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PHV02 活、减毒重组水疱性口炎病毒载体疫苗对尼帕病毒病提供的免疫相关性。

Immunological correlates of protection afforded by PHV02 live, attenuated recombinant vesicular stomatitis virus vector vaccine against Nipah virus disease.

机构信息

Crozet Biopharma LLC, Lexington, MA, United States.

Public Health Vaccines Inc., Cambridge, MA, United States.

出版信息

Front Immunol. 2023 Sep 4;14:1216225. doi: 10.3389/fimmu.2023.1216225. eCollection 2023.

DOI:10.3389/fimmu.2023.1216225
PMID:37731485
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10507387/
Abstract

INTRODUCTION

Immune correlates of protection afforded by PHV02, a recombinant vesicular stomatitis (rVSV) vector vaccine against Nipah virus (NiV) disease, were investigated in the African green monkey (AGM) model. Neutralizing antibody to NiV has been proposed as the principal mediator of protection against future NiV infection.

METHODS

Two approaches were used to determine the correlation between neutralizing antibody levels and outcomes following a severe (1,000 median lethal doses) intranasal/intratracheal (IN/IT) challenge with NiV (Bangladesh): (1) reduction in vaccine dose given 28 days before challenge and (2) challenge during the early phase of the antibody response to the vaccine.

RESULTS

Reduction in vaccine dose to very low levels led to primary vaccine failure rather than a sub-protective level of antibody. All AGMs vaccinated with the nominal clinical dose (2 × 10 pfu) at 21, 14, or 7 days before challenge survived. AGMs vaccinated at 21 days before challenge had neutralizing antibodies (geometric mean titer, 71.3). AGMs vaccinated at 7 or 14 days before challenge had either undetectable or low neutralizing antibody titers pre-challenge but had a rapid rise in titers after challenge that abrogated the NiV infection. A simple logistic regression model of the combined studies was used, in which the sole explanatory variable was pre-challenge neutralizing antibody titers. For a pre-challenge titer of 1:5, the predicted survival probability is 100%. The majority of animals with pre-challenge neutralizing titer of ≥1:20 were protected against pulmonary infiltrates on thoracic radiograms, and a majority of those with titers ≥1:40 were protected against clinical signs of illness and against a ≥fourfold antibody increase following challenge (indicating sterile immunity). Controls receiving rVSV-Ebola vaccine rapidly succumbed to NiV challenge, eliminating the innate immunity stimulated by the rVSV vector as a contributor to survival in monkeys challenged as early as 7 days after vaccination.

DISCUSSION AND CONCLUSION

It was concluded that PHV02 vaccine elicited a rapid onset of protection and that any detectable level of neutralizing antibody was a functional immune correlate of survival.

摘要

简介

本研究旨在探究 PHV02(一种重组水疱性口炎病毒 [rVSV] 载体疫苗)对尼帕病毒(NiV)疾病的保护作用与免疫相关性。针对 NiV 的中和抗体被认为是预防未来 NiV 感染的主要保护因素。

方法

本研究采用两种方法在非洲绿猴(AGM)模型中评估针对 NiV 的中和抗体水平与结果之间的相关性:(1)在严重(1000 中位致死剂量)经鼻/经气管(IN/IT)挑战前 28 天降低疫苗剂量;(2)在疫苗引发抗体反应的早期阶段进行挑战。

结果

疫苗剂量降至极低水平导致原发性疫苗失败,而非亚保护水平的抗体。所有在挑战前 21、14 或 7 天接种名义临床剂量(2×10pfu)的 AGM 均存活。在挑战前 21 天接种的 AGM 具有中和抗体(几何平均滴度为 71.3)。在挑战前 7 或 14 天接种的 AGM ,在挑战前具有无法检测或低水平的中和抗体滴度,但在挑战后迅速升高,从而阻止了 NiV 感染。采用简单的逻辑回归模型对联合研究进行分析,唯一的解释变量是挑战前的中和抗体滴度。对于挑战前滴度为 1:5 的情况,预测的存活率为 100%。大多数具有挑战前中和滴度≥1:20 的动物在胸部 X 光片上没有肺部浸润,大多数具有滴度≥1:40 的动物免受疾病临床症状的影响,并且在挑战后抗体增加≥四倍(表明无菌免疫)。接受 rVSV-埃博拉疫苗的对照动物迅速死于 NiV 挑战,消除了 rVSV 载体刺激的先天免疫作为接种后 7 天内接受挑战的猴子存活的贡献。

讨论与结论

研究结果表明,PHV02 疫苗能迅速引发保护作用,任何可检测水平的中和抗体均是生存的功能免疫相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3a14/10507387/dae66aa3b99e/fimmu-14-1216225-g007.jpg
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