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表达反义胰岛素样生长因子I受体的腺病毒对人肺癌细胞系的抗肿瘤作用。

Antitumor effects of an adenovirus expressing antisense insulin-like growth factor I receptor on human lung cancer cell lines.

作者信息

Lee C T, Wu S, Gabrilovich D, Chen H, Nadaf-Rahrov S, Ciernik I F, Carbone D P

机构信息

Hamon Center for Therapeutic Oncology Research, University of Texas Southwestern Medical Center, Dallas 75235, USA.

出版信息

Cancer Res. 1996 Jul 1;56(13):3038-41.

PMID:8674059
Abstract

Insulin-like growth factors (IGFs) are often essential for the maintenance of the malignant phenotype, and in lung cancer the IGF-I receptor (IGF-Ir) is often expressed at high levels. Stable transfection of antisense plasmids expressing the first 300 bp of the IGF-Ir reduces the tumorigenicity of a variety of tumor cell lines and has been reported to induce systemic antitumor effects on established, non-gene-modified tumors in animal model systems. We have constructed an adenovirus expressing an antisense IGF-Ir (Ad-IGF-Ir/as) in an attempt to develop these observations into a clinical therapeutic approach. A single transduction by Ad-IGF-Ir/as (at a multiplicity of infection of 10:1) decreased the IGF-Ir number by about 50% in human lung cancer cell lines NCI H460 and SCC5, as measured by an 125I-labeled IGF-I competitive binding assay. After the transduction of these human lung cancer cell lines by Ad-IGF-Ir/as, the soft agar clonogenicity was reduced by 84%. The i.p. treatment of nude mice bearing established i.p. NCI H460 cells resulted in prolonged survival compared to that of nude mice treated with a reporter virus. These results suggest that Ad-IGF-Ir/as has a therapeutic effect on established human lung cancer xenografts and may represent an effective and practical cancer gene therapy strategy.

摘要

胰岛素样生长因子(IGFs)通常对维持恶性表型至关重要,在肺癌中,胰岛素样生长因子I受体(IGF-Ir)常常高表达。稳定转染表达IGF-Ir前300 bp的反义质粒可降低多种肿瘤细胞系的致瘤性,并且据报道在动物模型系统中对已形成的、未进行基因修饰的肿瘤具有全身抗肿瘤作用。我们构建了一种表达反义IGF-Ir的腺病毒(Ad-IGF-Ir/as),试图将这些观察结果转化为临床治疗方法。通过125I标记的IGF-I竞争性结合试验测定,Ad-IGF-Ir/as单次转导(感染复数为10:1)可使人类肺癌细胞系NCI H460和SCC5中的IGF-Ir数量减少约50%。用Ad-IGF-Ir/as转导这些人类肺癌细胞系后,软琼脂克隆形成能力降低了84%。与用报告病毒处理的裸鼠相比,对已形成腹腔内NCI H460细胞的裸鼠进行腹腔内治疗可延长其生存期。这些结果表明,Ad-IGF-Ir/as对已形成的人肺癌异种移植瘤具有治疗作用,可能代表一种有效且实用的癌症基因治疗策略。

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