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通过气管内滴注逆转录病毒反义K-ras构建体预防原位人肺癌生长。

Prevention of orthotopic human lung cancer growth by intratracheal instillation of a retroviral antisense K-ras construct.

作者信息

Georges R N, Mukhopadhyay T, Zhang Y, Yen N, Roth J A

机构信息

Department of Thoracic Surgery, University of Texas M. D. Anderson Cancer Center, Houston 77030.

出版信息

Cancer Res. 1993 Apr 15;53(8):1743-6.

PMID:8467490
Abstract

An orthotopic human lung cancer model in nu/nu mice was used to study the effect of an antisense K-ras (AS-K-ras) retroviral construct on tumor growth in vivo. A 2-kilobase genomic AS-K-ras DNA fragment linked to a beta-actin promoter was cloned into the LNSX retroviral vector. The recombinant construct was packaged into GP+envAm12 cells and titers greater than 10(6) colony-forming units/ml were obtained. Irradiated (350 cGy) nu/nu mice were first inoculated intratracheally with 10(5) H460a human large cell lung carcinoma cells which have a codon 61 mutation of the K-ras oncogene. Three days later they received intratracheal instillation of viral supernatant (5 x 10(6) colony-forming units/ml) from either LNSX, LNSX-AS-K-ras, LNSX-sense-K-ras producer cells, or medium daily for 3 days. At autopsy, 30 days after tumor cell inoculation, 90% of the control mice had tumors whereas 87% of mice treated with the LNSX-AS-K-ras viral supernatant were free of tumors. The efficacy of the viral supernatant was dose dependent. Intratracheal administration of retroviral LNSX-AS-K-ras supernatant prevents the growth of human lung cancer cells implanted orthotopically in nu/nu mice.

摘要

利用裸鼠原位人肺癌模型研究反义K-ras(AS-K-ras)逆转录病毒构建体对体内肿瘤生长的影响。将与β-肌动蛋白启动子相连的2千碱基基因组AS-K-ras DNA片段克隆到LNSX逆转录病毒载体中。将重组构建体包装到GP+envAm12细胞中,获得了滴度大于10(6)集落形成单位/毫升的病毒液。首先给经350 cGy照射的裸鼠气管内接种10(5)个具有K-ras癌基因密码子61突变的H460a人肺大细胞癌细胞。三天后,它们每天接受来自LNSX、LNSX-AS-K-ras、LNSX-正义K-ras产生细胞的病毒上清液(5×10(6)集落形成单位/毫升)气管内滴注,持续3天。在接种肿瘤细胞30天后进行尸检时,90%的对照小鼠有肿瘤,而用LNSX-AS-K-ras病毒上清液处理的小鼠中有87%无肿瘤。病毒上清液的疗效呈剂量依赖性。气管内给予逆转录病毒LNSX-AS-K-ras上清液可抑制原位植入裸鼠体内的人肺癌细胞生长。

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