门1
生物
多发性内分泌肿瘤
胰腺
外显子
胰岛素瘤
癌变
β细胞
内分泌学
转基因小鼠
癌症研究
体细胞
内科学
腺瘤
肠内分泌细胞
分子生物学
转基因
内分泌系统
小岛
基因
遗传学
激素
胰岛素
医学
作者
Judy S. Crabtree,Peter C. Scacheri,Jerrold M. Ward,Sara R. McNally,Gary P. Swain,Cristina Montagna,Jeffrey H. Hager,Douglas Hanahan,Helena Edlund,Mark A. Magnuson,Lisa Garrett‐Beal,A. Lee Burns,Thomas Ried,Settara C. Chandrasekharappa,Stephen J. Marx,Allen M. Spiegel,Francis S. Collins
标识
DOI:10.1128/mcb.23.17.6075-6085.2003
摘要
Patients with multiple endocrine neoplasia type 1 (MEN1) develop multiple endocrine tumors, primarily affecting the parathyroid, pituitary, and endocrine pancreas, due to the inactivation of the MEN1 gene. A conditional mouse model was developed to evaluate the loss of the mouse homolog, Men1, in the pancreatic beta cell. Men1 in these mice contains exons 3 to 8 flanked by loxP sites, such that, when the mice are crossed to transgenic mice expressing cre from the rat insulin promoter (RIP-cre), exons 3 to 8 are deleted in beta cells. By 60 weeks of age, >80% of mice homozygous for the floxed Men1 gene and expressing RIP-cre develop multiple pancreatic islet adenomas. The formation of adenomas results in elevated serum insulin levels and decreased blood glucose levels. The delay in tumor appearance, even with early loss of both copies of Men1, implies that additional somatic events are required for adenoma formation in beta cells. Comparative genomic hybridization of beta cell tumor DNA from these mice reveals duplication of chromosome 11, potentially revealing regions of interest with respect to tumorigenesis.
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