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抗结核 TB/FLU-04L-一种基于鼻内流感载体的增强型疫苗的临床前评价。

Preclinical Evaluation of TB/FLU-04L-An Intranasal Influenza Vector-Based Boost Vaccine against Tuberculosis.

机构信息

Smorodintsev Research Institute of Influenza of the Ministry of Health of the Russian Federation, 197022 St. Petersburg, Russia.

Saint-Petersburg State Research Institute of Phthisiopulmonology of the Ministry of Health of the Russian Federation, 191036 St. Petersburg, Russia.

出版信息

Int J Mol Sci. 2023 Apr 18;24(8):7439. doi: 10.3390/ijms24087439.

Abstract

Tuberculosis is a major global threat to human health. Since the widely used BCG vaccine is poorly effective in adults, there is a demand for the development of a new type of boost tuberculosis vaccine. We designed a novel intranasal tuberculosis vaccine candidate, TB/FLU-04L, which is based on an attenuated influenza A virus vector encoding two mycobacterium antigens, Ag85A and ESAT-6. As tuberculosis is an airborne disease, the ability to induce mucosal immunity is one of the potential advantages of influenza vectors. Sequences of ESAT-6 and Ag85A antigens were inserted into the NS1 open reading frame of the influenza A virus to replace the deleted carboxyl part of the NS1 protein. The vector expressing chimeric NS1 protein appeared to be genetically stable and replication-deficient in mice and non-human primates. Intranasal immunization of C57BL/6 mice or cynomolgus macaques with the TB/FLU-04L vaccine candidate induced -specific Th1 immune response. Single TB/FLU-04L immunization in mice showed commensurate levels of protection in comparison to BCG and significantly increased the protective effect of BCG when applied in a "prime-boost" scheme. Our findings show that intranasal immunization with the TB/FLU-04L vaccine, which carries two mycobacterium antigens, is safe, and induces a protective immune response against virulent

摘要

结核病是对全球人类健康的重大威胁。由于广泛使用的卡介苗(BCG)在成人中的效果不佳,因此需要开发新型结核增强疫苗。我们设计了一种新型鼻内结核疫苗候选物 TB/FLU-04L,它基于编码两种分枝杆菌抗原(Ag85A 和 ESAT-6)的减毒甲型流感病毒载体。由于结核病是一种空气传播疾病,因此诱导黏膜免疫的能力是流感载体的潜在优势之一。ESAT-6 和 Ag85A 抗原序列被插入甲型流感病毒的 NS1 开放阅读框中,取代 NS1 蛋白缺失的羧基部分。在小鼠和非人类灵长类动物中,表达嵌合 NS1 蛋白的载体似乎具有遗传稳定性和复制缺陷。用 TB/FLU-04L 疫苗候选物对 C57BL/6 小鼠或食蟹猴进行鼻内免疫,可诱导产生特异性 Th1 免疫应答。与 BCG 相比,单次 TB/FLU-04L 免疫在小鼠中显示出相当水平的保护作用,并且当在“初免-加强”方案中应用时,显著增加了 BCG 的保护作用。我们的研究结果表明,携带两种分枝杆菌抗原的鼻内免疫 TB/FLU-04L 疫苗是安全的,并可诱导针对强毒力的保护性免疫应答。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5ba3/10138401/1625a86db1e8/ijms-24-07439-g001.jpg

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