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将藻酸盐与含有T细胞和B细胞表位的合成肽偶联,作为诱导针对铜绿假单胞菌的保护性免疫的方法。

Conjugation of alginate to a synthetic peptide containing T- and B-cell epitopes as an induction for protective immunity against Pseudomonas aeruginosa.

作者信息

Farjaha Ali, Owlia Parviz, Siadat Seyed Davar, Mousavi Seyed Fazlollah, Shafieeardestani Mehdi

出版信息

J Biotechnol. 2014 Dec 20;192 Pt A:240-7. doi: 10.1016/j.jbiotec.2014.10.025.

DOI:10.1016/j.jbiotec.2014.10.025
PMID:25449544
Abstract

Pseudomonas aeruginosa is a major cause of respiratory tract infections worldwide, particularly in hospitalized patients with immunosuppressed conditions and cystic fibrosis (CF). Excessive use of antibiotics means that there is currently resistance among bacterial infections to many drugs. Vaccination is a strategy that can reduce mortality and morbidity rates in infections such as those caused by P. aeruginosa. Alginate has a critical role in such infections and affects pathogenicity of the bacterium. In this work, the bioinformatics approach was used to design and synthesis a carrier peptide (ERRANAVRDVLVNEY), derived from OMP F P. aeruginosa. This peptide contained both B- and T-cell epitopes based on prediction models. Conjugation of alginate to carrier peptide was performed and then analyzed by Fourier transform infrared spectroscopy (FTIR). Results of this study on mice showed that the conjugate elicited anti-alginate-IgG that were not detected after immunization with naive alginate. The effect of the antibodies to alginate conjugate was evaluated as highly opsonic and showed moderate to high-level killing activity against two mucoid strains. IgG1 was also dominant among IgG subclasses. Mice vaccinated with the conjugate vaccine survived lethal challenges (2 ×LD 50). Furthermore, using an acute pneumonia model of infection in mice, determined that levels of P. aeruginosa in mice were significantly reduced in the vaccinated group. Thus, tests confirmed ability of this conjugate to elicit protective and opsonophagocytic antibodies that candidate our vaccine for further studies.

摘要

铜绿假单胞菌是全球呼吸道感染的主要病因,尤其是在免疫功能低下的住院患者和囊性纤维化(CF)患者中。抗生素的过度使用意味着目前细菌感染对许多药物都有耐药性。疫苗接种是一种可以降低由铜绿假单胞菌等引起的感染的死亡率和发病率的策略。藻酸盐在这类感染中起关键作用,并影响细菌的致病性。在这项工作中,采用生物信息学方法设计并合成了一种源自铜绿假单胞菌外膜蛋白F的载体肽(ERRANAVRDVLVNEY)。基于预测模型,该肽同时包含B细胞和T细胞表位。将藻酸盐与载体肽进行偶联,然后通过傅里叶变换红外光谱(FTIR)进行分析。对小鼠的这项研究结果表明,该偶联物能引发抗藻酸盐IgG,而用单纯藻酸盐免疫后未检测到这种抗体。对藻酸盐偶联物抗体的作用评估为具有高度调理作用,并对两种黏液型菌株显示出中度至高度的杀伤活性。IgG1在IgG亚类中也占主导地位。用偶联疫苗接种的小鼠在致死性攻击(2×LD50)中存活下来。此外,利用小鼠急性肺炎感染模型确定,接种组小鼠体内的铜绿假单胞菌水平显著降低。因此,试验证实了这种偶联物能够引发保护性和调理吞噬性抗体,使我们的候选疫苗有进一步研究的可能。

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