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首页> 外文期刊>Virology >HAdV-2-suppressed growth of SV40 T antigen-transformed mouse mammary epithelial cell-induced tumours in SCID mice
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HAdV-2-suppressed growth of SV40 T antigen-transformed mouse mammary epithelial cell-induced tumours in SCID mice

机译:HAdV-2抑制SCID小鼠中SV40 T抗原转化的小鼠乳腺上皮细胞诱导的肿瘤的生长

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摘要

Human adenovirus (HAdV) vectors are promising tools for cancer therapy, but the shortage of efficient animal models for productive HAdV infections has restricted the evaluation of systemic effects to mainly immunodeficient mice. Previously, we reported a highly efficient replication of HAdV-2 in a non-tumorigenic mouse mammary epithelial cell line, NMuMG. Here we show that HAdV-2 gene expression and progeny formation in NMuMG cells transformed with the SV40 T antigen (NMuMG-T cells) were as efficient as in the parental NMuMG cells. Injection of HAdV-2 into tumours established by NMuMG-T in SCID mice caused reduced tumour growth and signs of intratumoural lesions. HAdV-2 replicated within the NMuMG-T-established tumours, but not in interspersed host-derived tissues within the tumours. The specific infection of NMuMG-T-derived tumours was verified by the lack of viral DNA in kidney, lung or spleen although low levels of viral DNA was occasionally found in liver. (C) 2015 Elsevier Inc. All rights reserved.
机译:人腺病毒(HAdV)载体是用于癌症治疗的有前途的工具,但是缺乏有效的生产性HAdV感染动物模型的应用已经限制了对主要免疫缺陷小鼠的全身作用的评估。以前,我们报道了HAdV-2在非致瘤性小鼠乳腺上皮细胞系NMuMG中的高效复制。在这里,我们显示在用SV40 T抗原转化的NMuMG细胞(NMuMG-T细胞)中,HAdV-2基因表达和子代形成与在亲本NMuMG细胞中一样有效。在SCID小鼠中由NMuMG-T建立的肿瘤中注射HAdV-2导致肿瘤生长减少和肿瘤内病变的迹象。 HAdV-2在NMuMG-T建立的肿瘤中复制,但在散布的宿主来源的组织中不复制。肾脏,肺或脾脏中病毒DNA的缺乏证实了NMuMG-T来源的肿瘤的特异性感染,尽管偶尔在肝脏中发现病毒DNA的水平较低。 (C)2015 Elsevier Inc.保留所有权利。

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