增强1型菌毛表达以优化鼠伤寒沙门菌保护的候选减毒活疫苗的工程与评价

IF 5.2 3区医学 Q1 IMMUNOLOGY

Vaccines Pub Date : 2025-06-19 DOI:10.3390/vaccines13060659

Patricia García, Arianna Rodríguez-Coello, Andrea García-Pose, María Del Carmen Fernández-López, Andrea Muras, Miriam Moscoso, Alejandro Beceiro, Germán Bou

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引用次数: 0

摘要

背景：鼠伤寒沙门氏菌是一种主要的人畜共患病原体，其1型菌毛在肠道定植和免疫调节中起着至关重要的作用。本研究旨在通过设计1型菌毛的诱导表达来提高先前开发的生长缺陷菌株（d -谷氨酸和d -丙氨酸双缺陷菌株）的保护性免疫。方法：通过λ-Red诱变实现pta驱动膜操纵子的表达。qRT-PCR检测fimA的表达，透射电镜观察fimA的表达。通过FimH序列分析、酵母凝集、甘露糖结合/抑制试验和HT-29细胞粘附来评估粘附性能。用IRTA ΔΔΔ或IRTA ΔΔΔ PtetA:：薄膜对BALB/c小鼠进行口胃免疫。安全性和免疫原性通过临床监测、细菌负荷、粪便脱落、ELISA试验和使用粪便提取物的粘附/阻断试验来评估。对野生型和异种菌株攻毒后的保护作用进行了评价。结果：IRTA ΔΔΔ PtetA:：膜显示强劲的fimA表达，密集的毛覆盖，明显的甘露糖敏感粘附表型和增强的HT-29附着。菌缘过表达不改变肠道定植或转移到肠系膜淋巴结（mLNs）。免疫诱导了IgG1/IgG2a的混合表达，显著增加了对表达1型菌毛的沙门氏菌的IgA和IgG，并增强了粪便提取物抑制野生型菌株粘附的能力。在攻击（IRTA野生型/20220258）后，IRTA ΔΔΔ PtetA:：薄膜比IRTA ΔΔΔ更有效地减少了盲肠（-1.46/1.47-log）、大肠（-1.35/2.17-log）、mLNs （-1.32/0.98-log）和系统器官的感染负担。结论：1型菌毛的诱导表达增强了粘膜免疫和保护作用，支持将其纳入下一代沙门氏菌疫苗。未来的工作应该评估交叉保护并优化fimh介导的粘膜递送靶向。

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Engineering and Evaluation of a Live-Attenuated Vaccine Candidate with Enhanced Type 1 Fimbriae Expression to Optimize Protection Against Salmonella Typhimurium.

Background:Salmonella Typhimurium is a major zoonotic pathogen, in which type 1 fimbriae play a crucial role in intestinal colonization and immune modulation. This study aimed to improve the protective immunity of a previously developed growth-deficient strain-a double auxotroph for D-glutamate and D-alanine-by engineering the inducible expression of type 1 fimbriae. Methods: P_tetA-driven expression of the fim operon was achieved by λ-Red mutagenesis. fimA expression was quantified by qRT-PCR, and fimbriation visualized by transmission electron microscopy. Adhesive properties were evaluated through FimH sequence analysis, yeast agglutination, mannose-binding/inhibition assays, and HT-29 cell adherence. BALB/c mice were immunized orogastrically with IRTA ΔΔΔ or IRTA ΔΔΔ P_tetA::fim. Safety and immunogenicity were assessed by clinical monitoring, bacterial load, fecal shedding, ELISA tests, and adhesion/blocking assays using fecal extracts. Protection was evaluated after challenging with wild-type and heterologous strains. Results: IRTA ΔΔΔ P_tetA::fim showed robust fimA expression, dense fimbrial coverage, a marked mannose-sensitive adhesive phenotype and enhanced HT-29 attachment. Fimbrial overexpression did not alter intestinal colonization or translocation to mesenteric lymph nodes (mLNs). Immunization elicited a mixed IgG1/IgG2a, significantly increased IgA and IgG against type 1 fimbriae-expressing Salmonella, and enhanced the ability of fecal extracts to inhibit the adherence of wild-type strains. Upon challenge (IRTA wild-type/20220258), IRTA ΔΔΔ P_tetA::fim reduced infection burden in the cecum (-1.46/1.47-log), large intestine (-1.35/2.17-log), mLNs (-1.32/0.98-log) and systemic organs more effectively than IRTA ΔΔΔ. Conclusions: Inducible expression of type 1 fimbriae enhances mucosal immunity and protection, supporting their inclusion in next-generation Salmonella vaccines. Future work should assess cross-protection and optimize FimH-mediated targeting for mucosal delivery.

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来源期刊

Vaccines Pharmacology, Toxicology and Pharmaceutics-Pharmacology

CiteScore

8.90

自引率

16.70%

发文量

1853

审稿时长

18.06 days

期刊介绍： Vaccines (ISSN 2076-393X) is an international, peer-reviewed open access journal focused on laboratory and clinical vaccine research, utilization and immunization. Vaccines publishes high quality reviews, regular research papers, communications and case reports.