Liu L, Leaman D, Villalta M, Roberts R M
Department of Biological Sciences, University of Missouri, Columbia 65211, USA.
Mol Endocrinol. 1997 Oct;11(11):1651-8. doi: 10.1210/mend.11.11.9971.
CG is required for maintenance of the corpus luteum during pregnancy in higher primates. As CG is a heterodimeric molecule, some form of coordinated control must be maintained over the transcription of its two subunit genes. We recently found that expression of human CG beta-subunit (hCGbeta) in JAr human choriocarcinoma cells was almost completely silenced by the embryonic transcription factor Oct-3/4, which bound to a unique ACAATAATCA octameric sequence in the hCGbeta gene promoter. Here we report that Oct-3/4 is also a potent inhibitor of hCG alpha-subunit (hCGalpha) expression in JAr cells. Oct-3/4 reduced human GH reporter expression from the -170 hCGalpha promoter in either the presence or absence of cAMP by about 70% in transient cotransfection assays, but had no effect on expression from either the -148 hCGalpha or the -99 hCGalpha promoter. Unexpectedly, no Oct-3/ 4-binding site was identified within the -170 to -148 region of the hCGalpha promoter, although one was found around position -115 by both methylation interference footprinting and electrophoretic mobility shift assays. Site-directed mutagenesis of this binding site destroyed the affinity of the promoter for Oct-3/4, but did not affect repression of the promoter. Therefore, inhibition of hCGalpha gene transcription by Oct-3/4 appears not to involve direct binding of this factor to the site responsible for silencing. When stably transfected into JAr cells, Oct-3/4 reduced the amounts of both endogenous hCGalpha mRNA and protein by 70-80%. Oct-3/4 is therefore capable of silencing both hCGalpha and hCGbeta gene expression. We suggest that as the trophoblast begins to form, reduction of Oct-3/4 expression permits the coordinated onset of transcription from the hCGalpha and hCGbeta genes.
在高等灵长类动物的孕期,维持黄体需要人绒毛膜促性腺激素(CG)。由于CG是一种异源二聚体分子,其两个亚基基因的转录必须保持某种形式的协调控制。我们最近发现,胚胎转录因子Oct-3/4几乎完全沉默了JAr人绒毛膜癌细胞中人CGβ亚基(hCGβ)的表达,该因子与hCGβ基因启动子中一个独特的ACAATAATCA八聚体序列结合。在此我们报告,Oct-3/4也是JAr细胞中hCGα亚基(hCGα)表达的有效抑制剂。在瞬时共转染实验中,无论有无环磷酸腺苷(cAMP),Oct-3/4都使来自-170 hCGα启动子的人生长激素(GH)报告基因表达降低了约70%,但对-148 hCGα或-99 hCGα启动子的表达没有影响。出乎意料的是,在hCGα启动子的-170至-148区域内未发现Oct-3/4结合位点,尽管通过甲基化干扰足迹法和电泳迁移率变动分析在-115位左右发现了一个。该结合位点的定点诱变破坏了启动子对Oct-3/4的亲和力,但不影响启动子的抑制作用。因此,Oct-3/4对hCGα基因转录的抑制似乎不涉及该因子与负责沉默的位点的直接结合。当稳定转染到JAr细胞中时,Oct-3/4使内源性hCGα mRNA和蛋白的量减少了70 - 80%。因此,Oct-3/4能够沉默hCGα和hCGβ基因的表达。我们认为,随着滋养层开始形成,Oct-3/4表达的降低允许hCGα和hCGβ基因转录的协调启动。
