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The pluripotency regulator Zic3 is a direct activator of the Nanog promoter in ESCs.

机译:多能性调节剂Zic3是ESC中Nanog启动子的直接激活剂。

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The transcription factor Zic3 is required for maintenance of ESC pluripotency. By genome-wide chromatin immunoprecipitation (ChIP-chip) in ESCs, we have identified 379 direct Zic3 targets, many of which are functionally associated with pluripotency, cell cycle, proliferation, oncogenesis, and early embryogenesis. Through a computational analysis of Zic3 target sequences, we have identified a novel Zic3 consensus binding motif (5'-CC(C)/(T) GCTGGG-3'). ChIP results and in vitro DNA binding assays revealed that Zic3 binds with high affinity and specificity on the Nanog promoter. Here, we demonstrate that Zic3 functions as a transcriptional activator of the Nanog promoter in three ways: (a) Nanog transcript levels are sustained with Zic3 overexpression in differentiating ESCs, (b) Zic3 depletion in ESCs downregulates Nanog promoter activity, and (c) Zic3 overexpression leads to increased Nanog promoter activity. Furthermore, the activity of a mutant Nanog promoter with ablated Oct4/Sox2 binding is rescued by Zic3 overexpression to nearly wild-type levels. This indicates that Nanog is a positive transcriptional target of Zic3 in a mechanism that is independent of Oct4/Sox2 binding. Hence, we demonstrate an important pathway for regulation of Nanog expression in pluripotent ESCs through direct activation by Zic3.
机译:转录因子Zic3是维持ESC多能性所必需的。通过全基因组染色质免疫沉淀(ChIP芯片)在ESC中,我们已经确定了379个直接的Zic3靶标,其中许多在功能上与多能性,细胞周期,增殖,肿瘤发生和早期胚胎发生有关。通过对Zic3目标序列的计算分析,我们确定了一个新颖的Zic3共有结合基序(5'-CC(C)/(T)GCTGGG-3')。 ChIP结果和体外DNA结合测定表明Zic3在Nanog启动子上具有高亲和力和特异性结合。在这里,我们证明Zic3通过以下三种方式充当Nanog启动子的转录激活因子:(a)Nanog转录物水平在分化的ESC中通过Zic3过表达得以维持;(b)ESC中的Zic3耗尽下调了Nanog启动子的活性;以及(c) Zic3过表达导致Nanog启动子活性增加。此外,具有消融的Oct4 / Sox2结合的突变Nanog启动子的活性可通过Zic3过表达恢复到接近野生型水平。这表明Nanog是Zic3的阳性转录靶标,其机制与Oct4 / Sox2的结合无关。因此,我们展示了通过Zic3直接激活调节多能ESC中Nanog表达的重要途径。

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