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Creation and preliminary characterization of a Tp53 knockout rat

机译:Tp53基因敲除大鼠的创建和初步表征

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The tumor suppressor TP53 plays a crucial role in cancer biology, and the TP53 gene is the most mutated gene in human cancer. Trp53 knockout mouse models have been widely used in cancer etiology studies and in search for a cure of cancer with some limitations that other model organisms might help overcome. Via pronuclear microinjection of zinc finger nucleases (ZFNs), we created a Tp53 knockout rat that contains an 11-bp deletion in exon 3, resulting in a frameshift and premature terminations in the open reading frame. In cohorts of 25 homozygous ( Tp53Δ11/Δ11 ), 37 heterozygous ( Tp53Δ11/+ ) and 30 wild-type rats, the Tp53Δ11/Δ11 rats lived an average of 126 days before death or removal from study because of clinical signs of abnormality or formation of tumors. Half of Tp53Δ11/+ were removed from study by 1 year of age because of tumor formation. Both Tp53Δ11/+ and Tp53Δ11/Δ11 rats developed a wide spectrum of tumors, most commonly sarcomas. Interestingly, there was a strikingly high incidence of brain lesions, especially in Tp53Δ11/Δ11 animals. We believe that this mutant rat line will be useful in studying cancer types rarely observed in mice and in carcinogenicity assays for drug development.
机译:抑癌基因TP53在癌症生物学中起着至关重要的作用,而TP53基因是人类癌症中突变最多的基因。 Trp53基因敲除小鼠模型已广泛用于癌症病因学研究和寻找治愈癌症的方法,但其他模型生物可能会克服这些限制。通过前核显微注射锌指核酸酶(ZFNs),我们创建了一个Tp53基因敲除大鼠,该大鼠在外显子3中含有11bp的缺失,导致移码和开放阅读框中的提前终止。在25个纯合子(Tp53Δ11/Δ11),37个杂合子(Tp53Δ11/ +)和30只野生型大鼠中,由于异常或形成的临床迹象,Tp53Δ11/Δ11大鼠平均死亡或离开研究前平均生活126天。肿瘤。由于肿瘤形成,到1岁时一半的Tp53Δ11/ +被从研究中移除。 Tp53Δ11/ +和Tp53Δ11/Δ11大鼠均出现多种肿瘤,最常见的是肉瘤。有趣的是,脑损伤的发生率非常高,尤其是在Tp53Δ11/Δ11动物中。我们相信,这种突变大鼠系将有助于研究在小鼠中很少观察到的癌症类型以及在药物开发的致癌性分析中。

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