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小鼠植入前发育过程中TATA盒利用的发育变化。

Developmental change in TATA-box utilization during preimplantation mouse development.

作者信息

Davis W, Schultz R M

机构信息

Department of Biology, University of Pennsylvania, Philadelphia, Pennsylvania 19104-6018, USA.

出版信息

Dev Biol. 2000 Feb 15;218(2):275-83. doi: 10.1006/dbio.1999.9486.

Abstract

Activation of the embryonic genome during preimplantation mouse development is characterized by a marked reprogramming of gene expression that is essential for further development. Expression of the protein translation initiation factor eIF-1A gene is driven by a proximal TATA-containing promoter and a distal TATA-less promoter. Using specific amplification of cDNA ends that resolves transcripts derived from the TATA-less and TATA-containing promoters, we find that 70% of the eIF-1A transcripts are derived from the TATA-containing promoter in the fully-grown oocyte. Activation of the embryonic genome during the two-cell stage is accompanied by a change in promoter utilization such that only 25% of the transcripts are now derived from the TATA-containing promoter, i.e., 75% are derived from the TATA-less promoter. When one-cell embryos are cultured to the two-cell stage in the presence of alpha-amanitin, this change in transcript abundance is not observed, i.e., the distribution of transcripts is similar to that observed in the oocyte. By the blastocyst stage only 5% of the transcripts are generated from the TATA-containing promoter. If the change in TATA-box utilization for the eIF-1A reflects an underlying global change in TATA-box utilization, a dramatic change in promoter utilization may occur during preimplantation development such that TATA-less promoters are more efficiently utilized. Such a change in promoter utilization could contribute significantly to the reprogramming of gene expression that occurs during the maternal-to-zygotic transition.

摘要

在小鼠着床前发育过程中,胚胎基因组的激活以基因表达的显著重编程为特征,这对进一步发育至关重要。蛋白质翻译起始因子eIF - 1A基因的表达由近端含TATA的启动子和远端不含TATA的启动子驱动。通过特异性扩增cDNA末端来解析源自不含TATA和含TATA启动子的转录本,我们发现,在完全成熟的卵母细胞中,70%的eIF - 1A转录本源自含TATA的启动子。在二细胞阶段胚胎基因组的激活伴随着启动子利用的变化,使得现在只有25%的转录本源自含TATA的启动子,即75%源自不含TATA的启动子。当单细胞胚胎在α-鹅膏蕈碱存在的情况下培养到二细胞阶段时,未观察到转录本丰度的这种变化,即转录本的分布与在卵母细胞中观察到的相似。到囊胚阶段时,只有5%的转录本由含TATA的启动子产生。如果eIF - 1A的TATA框利用变化反映了TATA框利用的潜在全局变化,那么在着床前发育过程中可能会发生启动子利用的显著变化,使得不含TATA的启动子得到更有效的利用。这种启动子利用的变化可能对母源-合子转变期间发生的基因表达重编程有重大贡献。

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