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Artificial 64-Residue HIV-1 Enhancer-Binding Peptide Is a Potent Inhibitor of Viral Replication in HIV-1-Infected Cells

机译:人工的64残基HIV-1增强剂结合肽是HIV-1感染细胞中病毒复制的有效抑制剂。

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摘要

An artificial HIV-1 enhancer-binding peptide was extended by nine consecutive arginine residues at the C-terminus and by the nuclear localization signal of SV40 large T antigen at the N-terminus. The resulting synthetic 64-residue peptide was found to bind to the two enhancers of the HIV-1 long terminal repeat, cross the plasma membrane and the nuclear envelope of human cells, and suppress the HIV-1 enhancer-controlled expression of a green fluorescent protein reporter gene. Moreover, HIV-1 replication is inhibited by this peptide in HIV-1-infected CEM-GFP cells as revealed by HIV-1 p24 ELISA and real-time RT-PCR of HIV-1 RNA. Rapid uptake of this intracellular stable and inhibitory peptide into the cells implies that this peptide may have the potential to attenuate HIV-1 replication in vivo.
机译:人工HIV-1增强剂结合肽在C端延伸了9个连续的精氨酸残基,在N端延伸了SV40大T抗原的核定位信号。发现所得的合成64残基肽与HIV-1长末端重复序列的两个增强子结合,穿过人细胞的质膜和核被膜,并抑制HIV-1增强子控制的绿色荧光的表达。蛋白质报告基因。此外,如HIV-1 p24 ELISA和HIV-1 RNA的实时RT-PCR所揭示的,在HIV-1感染的CEM-GFP细胞中,该肽抑制了HIV-1复制。这种细胞内稳定和抑制性肽迅速吸收到细胞中意味着该肽可能具有减弱体内HIV-1复制的潜力。

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