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Retroviral transduction of the human c-Ha-ras-1 oncogene into midgestation mouse embryos promotes rapid epithelial hyperplasia.

机译:人类c-Ha-ras-1癌基因逆转录病毒转入妊娠中期小鼠胚胎会促进快速上皮增生。

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摘要

Infection of mouse embryos at 8 days of gestation with a replication-defective retrovirus carrying the human c-Ha-ras-1 oncogene led to efficient and rapid induction of hyperplastic lesions. Twenty-four percent of viable off-spring developed abnormal growths after infection with purified virus. The lesions contained a single integrated provirus and produced viral RNA and the Ha-ras oncogene product (p21). The latency period between the time of infection and appearance of the lesions suggested that secondary alterations in addition to activated ras were necessary for neoplasms to develop. The earliest and most abundant growths were cutaneous and appeared from 4 to 36 weeks of age, with a median of 4 weeks of age. A number of subcutaneous lesions also developed over the same time span but at a median of 18 weeks of age. The rapid development of cutaneous lesions in response to transduction of the ras oncogene contrasts with other studies in which adult skin required secondary treatment with promoters prior to ras induction of epithelial hyperplasia. These results demonstrate that infection of midgestation mouse embryos allows rapid analysis of oncogene potency in skin.
机译:在妊娠8天时,带有人类c-Ha-ras-1癌基因的复制缺陷型逆转录病毒感染小鼠胚胎导致了增生性病变的快速有效诱导。感染纯病毒后,有24%的后代有异常生长。病变包含单个整合的原病毒,并产生病毒RNA和Ha-ras癌基因产物(p21)。感染时间与病变出现之间的潜伏期表明,除了活化的ras外,继发性改变对于肿瘤的形成是必要的。最早且最丰富的生长是皮肤性的,出现于4至36周龄,中位数为4周龄。在同一时间跨度也出现了许多皮下病变,但中位年龄为18周。响应于ras癌基因的转导,皮肤病变的快速发展与其他研究相反,在该研究中,成年皮肤在ras诱导上皮增生之前需要用启动子进行二次治疗。这些结果表明,妊娠中期小鼠胚胎的感染可以快速分析皮肤中癌基因的效力。

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