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新生大鼠肺炎球菌肺部清除功能受损。

Impaired pulmonary clearance of pneumococci in neonatal rats.

作者信息

Coonrod J D, Jarrells M C, Bridges R B

机构信息

Department of Medicine, Veterans Administration Medical Center, Lexington, Kentucky.

出版信息

Pediatr Res. 1987 Dec;22(6):736-42. doi: 10.1203/00006450-198712000-00025.

Abstract

Lung infections are a common cause of morbidity and mortality in neonates. To evaluate neonatal lung defenses against pneumococci, we challenged rats with aerosols of encapsulated pneumococci in an airborne infection apparatus. Whereas adult rats cleared greater than 95% of inhaled type 1 or type 25 pneumococci within 4 h, pneumococci proliferated in the lungs of newborn rats and reached 200-600% of the baseline value by 4 h and 1000-1700% by 24 h. As neonatal rats matured, their ability to clear inhaled pneumococci improved, but compared with adults some impairment in clearance was present until approximately 4 wk of age. Newborn rats had significantly fewer resident alveolar macrophages per g of lung tissue than did adults (p less than 0.001). Although the number of resident macrophages increased with time, a significant deficit in alveolar macrophages persisted for the first 3 wk of life (p less than 0.01). Aerosols of pneumococci caused an influx of granulocytes into the lungs of adult rats within 4 h, compared with 24 h for neonatal rats. Even at 24 h after pneumococcal challenge, newborn rats had significantly fewer granulocytes per g of lung tissue (p less than 0.05) than did adults, although 7-day-old rats had reached an adult level by this time. Significant (p less than 0.05) increases in granulocyte chemotactic activity were observed in lavage fluids of adult, but not newborn, rats after pneumococcal challenge. Thus, impaired clearance of pneumococcal aerosols by neonatal rats was associated with an age-dependent deficiency in numbers of resident alveolar macrophages and impaired generation of chemotactic activity and recruitment of granulocytes to the lung.

摘要

肺部感染是新生儿发病和死亡的常见原因。为了评估新生儿肺部对肺炎球菌的防御能力,我们在空气传播感染装置中用包裹性肺炎球菌气雾剂对大鼠进行了挑战。成年大鼠在4小时内清除了超过95%吸入的1型或25型肺炎球菌,而肺炎球菌在新生大鼠的肺部增殖,到4小时时达到基线值的200 - 600%,到24小时时达到1000 - 1700%。随着新生大鼠的成熟,它们清除吸入肺炎球菌的能力有所提高,但与成年大鼠相比,在大约4周龄之前清除能力仍存在一些损害。每克肺组织中,新生大鼠的驻留肺泡巨噬细胞数量明显少于成年大鼠(p < 0.001)。虽然驻留巨噬细胞的数量随时间增加,但在出生后的前3周,肺泡巨噬细胞仍存在显著不足(p < 0.01)。肺炎球菌气雾剂在4小时内使成年大鼠肺部有粒细胞流入,而新生大鼠则需要24小时。即使在肺炎球菌攻击后24小时,每克肺组织中新生大鼠的粒细胞数量仍明显少于成年大鼠(p < 0.05),尽管7日龄大鼠此时已达到成年水平。肺炎球菌攻击后,在成年大鼠而非新生大鼠的灌洗液中观察到粒细胞趋化活性显著(p < 0.05)增加。因此,新生大鼠对肺炎球菌气雾剂清除能力受损与驻留肺泡巨噬细胞数量的年龄依赖性不足、趋化活性生成受损以及粒细胞向肺部募集受损有关。

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