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初次免疫对不可分型流感嗜血杆菌肺部清除的影响。

Effect of primary immunization on pulmonary clearance of nontypable Haemophilus influenzae.

作者信息

McGehee J L, Radolf J D, Toews G B, Hansen E J

机构信息

Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas 75235.

出版信息

Am J Respir Cell Mol Biol. 1989 Sep;1(3):201-10. doi: 10.1165/ajrcmb/1.3.201.

Abstract

Nontypable Haemophilus influenzae (NTHI) is being increasingly recognized as a cause of both adult pneumonia and acute infectious exacerbations in chronic bronchitis. We used a mouse model to study the immune enhancement of pulmonary clearance of NTHI after a primary immunization. BALB/c mice were immunized with whole NTHI either by intraperitoneal (i.p.) or intratracheal (i.t.) routes. There was 10-fold more NTHI-directed antibody detected in the serum of the i.p.-immunized mice than in the serum from the i.t.-immunized animals. Western blot analysis revealed that these antibodies were directed against both NTHI lipooligosaccharide and the various outer membrane proteins of NTHI. The development of NTHI-directed antibodies in serum was associated with significant enhancement of early pulmonary clearance of NTHI. Six hours after delivery of an endobronchial challenge with NTHI, the i.p.-immunized mice had cleared most of the organisms from their lungs, while the i.t.-immunized mice did not clear NTHI any more rapidly than did unimmunized mice. Serum from the i.p.-immunized mice caused more than 99% uptake of NTHI in an in vitro opsonophagocytic assay, while serum from i.t.-immunized mice stimulated little or no phagocytosis of this organism. Opsonophagocytosis of NTHI was obtained with bronchoalveolar lavage (BAL) fluid collected from i.p.-immunized mice 6 h after, but not before, an endobronchial challenge with NTHI. Intravenous injection of an opsonic IgG monoclonal antibody directed against NTHI lipooligosaccharide resulted in both the appearance of this antibody in the alveolar spaces of the unperturbed lung and enhanced pulmonary clearance of NTHI. These data indicate that the i.p. (systemic) route of immunization is more effective than the i.t. route in establishing pulmonary immunity to NTHI in this model system. Furthermore, immune enhancement of clearance of NTHI from the lungs after a primary immunization apparently results from the exudation of opsonic and bactericidal antibodies from the serum into the alveolae in response to the inflammatory challenge.

摘要

不可分型流感嗜血杆菌(NTHI)日益被认为是成人肺炎和慢性支气管炎急性感染加重的病因。我们使用小鼠模型研究初次免疫后肺部清除NTHI的免疫增强作用。将BALB/c小鼠通过腹腔内(i.p.)或气管内(i.t.)途径用完整的NTHI进行免疫。在经腹腔免疫的小鼠血清中检测到的针对NTHI的抗体比经气管内免疫的动物血清中的抗体多10倍。蛋白质印迹分析表明,这些抗体针对NTHI脂寡糖和NTHI的各种外膜蛋白。血清中针对NTHI的抗体的产生与早期肺部清除NTHI的显著增强相关。在用NTHI进行支气管内攻击6小时后,经腹腔免疫的小鼠已从其肺部清除了大部分细菌,而经气管内免疫的小鼠清除NTHI的速度并不比未免疫的小鼠更快。在体外调理吞噬试验中,经腹腔免疫的小鼠血清导致NTHI的摄取率超过99%,而经气管内免疫的小鼠血清几乎没有刺激对该细菌的吞噬作用。在用NTHI进行支气管内攻击6小时后(而非攻击前),从经腹腔免疫的小鼠收集的支气管肺泡灌洗(BAL)液可实现对NTHI的调理吞噬作用。静脉注射针对NTHI脂寡糖的调理IgG单克隆抗体导致该抗体出现在未受干扰的肺部肺泡空间中,并增强了肺部对NTHI的清除。这些数据表明,在该模型系统中,腹腔内(全身)免疫途径在建立针对NTHI的肺部免疫方面比气管内途径更有效。此外,初次免疫后肺部清除NTHI的免疫增强显然是由于血清中调理和杀菌抗体响应炎症刺激而渗出到肺泡中所致。

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