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表达大鼠抑制素α亚基的转基因小鼠的性腺病理学

Gonadal pathologies in transgenic mice expressing the rat inhibin alpha-subunit.

作者信息

McMullen M L, Cho B N, Yates C J, Mayo K E

机构信息

Department of Biochemistry, Molecular Biology, and Cell Biology, Northwestern University, Evanston, Illinois 60208, USA.

出版信息

Endocrinology. 2001 Nov;142(11):5005-14. doi: 10.1210/endo.142.11.8472.

Abstract

Inhibin and activin are structurally related dimeric peptide hormones and are members of the TGF-beta superfamily of proteins. In the accompanying paper, we describe transgenic mice that overexpress the inhibin alpha-subunit gene from a metallothionein-I promoter (MT-alpha) and examine the effects of the MT-alpha transgene on gonadotropin levels and fertility. To characterize the effects of increased inhibin alpha-subunit on gonadal morphology and function, in this report we investigate gonadal histology, steroid hormone levels, and the basis of ovarian cyst formation in MT-alpha transgenic mice. MT-alpha transgenic female mice develop large fluid-filled ovarian cysts of follicular origin as early as 3 months of age. By 12 months of age, more than 92% of female MT-alpha transgenic mice develop ovarian cysts compared with less than 25% of wild-type littermates. Ovarian cysts form unilaterally or bilaterally, and cystic ovaries often have a greatly expanded bursal sac. Additionally, the ovaries of MT-alpha transgenic mice contain polyovular follicles and have fewer mature antral follicles and corpora lutea. MT-alpha female mice exhibit abnormal steroid hormone production, with increased serum T levels and reductions in serum E with corresponding reductions in uterine mass. In the MT-alpha transgenic males, testis size was decreased by 20-40% compared with control males, and there is a corresponding reduction in seminiferous tubule volume. After a chronic treatment with a GnRH antagonist, MT-alpha female mice continued to develop ovarian cysts and bursal sac expansions, although the cysts were markedly reduced in size. These results indicate that the expression of the rat inhibin alpha-subunit in mice results in significant ovarian pathology, reduced testicular size, and altered ovarian steroidogenesis. The antagonist studies are consistent with a direct ovarian effect of the alpha-subunit transgene product mediated by changes in the inhibin-to-activin ratio in these mice.

摘要

抑制素和激活素是结构相关的二聚体肽类激素,属于转化生长因子-β(TGF-β)超家族蛋白成员。在随附论文中,我们描述了从金属硫蛋白-I启动子(MT-α)过表达抑制素α亚基基因的转基因小鼠,并研究了MT-α转基因对促性腺激素水平和生育力的影响。为了表征抑制素α亚基增加对性腺形态和功能的影响,在本报告中,我们研究了MT-α转基因小鼠的性腺组织学、类固醇激素水平以及卵巢囊肿形成的基础。MT-α转基因雌性小鼠早在3月龄时就会形成起源于卵泡的充满液体的大型卵巢囊肿。到12月龄时,超过92%的MT-α转基因雌性小鼠出现卵巢囊肿,而野生型同窝小鼠的这一比例不到25%。卵巢囊肿单侧或双侧形成,囊性卵巢的囊状囊通常会大幅扩张。此外,MT-α转基因小鼠的卵巢含有多卵卵泡,成熟的窦状卵泡和黄体较少。MT-α雌性小鼠表现出异常的类固醇激素产生,血清睾酮(T)水平升高,血清雌二醇(E)水平降低,子宫重量相应减轻。在MT-α转基因雄性小鼠中,睾丸大小比对照雄性小鼠减小了20%-40%,生精小管体积也相应减小。用促性腺激素释放激素(GnRH)拮抗剂进行慢性治疗后,MT-α雌性小鼠继续形成卵巢囊肿和囊状囊扩张,尽管囊肿大小明显减小。这些结果表明,大鼠抑制素α亚基在小鼠中的表达导致了显著的卵巢病变、睾丸大小减小以及卵巢类固醇生成改变。拮抗剂研究结果与这些小鼠中抑制素与激活素比例变化介导的α亚基转基因产物对卵巢的直接作用一致。

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