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猕猴感染人类呼肠孤病毒BYD1株的实验性感染:一种用于研究严重急性呼吸综合征的动物模型。

Experimental infection of macaques with the human reovirus BYD1 strain: an animal model for the study of the severe acute respiratory syndrome.

作者信息

He Cheng, Pang Wanyong, Yong Xinhao, Zhu Hong, Lei Ming, Duan Qing

机构信息

Laboratory Animal Institute, College of Veterinary Medicine, China Agricultural University, Beijing, People's Republic of China.

出版信息

DNA Cell Biol. 2005 Aug;24(8):491-5. doi: 10.1089/dna.2005.24.491.

Abstract

Experimental studies were performed to determine the role of a newly isolated reovirus (ReoV) from a severe acute respiratory syndrome (SARS) patient in the etiology of this newly described serious respiratory syndrome. Four cynomologus macaques were inoculated with this reovirus (BYD1) in an attempt to replicate the infection and pathology observed in SARS. The body temperature of the infected monkeys was monitored three times a day, and blood and fecal samples were periodically collected for specific immunology determinations. On days 7 and 33 after inoculation, necropsies for pathological accessment and pathogen isolation were performed. The four infected macaques developed a fever on days 3 and 4 after inoculation, and maintainted a febrile state for 4-6 days. The highest temperature in the animals recorded was 40.4 degrees C. After a recovery phase, the macaques developed a second febrile condition. Antibody titers against the reovirus injected by the intravenous route occurred in higher number than those in the nasal cavity. Four macaque monkeys demonstrated diffuse alveolar damage, characterized by hemorrhagic pneumonia, serosanguineous exudates, formation of hyaline membranes, and type II pneumocyte hyperplasia, which were similar to those that have been noted in SARS patients. Lymphocytes decreased in the cortex of the lymph node and in the white pulp of the spleen. ReoV was detected in pneumonic tissue by virus isolation and RT-PCR. The macaques infected with the newly isolated reovirus developed a fever, diffuse alveolar damage and pulmonary interstitial inflammation similar to that noted in SARS patients. This evidence demonstrates that ReoV might have a primary role in the etiology of SARS.

摘要

进行了实验研究,以确定从一名严重急性呼吸综合征(SARS)患者新分离出的呼肠孤病毒(ReoV)在这种新描述的严重呼吸综合征病因中的作用。给四只食蟹猴接种了这种呼肠孤病毒(BYD1),试图复制在SARS中观察到的感染和病理情况。每天监测感染猴子的体温三次,并定期采集血液和粪便样本进行特异性免疫学测定。在接种后第7天和第33天,进行尸检以进行病理评估和病原体分离。四只受感染的食蟹猴在接种后第3天和第4天出现发热,并持续发热4 - 6天。动物记录的最高体温为40.4摄氏度。在恢复期后,食蟹猴出现了第二次发热情况。静脉注射途径注射呼肠孤病毒后的抗体滴度比鼻腔注射后的抗体滴度更高。四只食蟹猴表现出弥漫性肺泡损伤,其特征为出血性肺炎、浆液血性渗出物、透明膜形成和II型肺泡上皮细胞增生,这与在SARS患者中观察到的情况相似。淋巴结皮质和脾脏白髓中的淋巴细胞减少。通过病毒分离和逆转录聚合酶链反应(RT-PCR)在肺部组织中检测到呼肠孤病毒。感染新分离呼肠孤病毒的食蟹猴出现了发热、弥漫性肺泡损伤和肺间质炎症,与SARS患者中观察到的情况相似。这一证据表明,呼肠孤病毒可能在SARS的病因中起主要作用。

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