Less reactogenic whole-cell pertussis vaccine confers protection from Bordetella pertussis infection.

IF 3.7 2区 生物学 Q2 MICROBIOLOGY
mSphere Pub Date : 2025-04-29 Epub Date: 2025-03-12 DOI:10.1128/msphere.00639-24
Karolína Škopová, Jana Holubová, Barbora Bočková, Eva Slivenecká, João Melo Santos de Barros, Ondřej Staněk, Peter Šebo
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引用次数: 0

Abstract

Pertussis resurged over the last decade in most countries that replaced the traditional whole-cell pertussis vaccines (wP) by the less reactogenic acellular pertussis vaccines (aP). The aP vaccines induce a Th2-polarized immune response and by a yet unknown mechanism hamper the clearance of Bordetella pertussis from infected nasopharyngeal mucosa. The aP-induced pertussis toxin-neutralizing antibodies effectively prevent the life-threatening pertussis pneumonia in infants, but aP-elicited immunity fails to prevent infection of nasopharyngeal mucosa and transmission of B. pertussis. In contrast, the more reactogenic traditional wP vaccines, alike natural infection, elicit a broad antibody response and trigger a Th1/Th17-polarized T cell immunity. We tackled here the reactogenicity of the conventional wP vaccines by genetic modification of the Fim2 and Fim3-producing B. pertussis strains used for wP vaccine manufacturing. Mutations were introduced into the genomes of vaccine strains (i) to reduce the TLR4 signaling potency of the lipid A of B. pertussis lipooligosaccharide (ΔlgmB), (ii) eliminate the enzymatic (immunosuppressive) activity of the pertussis toxin (PtxS1-R9K/E129G), and (iii) ablate the production of the dermonecrotic toxin (Δdnt). Experimental alum-adjuvanted wP vaccines prepared from such triply modified bacteria exhibited a reduced pyrogenicity in rabbits and a reduced systemic toxicity in mice, while conferring a comparable protection from B. pertussis infection as the unmodified wP vaccine.IMPORTANCEThe occasionally severe adverse reactions associated with some lots of the whole-cell pertussis vaccine (wP) led the industrialized nations to switch to the use of less reactogenic acellular pertussis vaccines that confer shorter-lasting protection. This yielded whooping cough resurgence and large whooping cough outbreaks are currently sweeping throughout European countries, calling for the replacement of the pertussis vaccine component of pediatric hexavaccines by an improved wP vaccine. We show that genetic detoxification of the Bordetella pertussis bacteria used for wP preparation yields a reduced reactogenicity wP vaccine that exhibits a reduced systemic toxicity in mice and reduced pyrogenicity in rabbits, while retaining high immunogenicity and protective potency in the mouse model of pneumonic infection by B. pertussis. This result has now been confirmed in a nonhuman primate model of B. pertussis infection of olive baboons, paving the way for the development of the next generation of pertussis vaccines.

低反应性全细胞百日咳疫苗可预防百日咳杆菌感染。
在过去的十年中,百日咳在大多数国家重新兴起,这些国家用低反应性的无细胞百日咳疫苗(aP)取代了传统的全细胞百日咳疫苗(wP)。aP疫苗诱导th2极化免疫反应,并通过一种尚不清楚的机制阻碍百日咳杆菌从感染的鼻咽粘膜清除。ap诱导的百日咳毒素中和抗体能有效预防危及生命的婴儿百日咳肺炎,但ap诱导的免疫不能预防鼻咽黏膜感染和百日咳杆菌的传播。相比之下,反应性更强的传统wP疫苗与自然感染一样,会引发广泛的抗体反应,并引发Th1/ th17极化的T细胞免疫。我们通过对用于生产白粉病疫苗的产生Fim2和fim3的百日咳百日咳菌株进行基因改造,解决了传统白粉病疫苗的反应原性问题。在疫苗株的基因组中引入突变(i)降低百日咳低脂多糖脂质A的TLR4信号转导效力(ΔlgmB), (ii)消除百日咳毒素(PtxS1-R9K/E129G)的酶(免疫抑制)活性,(iii)减少皮肤萎黄毒素的产生(Δdnt)。由这种三次修饰的细菌制备的实验性铝佐剂wP疫苗在家兔中表现出降低的热原性,在小鼠中表现出降低的全身毒性,同时具有与未修饰的wP疫苗相当的百日咳感染保护作用。重要性:与一些批次全细胞百日咳疫苗(wP)相关的偶尔严重的不良反应导致工业化国家转向使用反应性较低的非细胞百日咳疫苗,这种疫苗提供的保护持续时间较短。这导致百日咳死灰复燃,目前大规模的百日咳疫情正在席卷整个欧洲国家,呼吁用改进的白垩白疫苗取代儿童六联疫苗中的百日咳疫苗成分。我们发现,用于制备白粉菌的百日咳杆菌的遗传解毒产生了降低反应原性的白粉菌疫苗,在小鼠中表现出降低的全身毒性和兔的热原性,同时在百日咳杆菌肺炎感染的小鼠模型中保持了高免疫原性和保护效力。这一结果现已在橄榄狒狒感染百日咳杆菌的非人灵长类动物模型中得到证实,为开发下一代百日咳疫苗铺平了道路。
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来源期刊
mSphere
mSphere Immunology and Microbiology-Microbiology
CiteScore
8.50
自引率
2.10%
发文量
192
审稿时长
11 weeks
期刊介绍: mSphere™ is a multi-disciplinary open-access journal that will focus on rapid publication of fundamental contributions to our understanding of microbiology. Its scope will reflect the immense range of fields within the microbial sciences, creating new opportunities for researchers to share findings that are transforming our understanding of human health and disease, ecosystems, neuroscience, agriculture, energy production, climate change, evolution, biogeochemical cycling, and food and drug production. Submissions will be encouraged of all high-quality work that makes fundamental contributions to our understanding of microbiology. mSphere™ will provide streamlined decisions, while carrying on ASM''s tradition for rigorous peer review.
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