医学
癌症
全身给药
病毒复制
癌症研究
效价
病毒载体
药理学
病毒学
病毒
免疫学
生物
内科学
基因
体内
生物化学
生物技术
重组DNA
作者
Carla Heise,Alan M Williams,Shengli Xue,Matthew Stephen Propst,David H. Kirn
出处
期刊:PubMed
日期:1999-06-01
卷期号:59 (11): 2623-8
被引量:104
摘要
Replication-incompetent viral vectors are being developed for the gene therapy of cancer. Although some of these may eventually be proven to have significant localized antitumoral activity, none to date have been shown to infect and cause regression of established tumors following i.v. administration. Because cancer is a systemic disease in almost all fatal cases, the lack of i.v. efficacy is a major limitation to treatment with replication-incompetent viral vectors. ONYX-015 (d11520) is an attenuated adenovirus that replicates in and causes selective lysis of cancer cells. We carried out i.v. efficacy and distribution studies in nude mice with s.c. and intraparenchymal tumor xenografts. ONYX-015 infected and replicated efficiently within tumors following i.v. administration. Viral titers in livers were relatively high 3 h after administration but decreased rapidly, becoming undetectable after 24 h. Effective antitumor doses were not associated with hepatic toxicity. Viral replication within tumors was associated with regressions in several tumor models. Selectively replicating viruses like ONYX-015 hold promise as agents to treat metastatic cancer.
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