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一项用于评估杀菌性抗体与伤寒疫苗诱导的抗感染保护作用之间相关性的伤寒杆菌受控人体感染研究。

A Typhi Controlled Human Infection Study for Assessing Correlation between Bactericidal Antibodies and Protection against Infection Induced by Typhoid Vaccination.

作者信息

Jones Elizabeth, Jin Celina, Stockdale Lisa, Dold Christina, Pollard Andrew J, Hill Jennifer

机构信息

Oxford Vaccine Group, Department of Paediatrics, University of Oxford, and the NIHR Oxford Biomedical Research Centre, Oxford OX3 9DU, UK.

出版信息

Microorganisms. 2021 Jun 28;9(7):1394. doi: 10.3390/microorganisms9071394.

Abstract

Vi-polysaccharide conjugate vaccines are efficacious against typhoid fever in children living in endemic settings, their recent deployment is a promising step in the control of typhoid fever. However, there is currently no accepted correlate of protection. IgG and IgA antibodies generated in response to Vi conjugate or Vi plain polysaccharide vaccination are important but there are no definitive protective titre thresholds. We adapted a luminescence-based serum bactericidal activity (SBA) for use with Typhi and assessed whether bactericidal antibodies induced by either Vi tetanus toxoid conjugate (Vi-TT) or Vi plain polysaccharide (Vi-PS) were associated with protection in a controlled human infection model of typhoid fever. Both Vi-PS and Vi-TT induced significant increase in SBA titre after 28 days (Vi-PS; < 0.0001, Vi-TT; = 0.003), however higher SBA titre at the point of challenge did not correlate with protection from infection or reduced symptom severity. We cannot eliminate the role of SBA as part of a multifactorial immune response which protects against infection, however, our results do not support a strong role for SBA as a mechanism of Vi vaccine mediated protection in the CHIM setting.

摘要

Vi多糖结合疫苗对生活在伤寒流行地区的儿童预防伤寒热有效,其近期的应用是控制伤寒热的一个有希望的进展。然而,目前尚无公认的保护相关性指标。接种Vi结合疫苗或Vi普通多糖疫苗后产生的IgG和IgA抗体很重要,但尚无明确的保护性滴度阈值。我们改良了一种基于发光的血清杀菌活性(SBA)检测方法用于伤寒杆菌,并在伤寒热的受控人体感染模型中评估由Vi破伤风类毒素结合疫苗(Vi-TT)或Vi普通多糖(Vi-PS)诱导的杀菌抗体是否与保护作用相关。Vi-PS和Vi-TT在28天后均诱导SBA滴度显著增加(Vi-PS;<0.0001,Vi-TT;=0.003),然而,攻击时较高的SBA滴度与预防感染或减轻症状严重程度无关。我们不能排除SBA作为预防感染的多因素免疫反应一部分的作用,但是,我们的结果不支持SBA在受控人体感染模型中作为Vi疫苗介导保护机制的重要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/df8e/8304662/6acda2dbbd79/microorganisms-09-01394-g001.jpg

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