Functional Studies of CCAAT/Enhancer Binding Protein Site Located Downstream of the Transcriptional Start Site.

Q3 Medicine Clinical Medicine Insights- Pathology Pub Date : 2017-11-15 eCollection Date: 2017-01-01 DOI:10.1177/1179555717694556
Yujie Liu, Michael R Nonnemacher, Aikaterini Alexaki, Vanessa Pirrone, Anupam Banerjee, Luna Li, Evelyn Kilareski, Brian Wigdahl
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引用次数: 3

Abstract

Previous studies have identified a CCAAT/enhancer binding protein (C/EBP) site located downstream of the transcriptional start site (DS3). The role of the DS3 element with respect to HIV-1 transactivation by Tat and viral replication has not been characterized. We have demonstrated that DS3 was a functional C/EBPβ binding site and mutation of this site to the C/EBP knockout DS3-9C variant showed lower HIV-1 long terminal repeat (LTR) transactivation by C/EBPβ. However, it was able to exhibit similar or even higher transcription levels by Tat compared to the parental LTR. C/EBPβ and Tat together further enhanced the transcription level of the parental LAI-LTR and DS3-9C LTR, with higher levels in the DS3-9C LTR. HIV molecular clone viruses carrying the DS3-9C variant LTR demonstrated a decreased replication capacity and delayed rate of replication. These results suggest that DS3 plays a role in virus transcriptional initiation and provides new insight into C/EBP regulation of HIV-1.

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CCAAT/增强子结合蛋白转录起始位点下游的功能研究。
先前的研究已经确定了位于转录起始位点(DS3)下游的CCAAT/增强子结合蛋白(C/EBP)位点。DS3元件在HIV-1被Tat转录激活和病毒复制中的作用尚未被描述。我们已经证明DS3是一个功能性的C/EBPβ结合位点,并且该位点突变为C/EBP敲除的DS3- 9c变体,显示C/EBPβ降低了HIV-1长末端重复(LTR)的转激活。C/EBPβ和Tat共同作用,进一步提高了亲本LAI-LTR和DS3-9C LTR的转录水平,其中DS3-9C LTR的转录水平更高,携带DS3-9C LTR变体的HIV分子克隆病毒表现出复制能力下降和复制速率延迟。这些结果表明DS3在病毒转录起始中起作用,并为C/EBP调控HIV-1提供了新的思路。
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