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评价劳森氏內变形菌亚单位疫苗介导的免疫原性和保护作用。

Evaluation of immunogenicity and protection mediated by Lawsonia intracellularis subunit vaccines.

机构信息

Department of Veterinary Microbiology, Western College of Veterinary Medicine, University of Saskatchewan, Saskatoon, Saskatchewan, Canada; Vaccine and Infectious Disease Organization (VIDO), University of Saskatchewan, Saskatoon, Saskatchewan, Canada.

Vaccine and Infectious Disease Organization (VIDO), University of Saskatchewan, Saskatoon, Saskatchewan, Canada.

出版信息

Vet Immunol Immunopathol. 2021 Jul;237:110256. doi: 10.1016/j.vetimm.2021.110256. Epub 2021 May 7.

Abstract

Lawsonia intracellularis is an economically important bacterium that causes ileitis in pigs. Current vaccines for L. intracellularis do not allow for differentiation between infected and vaccinated animals (DIVA), which is beneficial for disease tracking and surveillance. Previously, we identified five putative surface L. intracellularis proteins that were targeted by antibodies from pigs infected with L. intracellularis which could serve as antigens in a subunit vaccine. We conducted two trials to determine whether these antigens were immunogenic and provided protection against infectious challenge and whether truncated glycoprotein D could be used as a DIVA antigen. For Trial 1, 5 week-old piglets were administered intramuscular monovalent vaccines comprised of a recombinant (r) flagella subunit protein (rFliC,) and DIVA antigen (truncated glycoprotein D (TgD), a herpes virus antigen) both formulated with a combination adjuvant consisting of polyinosinic:polycytidylic acid(poly I:C), host defense peptide 1002 and polyphosphazene, referred to as Triple Adjuvant (TriAdj). Relative to control animals, animals vaccinated with rFliC and rTgD had significantly elevated antigen-specific humoral immunity in sera suggesting that rFliC and TgD are immunogenic. Control animals had negligible anti-TgD titres suggesting that TgD may be a suitable DIVA antigen for pigs. For Trial 2, piglets were immunized with a trivalent vaccine (FOG vaccine consisting of rFLiC, rOppA protein (a ABC Type dipeptide transport system) and rGroEL (a stress response protein)) and a divalent vaccine (CM vaccine consisting of rClpP (an ATP-dependent Clp protease proteolytic subunit) and rMetK (a S-adenosyl methionine synthase)) formulated with Emulsigen®. Relative to the control pigs, pigs immunized with the FOG vaccine produced robust and significantly higher serum IgG antibodies against rFliC and rGroEL, and significantly higher anti-FliC and anti-GroEL IgA antibodies in jejunal (GroEL only) and ileal intestinal mucosa. Pigs immunized with CM vaccine produced significantly higher serum antibodies against rClpP and rMetK and significantly higher anti-rClpP IgA antibodies in the ileum relative to the control pigs. Quantitative polymerase chain reaction (qPCR) analysis showed that 18 days after challenge with infectious L. intracellularis, challenged/control pigs and pigs that received the CM vaccine, but not the pigs vaccinated with the FOG vaccine, shed significantly more bacteria in feces than the unchallenged controls pigs. These data suggest that the FOG vaccinated pigs showed limited protection. While promising, more work is needed to enhance the efficiency of the intramuscular vaccine to show significant disease protection.

摘要

细胞内罗森菌是一种具有经济重要性的细菌,可引起猪的回肠炎。目前用于细胞内罗森菌的疫苗不能区分感染和接种的动物(DIVA),这有利于疾病跟踪和监测。以前,我们鉴定了五个假定的表面细胞内罗森菌蛋白,这些蛋白被感染细胞内罗森菌的猪的抗体靶向,可作为亚单位疫苗中的抗原。我们进行了两项试验,以确定这些抗原是否具有免疫原性,并提供针对传染性挑战的保护,以及截短糖蛋白 D 是否可用作 DIVA 抗原。对于试验 1,5 周龄的仔猪接受了肌肉内单价疫苗的接种,该疫苗由重组(r)鞭毛亚单位蛋白(rFliC)和 DIVA 抗原(截短糖蛋白 D(TgD),疱疹病毒抗原)组成,均与包含聚肌苷酸:聚胞苷酸(poly I:C)、宿主防御肽 1002 和聚磷腈的组合佐剂一起配制,称为三重佐剂(TriAdj)。与对照动物相比,用 rFliC 和 rTgD 接种的动物的血清中抗原特异性体液免疫显著升高,表明 rFliC 和 rTgD 具有免疫原性。对照动物的抗-TgD 滴度可忽略不计,表明 TgD 可能是猪的合适 DIVA 抗原。对于试验 2,仔猪用三价疫苗(FOG 疫苗,由 rFLiC、rOppA 蛋白(ABC 型二肽转运系统)和 rGroEL(应激反应蛋白)组成)和二价疫苗(CM 疫苗,由 rClpP(一种 ATP 依赖性 Clp 蛋白酶解亚基)和 rMetK(S-腺苷甲硫氨酸合酶)组成)与 Emulsigen®一起配制进行免疫。与对照猪相比,用 FOG 疫苗免疫的猪产生了针对 rFliC 和 rGroEL 的强大且显著更高的血清 IgG 抗体,并且在空肠(仅 GroEL)和回肠肠黏膜中产生了显著更高的抗-FliC 和抗-GroEL IgA 抗体。用 CM 疫苗免疫的猪产生了针对 rClpP 和 rMetK 的显著更高的血清抗体,并且在用 rClpP 免疫的猪的回肠中产生了显著更高的抗-rClpP IgA 抗体。定量聚合酶链反应(qPCR)分析显示,在感染性细胞内罗森菌攻毒后 18 天,攻毒/对照猪和接受 CM 疫苗但未接受 FOG 疫苗接种的猪的粪便中细菌载量明显高于未攻毒对照猪。这些数据表明,FOG 接种的猪显示出有限的保护。虽然有希望,但仍需要做更多的工作来提高肌肉内疫苗的效率,以显示出显著的疾病保护作用。

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