Ad26.RSV.preF completely protects calves from severe respiratory disease induced by bovine RSV challenge.

IF 6.9 1区 医学 Q1 IMMUNOLOGY NPJ Vaccines Pub Date : 2024-11-25 DOI:10.1038/s41541-024-01024-6
Leslie van der Fits, Rineke de Jong, Karin Dijkman, Marjolein Heemskerk-van der Meer, Lisanne Tettero, Judith Bonsing, Sophie van Oort, Jan Serroyen, Marianke van Schie, Norbert Stockhofe-Zurwieden, Benoit Callendret, Roland Zahn
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Abstract

Vaccination with Ad26.RSV.preF, an Adenoviral serotype 26 vector encoding RSV F protein stabilized in its prefusion conformation, has previously shown to be immunogenic and protective in RSV seropositive adults and immunogenic in seropositive infants. Human and bovine RSV (bRSV) are genetically highly related and share many aspects of pathogenesis, epidemiology and clinical manifestations at young age. As such, infection of calves with bRSV represents a clinically relevant model with high translational value, enabling preclinical evaluation of Ad26.RSV.preF vaccine efficacy in seronegative young animals. Immunization of young calves with Ad26.RSV.preF induced antibodies neutralizing both human and bovine RSV as well as RSV-specific cellular responses. After bRSV challenge, placebo immunized calves showed viral replication in the respiratory tract, and developed fever and lethargy accompanied with severe respiratory distress, resulting in pre-termination of 7/8 calves. In contrast, all Ad26.RSV.preF immunized calves completed the study with only mild clinical symptoms, strongly and significantly diminished viral loads in nasopharynx and lungs, and only minimal lung pathology. Thus, Ad26.RSV.preF is immunogenic in young calves and efficacious in a stringent heterologous bRSV challenge model, demonstrating induction of broadly protective immunity against severe disease.

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Ad26.RSV.preF可完全保护犊牛免受牛RSV挑战引起的严重呼吸道疾病。
Ad26.RSV.preF是一种编码RSV F蛋白的腺病毒血清型26载体,该蛋白稳定在预融合构象中,接种该载体曾被证明对RSV血清反应阳性的成人具有免疫原性和保护作用,对血清反应阳性的婴儿也具有免疫原性。人和牛 RSV(bRSV)在遗传学上高度相关,在发病机制、流行病学和幼年临床表现等许多方面都有相同之处。因此,小牛感染 bRSV 代表了一种具有高转化价值的临床相关模型,可对血清阴性幼畜的 Ad26.RSV.preF 疫苗疗效进行临床前评估。用Ad26.RSV.preF对幼犊进行免疫,可诱导中和人和牛RSV的抗体以及RSV特异性细胞反应。bRSV挑战后,安慰剂免疫犊牛的呼吸道出现病毒复制,并出现发热和嗜睡,伴有严重的呼吸困难,导致7/8的犊牛提前终止妊娠。相比之下,所有接受 Ad26.RSV.preF 免疫的小牛在完成研究后仅出现轻微的临床症状,鼻咽和肺部的病毒载量显著减少,肺部病理变化也很小。因此,Ad26.RSV.preF 对幼犊具有免疫原性,在严格的异源 bRSV 挑战模型中也有疗效,证明它能诱导广泛的保护性免疫,防止严重疾病的发生。
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来源期刊
NPJ Vaccines
NPJ Vaccines Immunology and Microbiology-Immunology
CiteScore
11.90
自引率
4.30%
发文量
146
审稿时长
11 weeks
期刊介绍: Online-only and open access, npj Vaccines is dedicated to highlighting the most important scientific advances in vaccine research and development.
期刊最新文献
Ad26.RSV.preF completely protects calves from severe respiratory disease induced by bovine RSV challenge. Author Correction: Reply to: mRNA COVID-19 vaccinations are not associated with RVO development 21 days and 12 weeks after vaccination. A randomized trial comparing safety, immunogenicity and efficacy of self-amplifying mRNA and adenovirus-vector COVID-19 vaccines. The PvRBP2b-TfR1 interaction is not essential for reticulocytes invasion by Plasmodium vivax isolates from Cambodia. Effect of XBB.1.5-adapted booster vaccination on the imprinting of SARS-CoV-2 immunity.
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