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利用丝状血凝素作为载体,通过重组百日咳博德特氏菌生产不可分型流感嗜血杆菌HtrA。

Production of nontypeable Haemophilus influenzae HtrA by recombinant Bordetella pertussis with the use of filamentous hemagglutinin as a carrier.

作者信息

Alonso Sylvie, Willery Eve, Renauld-Mongénie Genevieve, Locht Camille

机构信息

INSERM U629, Institut Pasteur de Lille, 1 rue du Prof. Calmette, F-59019 Lille, France.

出版信息

Infect Immun. 2005 Jul;73(7):4295-301. doi: 10.1128/IAI.73.7.4295-4301.2005.

Abstract

Bordetella pertussis, the etiologic agent of whooping cough, is a highly infectious human pathogen capable of inducing mucosal and systemic immune responses upon a single intranasal administration. In an attenuated, pertussis toxin (PTX)-deficient recombinant form, it may therefore constitute an efficient bacterial vector that is particularly well adapted for the delivery of heterologous antigens to the respiratory mucosa. Filamentous hemagglutinin (FHA) has been used as a carrier to present foreign antigens at the bacterial surface, thereby inducing local, systemic, and protective immune responses to these antigens in mice. Both full-length and truncated (Fha44) forms of FHA have been used for antigen presentation. To investigate the effect of the carrier (FHA or Fha44) on antibody responses to passenger antigens, we genetically fused the HtrA protein of nontypeable Haemophilus influenzae to either FHA form. The fha-htrA and Fha44 gene-htrA hybrids were expressed as single copies inserted into the chromosome of PTX-deficient B. pertussis. Both chimeras were secreted into the culture supernatants of the recombinant strains and were recognized by anti-FHA and anti-HtrA antibodies. Intranasal infection with the strain producing the FHA-HtrA hybrid led to significantly higher anti-HtrA and anti-FHA antibody titers than those obtained in mice infected with the Fha44-HtrA-producing strain. Interestingly, the B. pertussis strain producing the Fha44-HtrA chimera colonized the mouse lungs more efficiently than the parental, Fha44-producing strain and gave rise to higher anti-FHA antibody titers than those induced by the parental strain.

摘要

百日咳博德特氏菌是百日咳的病原体,是一种高度传染性的人类病原体,单次鼻内给药即可诱导粘膜和全身免疫反应。因此,以减毒的、缺乏百日咳毒素(PTX)的重组形式存在时,它可能构成一种高效的细菌载体,特别适合于将异源抗原递送至呼吸道粘膜。丝状血凝素(FHA)已被用作载体,在细菌表面呈递外源抗原,从而在小鼠中诱导针对这些抗原的局部、全身和保护性免疫反应。FHA的全长和截短形式(Fha44)均已用于抗原呈递。为了研究载体(FHA或Fha44)对乘客抗原抗体反应的影响,我们将不可分型流感嗜血杆菌的HtrA蛋白与两种FHA形式进行了基因融合。fha-htrA和Fha44基因-htrA杂种以单拷贝形式表达,插入到缺乏PTX的百日咳博德特氏菌染色体中。两种嵌合体均分泌到重组菌株的培养上清液中,并被抗FHA和抗HtrA抗体识别。用产生FHA-HtrA杂种的菌株进行鼻内感染,导致抗HtrA和抗FHA抗体滴度显著高于用产生Fha44-HtrA的菌株感染的小鼠。有趣的是,产生Fha44-HtrA嵌合体的百日咳博德特氏菌菌株比亲本的、产生Fha44的菌株更有效地定殖于小鼠肺部,并产生比亲本菌株诱导的更高的抗FHA抗体滴度。

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