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一种呼吸道合胞病毒(RSV)亚单位候选疫苗G1F/M2的保护作用在小鼠中被一种类热休克蛋白70(HSP70)增强。

Protective effect of a RSV subunit vaccine candidate G1F/M2 was enhanced by a HSP70-Like protein in mice.

作者信息

Zeng Ruihong, Zhang Zhenya, Mei Xingguo, Gong Wei, Wei Lin

机构信息

Department of Immunology, Hebei Medical University, Zhongshan East Road 361, Shijiazhuang, Hebei province 050017, China.

The First Affiliated Hospital, Tsinghua University, Beijing 100016, China.

出版信息

Biochem Biophys Res Commun. 2008 Dec 12;377(2):495-499. doi: 10.1016/j.bbrc.2008.10.002. Epub 2008 Oct 11.

Abstract

Respiratory syncytial virus (RSV) is a major respiratory pathogen in newborns. Neonate vaccine should induce strong protective immunity. We have engineered a subunit vaccine candidate G1F/M2. A major problem in developing subunit vaccines is their limited immunogenicity. Aluminium adjuvants with a long history of use with routine childhood vaccines have some limitations, especially inability to elicit CTL response. There is a need for alternative adjuvants. Heat shock proteins (HSPs) are characterized as potent immunoadjuvants. In this study, HSP70-like protein 1 (HSP70L1) gene was cloned. The recombinant protein HSP70L1 was expressed in E. coli, purified and renaturated. We evaluated the potential of HSP70L1 used as the adjuvant of G1F/M2. G1F/M2 was chemically cross-linked with HSP70L1 (HSP-G1F/M2). HSP70L1 enhanced significantly the immunogenicity and protective effect of G1F/M2. HSP-G1F/M2 induced significant higher levels of antibodies, neutralizing antibodies and CTL activity than unadjuvanted G1F/M2. The antibody titers induced by HSP-G1F/M2 were similar to that by G1F/M2+Alum. RSV-specific CTL activity induced by HSP-G1F/M2 was stronger than that by G1F/M2+Alum. Interestingly, the protective effect of HSP-G1F/M2 against RSV was significantly stronger than that of G1F/M2+Alum. The results suggest that HSP70L1 is a potent adjuvant of G1F/M2.

摘要

呼吸道合胞病毒(RSV)是新生儿的主要呼吸道病原体。新生儿疫苗应诱导强大的保护性免疫。我们构建了一种亚单位疫苗候选物G1F/M2。开发亚单位疫苗的一个主要问题是其免疫原性有限。在常规儿童疫苗中使用历史悠久的铝佐剂有一些局限性,尤其是无法引发CTL反应。需要替代佐剂。热休克蛋白(HSPs)被认为是有效的免疫佐剂。在本研究中,克隆了HSP70样蛋白1(HSP70L1)基因。重组蛋白HSP70L1在大肠杆菌中表达、纯化并复性。我们评估了HSP70L1用作G1F/M2佐剂的潜力。G1F/M2与HSP70L1进行化学交联(HSP-G1F/M2)。HSP70L1显著增强了G1F/M2的免疫原性和保护作用。与未加佐剂的G1F/M2相比,HSP-G1F/M2诱导产生的抗体、中和抗体和CTL活性水平显著更高。HSP-G1F/M2诱导的抗体滴度与G1F/M2+明矾诱导的相似。HSP-G1F/M2诱导的RSV特异性CTL活性比G1F/M2+明矾诱导的更强。有趣的是,HSP-G1F/M2对RSV的保护作用明显强于G1F/M2+明矾。结果表明,HSP70L1是G1F/M2的有效佐剂。

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