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一种四联抗原疫苗在侵袭性疾病临床前模型中的性能

Performance of a Four-Antigen Vaccine in Preclinical Models of Invasive Disease.

作者信息

Scully Ingrid L, Timofeyeva Yekaterina, Illenberger Arthur, Lu Peimin, Liberator Paul A, Jansen Kathrin U, Anderson Annaliesa S

机构信息

Pfizer Vaccine Research & Development, Pearl River, NY 10965, USA.

出版信息

Microorganisms. 2021 Jan 15;9(1):177. doi: 10.3390/microorganisms9010177.

Abstract

A four-antigen vaccine (SA4Ag) was designed for the prevention of invasive disease in surgical patients. The vaccine is composed of capsular polysaccharide type 5 and type 8 CRM conjugates, a clumping factor A mutant (Y338A-ClfA) and manganese transporter subunit C (MntC). pathogenicity is characterized by an ability to rapidly adapt to the host environment during infection, which can progress from a local infection to sepsis and invasion of distant organs. To test the protective capacity of the SA4Ag vaccine against progressive disease stages of an invasive infection, a deep tissue infection mouse model, a bacteremia mouse model, a pyelonephritis model, and a rat model of infectious endocarditis were utilized. SA4Ag vaccination significantly reduced the bacterial burden in deep tissue infection, in bacteremia, and in the pyelonephritis model. Complete prevention of infection was demonstrated in a clinically relevant endocarditis model. Unfortunately, these positive preclinical findings with SA4Ag did not prove the clinical utility of SA4Ag in the prevention of surgery-associated invasive infection.

摘要

一种四抗原疫苗(SA4Ag)被设计用于预防外科手术患者的侵袭性疾病。该疫苗由5型和8型荚膜多糖CRM结合物、聚集因子A突变体(Y338A-ClfA)和锰转运蛋白亚基C(MntC)组成。病原体的致病性表现为在感染期间能够迅速适应宿主环境,这种感染可从局部感染发展为败血症并侵袭远处器官。为了测试SA4Ag疫苗对侵袭性感染进展阶段疾病的保护能力,使用了深部组织感染小鼠模型、菌血症小鼠模型、肾盂肾炎模型和感染性心内膜炎大鼠模型。SA4Ag疫苗接种显著降低了深部组织感染、菌血症和肾盂肾炎模型中的细菌负荷。在临床相关的心内膜炎模型中证明了对感染的完全预防。不幸的是,SA4Ag这些阳性的临床前研究结果并未证明SA4Ag在预防手术相关侵袭性感染方面的临床效用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9e5e/7830931/f6a5c0fb41f3/microorganisms-09-00177-g001a.jpg

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