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携带小鼠抑制素α亚基启动子/猿猴病毒T抗原融合基因的转基因小鼠的性腺肿瘤发生:卵巢肿瘤的特征及促性腺激素反应性颗粒细胞系的建立。

Gonadal tumorigenesis in transgenic mice bearing the mouse inhibin alpha-subunit promoter/simian virus T-antigen fusion gene: characterization of ovarian tumors and establishment of gonadotropin-responsive granulosa cell lines.

作者信息

Kananen K, Markkula M, Rainio E, Su J G, Hsueh A J, Huhtaniemi I T

机构信息

Department of Physiology, University of Turku, Finland.

出版信息

Mol Endocrinol. 1995 May;9(5):616-27. doi: 10.1210/mend.9.5.7565808.

DOI:10.1210/mend.9.5.7565808
PMID:7565808
Abstract

To establish in vivo gonadal tumor models and permanent lines of gonadal somatic cells we produced transgenic (TG) mice expressing the Simian virus (SV) 40 T-antigens (T-ag), driven by 6 or 2.1 kilobase fragments of the mouse inhibin alpha-subunit promoter. Hitherto, altogether 44 TG mice, one of which carried the shorter transgene, have produced gonadal tumors. Two founder females expressing the longer transgene, KK1 and KK3, and three established TG mouse lines were studied in detail. Penetrance of the phenotype in IT6-M and IT6-F mouse lines was 100% (tumors/TG: IT6-M 22/22, IT6-F 14/14). The T-ag mRNA was strongly expressed in the gonads, adrenal glands, pituitary, and brain. The KK-1 and KK-3 ovarian tumor cells immunostained with anti-SV40 large-T antibody. The KK-1 cells possessed high-affinity LH receptors [equilibrium association constant (Ka = 7.8 x 10(10) liters/mol] and responded to human CG by elevated cAMP and progesterone production. Also FSH slightly stimulated their cAMP and estradiol production (P < 0.01). These cells expressed cytochrome P450arom and inhibin alpha mRNA, but not cytochrome P450c17 alpha. In conclusion, the KK-1 cells are immortalized luteinizing granulosa cells expressing endogenous gonadotropin receptors, steroidogenic enzymes, and inhibin alpha. These cells will be useful in studies on the molecular aspects of granulosa cell function. The present study indicates that the 6-kilobase fragment of the inhibin alpha promoter described in this article contains the elements directing tissue-specific expression in vivo and is useful for targeted expression of other genes in the gonads.

摘要

为建立体内性腺肿瘤模型和性腺体细胞永久系,我们制备了转基因(TG)小鼠,其表达由小鼠抑制素α亚基启动子的6或2.1千碱基片段驱动的猿猴病毒(SV)40 T抗原(T-ag)。迄今为止,总共44只TG小鼠产生了性腺肿瘤,其中1只携带较短的转基因。对两只表达较长转基因的奠基雌性小鼠KK1和KK3以及三个已建立的TG小鼠品系进行了详细研究。IT6-M和IT6-F小鼠品系中表型的发生率为100%(肿瘤/TG:IT6-M为22/22,IT6-F为14/14)。T-ag mRNA在性腺、肾上腺、垂体和脑中强烈表达。KK-1和KK-3卵巢肿瘤细胞用抗SV40大T抗体进行免疫染色。KK-1细胞具有高亲和力的促黄体生成素受体[平衡缔合常数(Ka = 7.8 x 10(10)升/摩尔],并通过升高的环磷酸腺苷(cAMP)和孕酮产生对人绒毛膜促性腺激素(hCG)作出反应。促卵泡生成素(FSH)也轻微刺激其cAMP和雌二醇产生(P < 0.01)。这些细胞表达细胞色素P450芳香化酶和抑制素α mRNA,但不表达细胞色素P450c17α。总之,KK-1细胞是永生化的促黄体化颗粒细胞,表达内源性促性腺激素受体、类固醇生成酶和抑制素α。这些细胞将有助于颗粒细胞功能分子方面的研究。本研究表明,本文所述的抑制素α启动子的6千碱基片段包含在体内指导组织特异性表达的元件,并且可用于性腺中其他基因的靶向表达。

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