首页> 美国卫生研究院文献>Infection and Immunity >Immunization with the Chlamydia trachomatis Mouse Pneumonitis Major Outer Membrane Protein by Use of CpG Oligodeoxynucleotides as an Adjuvant Induces a Protective Immune Response against an Intranasal Chlamydial Challenge
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Immunization with the Chlamydia trachomatis Mouse Pneumonitis Major Outer Membrane Protein by Use of CpG Oligodeoxynucleotides as an Adjuvant Induces a Protective Immune Response against an Intranasal Chlamydial Challenge

机译:沙眼衣原体小鼠肺炎主要外膜蛋白的免疫接种通过使用CpG寡脱氧核苷酸作为佐剂诱导针对鼻内衣原体挑战的保护性免疫反应。

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摘要

Recently, we have shown that a vaccine consisting of a purified preparation of the Chlamydia trachomatis mouse pneumonitis (MoPn) major outer membrane protein (MOMP) and Freund's adjuvant can protect mice against a genital challenge. Here, we wanted to determine if CpG motifs could be used as an immune modulator to the MOMP to induce protection in mice against an intranasal (i.n.) challenge. One-week-old BALB/c mice were immunized intramuscularly and subcutaneously either once or three times at 2-week intervals with MOMP and CpG suspended in aluminum hydroxide (alum). Negative controls received ovalbumin, CpG, and alum. Positive controls were immunized i.n. with C. trachomatis MoPn elementary bodies (EB). Six weeks after the last immunization, mice were challenged i.n. with 104 inclusion-forming units (IFU) of the C. trachomatis MoPn serovar. Mice that received MOMP, CpG, and alum had a strong immune response, as shown by a high titer of serum antibodies to Chlamydia and significant lymphoproliferation of T-cells following stimulation with C. trachomatis EB. After the i.n. challenge mice immunized with MOMP, CpG, and alum showed significantly less body weight loss than the corresponding control mice immunized with ovalbumin, CpG, and alum. Ten days after the challenge the animals were euthanized, their lungs were weighed, and the numbers of IFU in the lungs were determined. The average weight of the lungs of the mice immunized with MOMP, CpG, and alum was significantly less than average weight of the lungs of the mice immunized with ovalbumin, CpG, and alum. Also, the average number of IFU recovered per mouse immunized with MOMP, CpG, and alum was significantly less than the average number of IFU per mouse detected in the mice inoculated with ovalbumin, CpG, and alum. In conclusion, our data show that CpG sequences can be used as an effective adjuvant with the C. trachomatis MoPn MOMP to elicit a protective immune response in mice against a chlamydial respiratory challenge.
机译:最近,我们显示了由沙眼衣原体小鼠肺炎(MoPn)主要外膜蛋白(MOMP)和弗氏佐剂的纯化制剂组成的疫苗可以保护小鼠免受生殖器攻击。在这里,我们想确定CpG基序是否可以用作MOMP的免疫调节剂,以诱导小鼠对抗鼻内(i.n.)攻击的保护作用。用悬浮在氢氧化铝(铝)中的MOMP和CpG,以2周的间隔对1周龄的BALB / c小鼠进行肌肉内和皮下免疫1或3次。阴性对照接受卵清蛋白,CpG和明矾。阳性对照在当天免疫。沙眼衣原体MoPn基本体(EB)。在最后一次免疫后六周,对小鼠进行i.n攻击。与沙眼衣原体MoPn血清型的10 4 内含物形成单位(IFU)。接受MOMP,CpG和明矾的小鼠具有较强的免疫反应,如沙眼衣原体EB刺激后获得的抗衣原体血清抗体高滴度和T细胞明显的淋巴增殖所示。在i.n.之后与用卵清蛋白,CpG和明矾免疫的对照小鼠相比,用MOMP,CpG和明矾免疫的挑战小鼠的体重减轻明显更少。攻击后十天,对动物实施安乐死,称量其肺的重量,并确定肺中IFU的数量。用MOMP,CpG和明矾免疫的小鼠的肺的平均重量显着小于用卵白蛋白,CpG和明矾免疫的小鼠的肺的平均重量。同样,用MOMP,CpG和明矾免疫的每只小鼠回收的IFU平均数显着小于在接种卵白蛋白,CpG和明矾的小鼠中检测到的每只IFU平均数。总之,我们的数据表明CpG序列可以用作沙眼衣原体MoPn MOMP的有效佐剂,以引起小鼠针对衣原体呼吸道攻击的保护性免疫应答。

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