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LT-IIb(T13I),一种非毒性 II 型不耐热肠毒素,增强了蓖麻毒素亚单位疫苗引发中和抗体和保护性免疫的能力。

LT-IIb(T13I), a non-toxic type II heat-labile enterotoxin, augments the capacity of a ricin toxin subunit vaccine to evoke neutralizing antibodies and protective immunity.

机构信息

The Witebsky Center for Microbial Pathogenesis and Immunology, The University at Buffalo, Buffalo, New York, United States of America.

出版信息

PLoS One. 2013 Aug 2;8(8):e69678. doi: 10.1371/journal.pone.0069678. Print 2013.

DOI:10.1371/journal.pone.0069678
PMID:23936344
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3732243/
Abstract

Currently, there is a shortage of adjuvants that can be employed with protein subunit vaccines to enhance protection against biological threats. LT-IIb(T13I) is an engineered nontoxic derivative of LT-IIb, a member of the type II subfamily of heat labile enterotoxins expressed by Escherichia coli, that possesses potent mucosal adjuvant properties. In this study we evaluated the capacity of LT-IIb(T13I) to augment the potency of RiVax, a recombinant ricin toxin A subunit vaccine, when co-administered to mice via the intradermal (i.d.) and intranasal (i.n.) routes. We report that co-administration of RiVax with LT-IIb(T13I) by the i.d. route enhanced the levels of RiVax-specific serum IgG antibodies (Ab) and elevated the ratio of ricin-neutralizing to non-neutralizing Ab, as compared to RiVax alone. Protection against a lethal ricin challenge was also augmented by LT-IIb(T13I). While local inflammatory responses elicited by LT-IIb(T13I) were comparable to those elicited by aluminum salts (Imject®), LT-IIb(T13I) was more effective than aluminum salts at augmenting production of RiVax-specific serum IgG. Finally, i.n. administration of RiVax with LT-IIb(T13I) also increased levels of RiVax-specific serum and mucosal Ab and enhanced protection against ricin challenge. Collectively, these data highlight the potential of LT-IIb(T13I) as an effective next-generation i.d., or possibly i.n. adjuvant for enhancing the immunogenicity of subunit vaccines for biodefense.

摘要

目前,缺乏可与蛋白质亚单位疫苗一起使用的佐剂来增强对生物威胁的保护。LT-IIb(T13I) 是 LT-IIb 的一种工程无毒衍生物,LT-IIb 是大肠杆菌表达的不耐热肠毒素 II 亚家族的成员,具有强大的粘膜佐剂特性。在这项研究中,我们评估了 LT-IIb(T13I) 增强重组蓖麻毒素 A 亚单位疫苗 RiVax 效力的能力,当通过皮内 (i.d.) 和鼻内 (i.n.) 途径共给予小鼠时。我们报告说,与单独给予 RiVax 相比,通过皮内途径共给予 RiVax 和 LT-IIb(T13I) 增强了 RiVax 特异性血清 IgG 抗体 (Ab) 的水平,并提高了蓖麻毒素中和与非中和 Ab 的比值。LT-IIb(T13I) 还增强了对致死性蓖麻毒素挑战的保护。虽然 LT-IIb(T13I) 引起的局部炎症反应与铝盐 (Imject®) 引起的反应相当,但 LT-IIb(T13I) 比铝盐更有效地增强 RiVax 特异性血清 IgG 的产生。最后,鼻内给予 RiVax 和 LT-IIb(T13I) 也增加了 RiVax 特异性血清和粘膜 Ab 的水平,并增强了对蓖麻毒素挑战的保护。总之,这些数据突出了 LT-IIb(T13I) 作为有效下一代皮内佐剂,或可能作为鼻内佐剂,用于增强生物防御用亚单位疫苗的免疫原性的潜力。

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本文引用的文献

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Pilot phase IB clinical trial of an alhydrogel-adsorbed recombinant ricin vaccine.铝佐剂吸附重组蓖麻毒素疫苗的1B期临床试验
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Activation of Toll-like receptor 3 amplifies mesenchymal stem cell trophic factors and enhances therapeutic potency.激活 Toll 样受体 3 可放大间充质干细胞营养因子,增强治疗效力。
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Distinctive immunomodulatory and inflammatory properties of the Escherichia coli type II heat-labile enterotoxin LT-IIa and its B pentamer following intradermal administration.
在不干扰共生菌定植的情况下预防流感病毒诱导的肺炎球菌疾病的新策略。
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Novel Ricin Subunit Antigens With Enhanced Capacity to Elicit Toxin-Neutralizing Antibody Responses in Mice.具有增强能力在小鼠中引发毒素中和抗体反应的新型蓖麻毒素亚基抗原。
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The Divergent CD8+ T Cell Adjuvant Properties of LT-IIb and LT-IIc, Two Type II Heat-Labile Enterotoxins, Are Conferred by Their Ganglioside-Binding B Subunits.两种II型不耐热肠毒素LT-IIb和LT-IIc不同的CD8 + T细胞佐剂特性,由其神经节苷脂结合B亚基赋予。
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Intradermal administration of the Type II heat-labile enterotoxins LT-IIb and LT-IIc of enterotoxigenic Escherichia coli enhances humoral and CD8+ T cell immunity to a co-administered antigen.产肠毒素大肠杆菌的II型热不稳定肠毒素LT-IIb和LT-IIc的皮内给药可增强对共同给药抗原的体液免疫和CD8 + T细胞免疫。
PLoS One. 2014 Dec 23;9(12):e113978. doi: 10.1371/journal.pone.0113978. eCollection 2014.
大肠杆菌II型不耐热肠毒素LT-IIa及其B五聚体皮内注射后的独特免疫调节和炎症特性。
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LT-IIc, a new member of the type II heat-labile enterotoxin family, exhibits potent immunomodulatory properties that are different from those induced by LT-IIa or LT-IIb.LT-IIc 是 II 型不耐热肠毒素家族的新成员,具有与 LT-IIa 或 LT-IIb 不同的强大免疫调节特性。
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Principles of antidote pharmacology: an update on prophylaxis, post-exposure treatment recommendations and research initiatives for biological agents.解毒药理学原则:生物制剂的预防、暴露后治疗建议和研究计划的更新。
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Folding domains within the ricin toxin A subunit as targets of protective antibodies.蓖麻毒素 A 亚基内的折叠结构域作为保护性抗体的靶标。
Vaccine. 2010 Oct 8;28(43):7035-46. doi: 10.1016/j.vaccine.2010.08.020. Epub 2010 Aug 18.
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Intradermal administration of RiVax protects mice from mucosal and systemic ricin intoxication.皮内给药 RiVax 可保护小鼠免受粘膜和全身蓖麻毒素中毒。
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Targeting of antigens to skin dendritic cells: possibilities to enhance vaccine efficacy.抗原靶向皮肤树突状细胞:增强疫苗效力的可能性。
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