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TRANSGENIC MOUSE LINES EXPRESSING HUMAN ACE2 AND USES THEREOF

机译:表达人类ACE2的转基因小鼠品系及其用途

摘要

Animal models for severe acute respiratory syndrome (SARS)-coronavirus infection of humans are needed to elucidate SARS pathogenesis and develop vaccines and antivirals. Transgenic mice were developed expressing human angiotensin-converting enzyme 2, a functional receptor for the virus, under the regulation of a global promoter. A transgenic lineage, designated AC70, was among the best characterized against SARS coronavirus infection, showing weight loss and other clinical manifestations before reaching 100% mortality within 8 days after intranasal infection. High virus titers were detected in the lungs and brains of transgene-positive mice on days 1 and 3 after infection. Inflammatory mediators were also detected in these tissues, coinciding with high levels of virus replication. In contrast, infected transgene-negative mice survived without showing any clinical illness. The severity of the disease developed in these transgenic mice, AC70 in particular, makes these mouse models valuable not only for evaluating the efficacy of antivirals and vaccines, but also for studying SARS coronavirus pathogenesis and infection by other coronaviruses utilizing human ACE2 for viral entry into cells.
机译:需要用于人类的严重急性呼吸综合征(SARS)-冠状病毒感染的动物模型,以阐明SARS的发病机理并开发疫苗和抗病毒药。在整体启动子的调控下,开发了表达人血管紧张素转化酶2(该病毒的功能性受体)的转基因小鼠。命名为AC70的转基因谱系是抗SARS冠状病毒感染的最佳特征之一,在鼻内感染后8天内达到100%的死亡率之前显示出体重减轻和其他临床表现。在感染后第1天和第3天,在转基因阳性小鼠的肺和脑中检测到高病毒滴度。在这些组织中还检测到炎性介质,这与高水平的病毒复制相吻合。相反,感染的转基因阴性小鼠存活下来,没有表现出任何临床疾病。这些转基因小鼠(尤其是AC70)所患疾病的严重性,使其不仅对评估抗病毒药和疫苗的效力具有重要价值,而且对于研究SARS冠状病毒的发病机理以及其他利用人类ACE2进入病毒的冠状病毒的感染也具有重要意义。细胞。

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