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胰岛素样生长因子-II转基因小鼠的身体成分改变及多种恶性肿瘤发生频率增加。

Altered body composition and increased frequency of diverse malignancies in insulin-like growth factor-II transgenic mice.

作者信息

Rogler C E, Yang D, Rossetti L, Donohoe J, Alt E, Chang C J, Rosenfeld R, Neely K, Hintz R

机构信息

Marion Bessin Liver Research Center, Albert Einstein College of Medicine, Bronx, New York 10461.

出版信息

J Biol Chem. 1994 May 13;269(19):13779-84.

PMID:7514593
Abstract

The physiological role of insulin-like growth factor (IGF) II (IGF-II) in adult humans is poorly understood. Rather high levels of IGF-II persist in adult human serum, whereas, in rodents, IGF-II levels are very low. To investigate the physiological and carcinogenic effects of persistently elevated IGF-II in adults, we have produced two lines of transgenic mice in which high levels of IGF-II (20- or 30-fold increase above normal) are persistently maintained in the blood. The transgene is driven by the major urinary protein promoter, and it is highly expressed in the liver and perputial glands in both lines. The adult transgenic mice are smaller than controls, and their body composition is altered. Their lean body mass is reduced by 5-8%, whereas fat mass is reduced between 44 and 77%. The mice expressing the highest level of IGF-II (30x) develop hypoglycemia and hypoinsulinemia and IGF-I levels are normal. Mice in the lower expression line (20-fold elevated IGF-II) develop hypoglycemia progressively over their lifetime. Mice from both lines also develop a diverse spectrum of tumors at a higher frequency than controls after 18 months of age, and the most frequent types of tumors are hepatocellular carcinomas and lymphomas. Squamous cell carcinoma, sarcoma, and thyroid carcinomas also occurred in our test group. The long latent period before tumors arise and the wide spectrum of tumor types suggest that IGF-II may function primarily as a tumor progression factor in mice via autocrine and endocrine mechanisms of action.

摘要

胰岛素样生长因子(IGF)II(IGF-II)在成年人体内的生理作用目前还知之甚少。在成年人类血清中,IGF-II水平持续较高,而在啮齿动物中,IGF-II水平则非常低。为了研究成年期持续升高的IGF-II的生理和致癌作用,我们培育了两系转基因小鼠,其血液中持续维持高水平的IGF-II(比正常水平高20至30倍)。转基因由主要尿蛋白启动子驱动,在两系小鼠的肝脏和包皮腺中均高度表达。成年转基因小鼠比对照小鼠体型小,身体组成也发生了改变。它们的瘦体重减少了5-8%,而脂肪量减少了44%至77%。表达最高水平IGF-II(30倍)的小鼠出现低血糖和低胰岛素血症,而IGF-I水平正常。低表达系(IGF-II升高20倍)的小鼠在其一生中逐渐出现低血糖。两系小鼠在18个月龄后也比对照小鼠更频繁地发生多种肿瘤,最常见的肿瘤类型是肝细胞癌和淋巴瘤。我们的试验组中还出现了鳞状细胞癌、肉瘤和甲状腺癌。肿瘤出现前的长潜伏期和广泛的肿瘤类型表明,IGF-II在小鼠中可能主要通过自分泌和内分泌作用机制作为肿瘤进展因子发挥作用。

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Altered body composition and increased frequency of diverse malignancies in insulin-like growth factor-II transgenic mice.胰岛素样生长因子-II转基因小鼠的身体成分改变及多种恶性肿瘤发生频率增加。
J Biol Chem. 1994 May 13;269(19):13779-84.
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