Department of Urology, Boston Children's Hospital, Department of Microbiology and Department of Surgery, Harvard Medical School, Boston, Massachusetts, United States of America.
Department of Biochemistry and Biophysics, Stockholm University, Stockholm, Sweden.
PLoS Biol. 2020 Mar 17;18(3):e3000618. doi: 10.1371/journal.pbio.3000618. eCollection 2020 Mar.
Botulinum neurotoxins (BoNTs) are a family of bacterial toxins with seven major serotypes (BoNT/A-G). The ability of these toxins to target and bind to motor nerve terminals is a key factor determining their potency and efficacy. Among these toxins, BoNT/B is one of the two types approved for medical and cosmetic uses. Besides binding to well-established receptors, an extended loop in the C-terminal receptor-binding domain (HC) of BoNT/B (HC/B) has been proposed to also contribute to toxin binding to neurons by interacting with lipid membranes (termed lipid-binding loop [LBL]). Analogous loops exist in the HCs of BoNT/C, D, G, and a chimeric toxin DC. However, it has been challenging to detect and characterize binding of LBLs to lipid membranes. Here, using the nanodisc system and biolayer interferometry assays, we find that HC/DC, C, and G, but not HC/B and HC/D, are capable of binding to receptor-free lipids directly, with HC/DC having the highest level of binding. Mutagenesis studies demonstrate the critical role of consecutive aromatic residues at the tip of the LBL for binding of HC/DC to lipid membranes. Taking advantage of this insight, we then create a "gain-of-function" mutant HC/B by replacing two nonaromatic residues at the tip of its LBL with tryptophan. Cocrystallization studies confirm that these two tryptophan residues do not alter the structure of HC/B or the interactions with its receptors. Such a mutated HC/B gains the ability to bind receptor-free lipid membranes and shows enhanced binding to cultured neurons. Finally, full-length BoNT/B containing two tryptophan mutations in its LBL, together with two additional mutations (E1191M/S1199Y) that increase binding to human receptors, is produced and evaluated in mice in vivo using Digit Abduction Score assays. This mutant toxin shows enhanced efficacy in paralyzing local muscles at the injection site and lower systemic diffusion, thus extending both safety range and duration of paralysis compared with the control BoNT/B. These findings establish a mechanistic understanding of LBL-lipid interactions and create a modified BoNT/B with improved therapeutic efficacy.
肉毒神经毒素(BoNTs)是一类具有七种主要血清型的细菌毒素(BoNT/A-G)。这些毒素靶向和结合运动神经末梢的能力是决定其效力和疗效的关键因素。在这些毒素中,BoNT/B 是两种获准用于医疗和美容用途的毒素之一。除了与既定受体结合外,BoNT/B 的 C 末端受体结合结构域(HC)中的扩展环(HC/B)也被提议通过与脂质膜相互作用(称为脂质结合环 [LBL])有助于毒素与神经元结合。类似的环存在于 BoNT/C、D、G 和嵌合毒素 DC 的 HCs 中。然而,检测和表征 LBL 与脂质膜的结合一直具有挑战性。在这里,我们使用纳米盘系统和生物层干涉测定法发现,HC/DC、C 和 G,但不是 HC/B 和 HC/D,能够直接与无受体的脂质结合,其中 HC/DC 的结合水平最高。突变研究表明,LBL 尖端连续的芳香族残基对于 HC/DC 与脂质膜的结合至关重要。利用这一见解,我们随后通过用色氨酸替换 LBL 尖端的两个非芳香族残基来创建具有“功能增益”的突变体 HC/B。共结晶研究证实,这两个色氨酸残基不会改变 HC/B 的结构或与其受体的相互作用。这种突变的 HC/B 获得了与无受体脂质膜结合的能力,并显示出对培养神经元的结合增强。最后,全长 BoNT/B 在其 LBL 中包含两个色氨酸突变,以及另外两个增加与人类受体结合的突变(E1191M/S1199Y),并在体内使用 Digit Abduction Score 测定法在小鼠中进行了生产和评估。与对照 BoNT/B 相比,这种突变毒素在注射部位麻痹局部肌肉的效果增强,全身扩散降低,从而延长了麻痹的安全性范围和持续时间。这些发现建立了对 LBL-脂质相互作用的机制理解,并创建了一种改良的 BoNT/B,其治疗效果得到改善。
Zotero 插件
