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在成年小鼠中建立肺炎链球菌鼻咽定植模型。

Establishment of a Streptococcus pneumoniae nasopharyngeal colonization model in adult mice.

作者信息

Wu H Y, Virolainen A, Mathews B, King J, Russell M W, Briles D E

机构信息

Department of Microbiology, Bevill Biomedical Research Building, University of Alabama at Birmingham, Birmingham, AL 35294, USA.

出版信息

Microb Pathog. 1997 Sep;23(3):127-37. doi: 10.1006/mpat.1997.0142.

Abstract

Human nasopharyngeal carriage of Streptococcus pneumoniae constitutes the major natural reservoir of pneumococci and is thought to be the prelude to virtually all pneumococcal disease. If carriage could be greatly reduced, pneumococcal transmission and disease could be largely eliminated. To facilitate the studies of mechanisms important in carriage and to identify immunogens that can elicit protection against carriage, we characterized an adult mouse model of nasopharyngeal carriage. Non-anaesthetized mice were inoculated intranasally with pneumococci in 10 microl of fluid. Nasopharyngeal carriage was observed with strains of capsular types 3, 4, 6A, 6B, 14, 19, and 23. Carriage was stable over time, and the numbers of pneumococci carried were relatively independent of inoculation dose; findings which indicate that the recovery of pneumococci from 1 day to 2 weeks post inoculation was dependent on colonization, rather than just temporary contamination. To ensure carriage in the largest percentage of mice, without causing sepsis or death, inoculations of 10(7) colony forming units (cfu) should be used. In this model, carriage was generally observed without concomitant bacteremia or sepsis and carriage was observed even with strains that were avirulent when injected i.v. The model should be useful for the identification of protection-eliciting antigens, since intranasal immunization with heat-killed pneumococci or lysates of pneumococci protected against carriage.

摘要

人类鼻咽部肺炎链球菌携带是肺炎链球菌的主要自然储存库,被认为几乎是所有肺炎球菌疾病的前奏。如果携带率能大幅降低,肺炎球菌的传播和疾病在很大程度上就能消除。为了便于研究携带过程中重要的机制,并确定能引发针对携带的保护作用的免疫原,我们对一种成年小鼠鼻咽部携带模型进行了特征描述。未麻醉的小鼠经鼻内接种10微升液体中的肺炎球菌。观察到3型、4型、6A 型、6B型、14型、19型和23型荚膜菌株的携带情况。携带情况随时间稳定,携带的肺炎球菌数量相对独立于接种剂量;这些发现表明,接种后1天至2周内肺炎球菌的恢复取决于定植,而不仅仅是暂时污染。为了确保在最大比例的小鼠中出现携带情况,又不引起败血症或死亡,应使用10⁷ 集落形成单位(cfu)进行接种。在这个模型中,通常观察到携带情况而无伴随的菌血症或败血症,即使是静脉注射无毒性的菌株也能观察到携带情况。该模型对于鉴定能引发保护作用的抗原应该是有用的,因为用热灭活的肺炎球菌或肺炎球菌裂解物进行鼻内免疫可预防携带。

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