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免疫血清对小鼠布鲁氏菌病病程的影响。

Immune serum-mediated effects on brucellosis evolution in mice.

作者信息

Plommet M, Plommet A M

出版信息

Infect Immun. 1983 Jul;41(1):97-105. doi: 10.1128/iai.41.1.97-105.1983.

Abstract

Immune serum injected into mice before a footpad challenge of virulent strain Brucella abortus 544 can prevent dissemination of infection to the spleen. Sera from mice infected with Brucella for at least 2 months or from mice vaccinated with a protein-bound cell wall peptidoglycan Brucella fraction completely stopped dissemination. Brucella lipopolysaccharide and polysaccharide cross-reacting Yersinia immune sera reduced dissemination. Both peptidoglycan and lipopolysaccharide immune sera injected simultaneously with an intravenous challenge caused a shift in Brucella from spleen to liver. When immune sera were injected simultaneously with an intravenous challenge, the kinetics of splenic infection showed two effects: an early one, optimally measured at day 7 postchallenge, showed reduced numbers in the spleen due to the shift of Brucella to the liver; a late effect, measured at day 21 postchallenge, showed reduced numbers in spleen and liver with nearly complete clearance by day 49 postchallenge. Brucella lipopolysaccharide and cross-reacting bacterial antisera induced the early effect only, whereas peptidoglycan and infected mouse sera induced both effects. When peptidoglycan immune serum was injected 2 or 7 days after intravenous challenge, the late effect was somewhat reduced. Hence, immune sera to protein and polysaccharide surface antigens can (i) prevent dissemination of systemic infection and (ii) help destroy intercellular bacteria (protein antigen only). These effects may represent a large part of vaccinal immunity.

摘要

在对小鼠进行强毒株布鲁氏菌544足垫攻击之前注射免疫血清,可防止感染扩散至脾脏。来自感染布鲁氏菌至少2个月的小鼠或接种结合蛋白的细胞壁肽聚糖布鲁氏菌组分的小鼠的血清可完全阻止感染扩散。布鲁氏菌脂多糖和多糖交叉反应耶尔森氏菌免疫血清可减少感染扩散。与静脉内攻击同时注射肽聚糖和脂多糖免疫血清会导致布鲁氏菌从脾脏转移至肝脏。当与静脉内攻击同时注射免疫血清时,脾脏感染的动力学表现出两种效应:一种早期效应,在攻击后第7天测量最佳,表现为由于布鲁氏菌转移至肝脏,脾脏中的数量减少;一种晚期效应,在攻击后第21天测量,表现为脾脏和肝脏中的数量减少,到攻击后第49天几乎完全清除。布鲁氏菌脂多糖和交叉反应细菌抗血清仅诱导早期效应,而肽聚糖和感染小鼠血清诱导两种效应。当在静脉内攻击后2天或7天注射肽聚糖免疫血清时,晚期效应会有所降低。因此,针对蛋白质和多糖表面抗原的免疫血清可以(i)防止全身感染的扩散,以及(ii)帮助破坏细胞内细菌(仅蛋白质抗原)。这些效应可能代表了疫苗免疫的很大一部分。

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