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The Neisseria meningitidis Macrophage Infectivity Potentiator Protein Induces Cross-Strain Serum Bactericidal Activity and Is a Potential Serogroup B Vaccine Candidate ▿

机译:脑膜炎奈瑟氏球菌巨噬细胞感染增强剂蛋白诱导跨菌株血清杀菌活性,是潜在的血清群B疫苗候选者 ▿

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摘要

A gene encoding a 29-kDa protein from Neisseria meningitidis serogroup B strain MC58 with homology to the macrophage infectivity potentiator (MIP) protein of Legionella pneumophila was cloned and expressed in Escherichia coli, and the purified soluble recombinant protein (rMIP) was used for immunization studies. Analysis of the predicted amino acid sequences of MIP from 13 well-characterized meningococcal strains, isolated from carriers or patients and differing in serogroup, serotype, and subtype, showed that the protein was highly conserved (98 to 100%), with only three distinct sequence types (designated I, II, and III) found. Western blotting showed that the MIP protein was expressed at similar levels by all of these strains. Immunization of mice with type I MC58 rMIP in detergent micelles and liposomes containing monophosphoryl lipid A (MPLA) induced high levels of surface-reactive antibodies with serum bactericidal activity (SBA) titers of 1/1,024 against the homologous strain. Bactericidal antibodies were also induced with the protein in saline alone and liposomes alone (titers, 1/128) but not following adsorption to Al(OH)3. Significantly, antisera raised against type I rMIP administered in saline or liposomes killed strains of heterologous sequence types II and III with similar SBA titers (1/128 to 1/256). Taken together, these findings suggest that rMIP can provide cross-strain protection against meningococci and should be considered a potential antigen for inclusion in new vaccines against meningococcal infection.
机译:克隆和编码与嗜肺军团菌巨噬细胞感染增强剂(MIP)蛋白同源的脑膜炎奈瑟氏球菌血清群B株MC58的29 kDa蛋白的基因,并在大肠杆菌中表达,并使用纯化的可溶性重组蛋白(rMIP)进行免疫学习。从携带者或患者中分离出的,血清型,血清型和亚型不同的13种特征明确的脑膜炎球菌菌株的MIP预测氨基酸序列分析表明,该蛋白是高度保守的(98%至100%),只有三种不同找到序列类型(指定为I,II和III)。 Western印迹显示,所有这些菌株均以相似的水平表达MIP蛋白。用去污剂微团和含单磷酰脂质A(MPLA)的脂质体对I型MC58 rMIP小鼠进行免疫,可诱导高水平的表面反应抗体,其针对同源菌株的血清杀菌活性(SBA)效价为1/024。蛋白质也可以在单独的盐水和单独的脂质体中诱导杀菌抗体(滴度,1/128),但在吸附到Al(OH)3之后不诱导。显着地,针对在盐水或脂质体中施用的I型rMIP产生的抗血清杀死了具有相似SBA滴度(1/128至1/256)的异源序列II和III菌株。综上所述,这些发现表明,rMIP可以提供针对脑膜炎球菌的跨株保护,应该被认为是包含在针对脑膜炎球菌感染的新疫苗中的潜在抗原。

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