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分枝杆菌热休克蛋白作为载体分子。II:使用70 kDa分枝杆菌热休克蛋白作为结合疫苗的载体可避免使用佐剂和卡介苗初免。

Mycobacterial heat-shock proteins as carrier molecules. II: The use of the 70-kDa mycobacterial heat-shock protein as carrier for conjugated vaccines can circumvent the need for adjuvants and Bacillus Calmette Guérin priming.

作者信息

Barrios C, Lussow A R, Van Embden J, Van der Zee R, Rappuoli R, Costantino P, Louis J A, Lambert P H, Del Giudice G

机构信息

World Health Organization-Immunology Research and Training Center, Department of Pathology, University of Geneva, Switzerland.

出版信息

Eur J Immunol. 1992 Jun;22(6):1365-72. doi: 10.1002/eji.1830220606.

Abstract

In a recent work, we have shown that mycobacterial heat-shock proteins (hsp) of 65-kDa (GroEL-type) and 70-kDa (DnaK-type) acted as carrier molecules in mice, previously primed with Mycobacterium tuberculosis var. bovis (bacillus Calmette-Guérin, BCG), for the induction of high and long-lasting titers of IgG against the repetitive malaria synthetic peptide (NANP)40. Anti-peptide antibodies were induced when the malaria peptide, conjugated to the mycobacterial hsp, was given in the absence of any adjuvants (Lussow et al., Eur. J. Immunol. 1991. 87:2960). In this report, we show that mice immunized with peptides or oligosaccharides conjugated to the 70-kDa hsp produced high titers of IgG antibodies in the absence of any previous priming with BCG. The anti-peptide antibody response persisted for at least 1 year. This adjuvant-free carrier effect of the 70-kDa hsp was T cell dependent, since no anti-peptide nor anti-70-kDa IgG antibodies were induced in athymic nu/nu mice. Previous immunization of mice with the 65-kDa or 70-kDa hsp did not have any negative effect on the induction of anti-peptide IgG antibodies after immunization with hsp-peptide conjugates in the absence of adjuvants. Furthermore, preimmunization with the 65-kDa hsp could substitute for BCG in providing an effective priming for the induction of anti-(NANP) antibodies. Finally, both the 65-kDa and 70-kDa hsp acted as carrier molecules for the induction of IgG antibodies to group C meningococcal oligosaccharides, in the absence of adjuvants. These findings strongly suggest that the use of hsp as carriers in conjugated constructs for the induction of anti-peptide and anti-oligosaccharide antibodies could be of value in the design of new vaccines for eventual use in humans.

摘要

在最近的一项研究中,我们发现,65 kDa(GroEL型)和70 kDa(DnaK型)的分枝杆菌热休克蛋白(hsp)在预先用牛型结核分枝杆菌(卡介苗,BCG)致敏的小鼠中可作为载体分子,用于诱导针对重复性疟疾合成肽(NANP)40产生高滴度且持久的IgG。当与分枝杆菌hsp偶联的疟疾肽在无任何佐剂的情况下给予时,可诱导产生抗肽抗体(Lussow等人,《欧洲免疫学杂志》,1991年,87:2960)。在本报告中,我们表明,用与70 kDa hsp偶联的肽或寡糖免疫的小鼠,在未预先用BCG致敏的情况下产生了高滴度的IgG抗体。抗肽抗体反应持续了至少1年。70 kDa hsp的这种无佐剂载体效应依赖于T细胞,因为在无胸腺裸鼠(nu/nu)中未诱导出抗肽或抗70 kDa IgG抗体。在用65 kDa或70 kDa hsp预先免疫小鼠后,在无佐剂的情况下用hsp - 肽偶联物免疫,对诱导抗肽IgG抗体没有任何负面影响。此外,用65 kDa hsp进行预免疫可替代BCG,为诱导抗(NANP)抗体提供有效的致敏作用。最后,在无佐剂的情况下,65 kDa和70 kDa hsp均作为载体分子,用于诱导针对C群脑膜炎球菌寡糖的IgG抗体。这些发现有力地表明,在偶联构建物中使用hsp作为载体来诱导抗肽和抗寡糖抗体,在设计最终用于人类的新型疫苗方面可能具有价值。

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