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新型肉毒杆菌神经毒素A8亚型的分离与功能特性研究

Isolation and functional characterization of the novel Clostridium botulinum neurotoxin A8 subtype.

作者信息

Kull Skadi, Schulz K Melanie, Weisemann Jasmin, Kirchner Sebastian, Schreiber Tanja, Bollenbach Alexander, Dabrowski P Wojtek, Nitsche Andreas, Kalb Suzanne R, Dorner Martin B, Barr John R, Rummel Andreas, Dorner Brigitte G

机构信息

Biological Toxins (ZBS3), Centre for Biological Threats and Special Pathogens, Robert Koch-Institut, Berlin, Germany.

Institut für Toxikologie, Medizinische Hochschule Hannover, Hannover, Germany.

出版信息

PLoS One. 2015 Feb 6;10(2):e0116381. doi: 10.1371/journal.pone.0116381. eCollection 2015.

Abstract

Botulism is a severe neurological disease caused by the complex family of botulinum neurotoxins (BoNT). Based on the different serotypes known today, a classification of serotype variants termed subtypes has been proposed according to sequence diversity and immunological properties. However, the relevance of BoNT subtypes is currently not well understood. Here we describe the isolation of a novel Clostridium botulinum strain from a food-borne botulism outbreak near Chemnitz, Germany. Comparison of its botulinum neurotoxin gene sequence with published sequences identified it to be a novel subtype within the BoNT/A serotype designated BoNT/A8. The neurotoxin gene is located within an ha-orfX+ cluster and showed highest homology to BoNT/A1, A2, A5, and A6. Unexpectedly, we found an arginine insertion located in the HC domain of the heavy chain, which is unique compared to all other BoNT/A subtypes known so far. Functional characterization revealed that the binding characteristics to its main neuronal protein receptor SV2C seemed unaffected, whereas binding to membrane-incorporated gangliosides was reduced in comparison to BoNT/A1. Moreover, we found significantly lower enzymatic activity of the natural, full-length neurotoxin and the recombinant light chain of BoNT/A8 compared to BoNT/A1 in different endopeptidase assays. Both reduced ganglioside binding and enzymatic activity may contribute to the considerably lower biological activity of BoNT/A8 as measured in a mouse phrenic nerve hemidiaphragm assay. Despite its reduced activity the novel BoNT/A8 subtype caused severe botulism in a 63-year-old male. To our knowledge, this is the first description and a comprehensive characterization of a novel BoNT/A subtype which combines genetic information on the neurotoxin gene cluster with an in-depth functional analysis using different technical approaches. Our results show that subtyping of BoNT is highly relevant and that understanding of the detailed toxin function might pave the way for the development of novel therapeutics and tailor-made antitoxins.

摘要

肉毒中毒是一种由肉毒杆菌神经毒素(BoNT)复杂家族引起的严重神经疾病。基于目前已知的不同血清型,根据序列多样性和免疫特性提出了一种称为亚型的血清型变体分类。然而,目前对BoNT亚型的相关性了解尚少。在此,我们描述了从德国开姆尼茨附近一起食源性肉毒中毒暴发中分离出的一株新型肉毒梭菌菌株。将其肉毒杆菌神经毒素基因序列与已发表序列进行比较,确定它是BoNT/A血清型内的一个新型亚型,命名为BoNT/A8。神经毒素基因位于一个ha-orfX+簇内,与BoNT/A1、A2、A5和A6具有最高的同源性。出乎意料的是,我们在重链的HC结构域中发现了一个精氨酸插入,这与迄今为止已知的所有其他BoNT/A亚型相比是独特的。功能特性表明,其与主要神经元蛋白受体SV2C的结合特性似乎未受影响,而与膜结合神经节苷脂的结合与BoNT/A1相比有所减少。此外,在不同的内肽酶测定中,我们发现BoNT/A8天然全长神经毒素和重组轻链的酶活性明显低于BoNT/A1。在小鼠膈神经半膈肌测定中,神经节苷脂结合减少和酶活性降低都可能导致BoNT/A8的生物活性显著降低。尽管活性降低,但新型BoNT/A8亚型在一名63岁男性中引起了严重的肉毒中毒。据我们所知,这是对一种新型BoNT/A亚型的首次描述和全面表征,它将神经毒素基因簇的遗传信息与使用不同技术方法的深入功能分析相结合。我们的结果表明,BoNT亚型分类高度相关,对毒素详细功能的了解可能为新型治疗方法和定制抗毒素的开发铺平道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1d79/4320087/291c002d6073/pone.0116381.g001.jpg

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