kinetics of substrate cleavage. We also discuss the target secretion inhibitor (TSI) platform, in which the neuronal binding domain of BoNTs is substituted with an alternative cellular ligand to re-target the toxins to non-neuronal systems. Understanding and harnessing the potential of the biological diversity of natural BoNTs, together with the ability to engineer novel mutations and further changes to the protein structure, will provide the basis for increasing the scope of future BoNT-based therapeutics.
机译:肉毒杆菌神经毒素(BoNT)是非常成功的蛋白质疗法。迄今为止,已经描述了超过40种天然存在的BoNT,其中只有2种可商业用于临床。 BoNT家族的不同成员具有不同的生物学特性,但是在分子水平上具有相似的多结构域结构。在自然界中,BoNT在生产梭菌中由DNA编码,因此,通过将编码DNA插入其他细菌物种中,可以重组生产。反过来,这为蛋白质工程创造了可能性。在这里,我们回顾了天然宿主对BoNTs的生产,以及在该领域利用的重组生产方法。重组BoNT生产的应用包括BoNT衍生域片段的产生,具有改进的性能和增强的治疗潜力的新型BoNT的产生以及BoNT疫苗的发展。在本文中,我们讨论了定点诱变,用于影响BoNT的生物学特性,包括改变其与神经元的结合以及改变底物裂解的特异性和动力学的方法。我们还讨论了靶标分泌抑制剂(TSI)平台,其中BoNTs的神经元结合域被替代的细胞配体取代,从而将毒素重新靶向非神经系统。了解和利用天然BoNTs的生物多样性的潜力,以及工程化新突变和蛋白质结构进一步改变的能力,将为扩大未来基于BoNT的疗法的范围提供基础。

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