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实验性麻疹。I. 正常宿主和免疫宿主中的发病机制。

Experimental measles. I. Pathogenesis in the normal and the immunized host.

作者信息

McChesney M B, Miller C J, Rota P A, Zhu Y D, Antipa L, Lerche N W, Ahmed R, Bellini W J

机构信息

California Regional Primate Research Center, University of California, Davis 95616, USA.

出版信息

Virology. 1997 Jun 23;233(1):74-84. doi: 10.1006/viro.1997.8576.

Abstract

An animal model to study measles pathogenesis and the correlates of protective immunity was established using rhesus monkeys. A measles isolate, obtained during an epidemic of measles in the primate colony at the University of California, Davis, was passaged through rhesus monkeys and amplified in rhesus mononuclear cells to create a pathogenic virus stock. Sequence analysis of the nucleoprotein and hemagglutinin genes of this isolate revealed strong homology with the Chicago 89 strain of measles virus. Conjunctival/intranasal inoculation of juvenile rhesus monkeys with this virus resulted in skin rash, pneumonia, and systemic infection with dissemination to other mucosal sites and to the lymphoid tissues. Inflammation and necrosis occurred in the lungs and lymphoid tissues and many cell types were infected with measles virus on Day 7 postinoculation (p.i.). The most commonly infected cell type was the B lymphocyte in lymphoid follicles. Measles antigen was found in follicular dendritic cells on Day 14 p.i. In contrast to naive monkeys infected with measles virus, animals vaccinated with the attenuated Moraten strain did not develop clinical or pathologic signs of measles after challenge. However, moderate to marked hyperplasia occurred in the lymph nodes and spleen of a vaccinated animal on Day 7 after pathogenic virus challenge, suggesting that an effective measles vaccine limits but does not prevent infection with wild-type measles virus.

摘要

利用恒河猴建立了一种用于研究麻疹发病机制及保护性免疫相关因素的动物模型。从加利福尼亚大学戴维斯分校灵长类动物群落麻疹流行期间分离得到的一株麻疹病毒,经恒河猴传代并在恒河猴单核细胞中扩增,从而制备出致病性病毒储备株。对该分离株的核蛋白和血凝素基因进行序列分析,发现其与麻疹病毒芝加哥89株具有高度同源性。用该病毒对幼年恒河猴进行结膜/鼻内接种后,出现皮疹、肺炎以及病毒播散至其他黏膜部位和淋巴组织的全身感染。接种后第7天,肺和淋巴组织出现炎症和坏死,许多细胞类型感染了麻疹病毒。最常被感染的细胞类型是淋巴滤泡中的B淋巴细胞。接种后第14天,在滤泡树突状细胞中发现了麻疹抗原。与感染麻疹病毒的未免疫猴子不同,接种减毒莫拉坦株疫苗的动物在受到攻击后未出现麻疹的临床或病理体征。然而,在致病性病毒攻击后第7天,接种疫苗的动物的淋巴结和脾脏出现中度至明显的增生,这表明有效的麻疹疫苗可限制但不能预防野生型麻疹病毒的感染。

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