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Passive Transfer of Antiserum Specific for Immunogens Derived from a Nontypeable Haemophilus influenzae Adhesin and Lipoprotein D Prevents Otitis Media after Heterologous Challenge

机译:被动转移抗血清特异的抗血清特异性抗原来自不可分型的流感嗜血杆菌粘附素和脂蛋白D预防异源性攻击后的中耳炎

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摘要

We recently determined that passive transfer of serum directed against a synthetic peptide called LB1 or a recombinant fusion protein immunogen [LPD-LB1(f)2,1,3] could prevent otitis media after challenge with a homologous nontypeable Haemophilus influenzae (NTHI) isolate. NTHI residing in the nasopharynx was rapidly cleared from this site, thus preventing it from ascending the eustachian tube and inducing otitis media in chinchillas compromised by an ongoing viral upper respiratory tract infection. While LB1 is based solely on one NTHI adhesin, the latter immunogen, LPD-LB1(f)2,1,3, was designed to incorporate two NTHI antigens shown to play a role in the pathogenesis of otitis media; lipoprotein D (LPD) and the P5-homologous fimbrin adhesin. The design of LPD-LB1(f)2,1,3 also accommodated for the recently demonstrated existence of three major groupings, based on amino acid sequence diversity, in the third surface-exposed region of P5-fimbrin. LPD-LB1(f)2,1,3 was thus designed to potentially confer broader protection against challenge by diverse strains of NTHI. Chinchillas were passively immunized here with serum specific for either LB1 or for LPD-LB1(f)2,1,3 prior to challenge with a member of all three groups of NTHI relative to diversity in region 3. The transferred serum pools were also analyzed for titer, specificity, and several functional activities. We found that both serum pools had equivalent ability to mediate C′-dependent killing and to inhibit adherence of NTHI strains to human oropharyngeal cells. When passively transferred, both serum pools significantly inhibited the signs and incidence of otitis media (P ≤ 0.01) induced by any of the three challenge isolates. Despite providing protection against disease, the ability of these antisera to induce total eradication of NTHI from the nasopharynx was not equivalent among NTHI groups. These data thus suggested that while early, complete eradication of NTHI from the nasopharynx was highly protective, reduction of the bacterial load to below a critical threshold level appeared to be similarly effective.
机译:我们最近确定,针对一种称为LB1的合成肽或重组融合蛋白免疫原[LPD-LB1(f)2,1,3]的血清的被动转移可以预防同源性不可分型流感嗜血杆菌(NTHI)分离株引起的中耳炎。驻留在鼻咽中的NTHI可从该部位迅速清除,从而防止其上升到咽鼓管并在龙猫中诱导被持续的病毒性上呼吸道感染损害的中耳炎。虽然LB1仅基于一种NTHI粘附素,但后者的免疫原LPD-LB1(f)2,1,3被设计为掺入两种NTHI抗原,这些抗原在中耳炎的发病机理中发挥作用。脂蛋白D(LPD)和P5同源纤维蛋白粘附素。 LPD-LB1(f)2,1,3的设计还适应了最近展示的基于氨基酸序列多样性在P5-膜蛋白第三暴露区域的三个主要组的存在。 LPD-LB1(f)2,1,3因此被设计为可能赋予更广泛的保护,以抵抗各种NTHI菌株的攻击。在用三组NTHI的所有成员攻击区域3多样性之前,在这里对LB1或LPD-LB1(f)2,1,3特异性的血清对龙猫进行被动免疫。还分析了转移的血清库以获得滴度,特异性和几种功能活性。我们发现这两个血清库具有介导C'依赖性杀伤和抑制NTHI菌株对人口咽细胞粘附的等效能力。当被动转移时,两个血清池均显着抑制了由三种挑战菌株中的任何一种引起的中耳炎的体征和发生率(P≤0.01)。尽管提供了抗疾病的保护,但这些抗血清从鼻咽中完全清除NTHI的能力在NTHI组之间并不相同。因此,这些数据表明,尽早从鼻咽中彻底清除NTHI具有高度保护性,但将细菌负荷降低至临界阈值水平以下似乎同样有效。

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