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Down-regulation of HIV-1 long terminal repeat controlled viral transcription by DNA-binding,arginine-rich fusion proteins derived from HIV-1 TAT for the direct delivery into the nucleus

机译：通过DNA结合的HIV-1长末端重复受控病毒转录的下调，从HIV-1 TAT衍生的精氨酸富融合蛋白，用于直接输送到细胞核中

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Modern biomedical research has shown that the majority of human diseases are based on cellular diseases.Thus,biomedical research is focusedon this cellular level to define the molecular reasons followed by the development of concept and chemical structures to target the disease.

机译：现代化的生物医学研究表明，大多数人类疾病都是基于细胞疾病的。生物医学研究是焦点这种细胞水平，以定义分子原因，然后开发概念和化学结构以靶向疾病。

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《the International Peptide Symposium》|2001年||共2页
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Stefan R.K.Hoffmann;
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入库时间 2022-08-20 19:26:44

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专利

1. 含HIV-1 Tat基因重组反转录病毒表达载体构建与表达Tat蛋白功能检测 [J] . 卢春, 钱超, 唐桂霞, 生物医学研究杂志（英文版） . 2003,第006期
2. Kaposi's sarcoma associated herpes virus-encoded viral FLICE inhibitory protein activates transcription from HIV-1 Long Terminal Repeat via the classical NF-κB pathway and functionally cooperates with Tat [J] . Qinmiao Sun, Hittu Matta, Preet M Chaudhary Retrovirology . 2005,第S1期

机译：卡波济氏肉瘤相关疱疹病毒编码的病毒FLICE抑制蛋白通过经典的NF-κB途径激活HIV-1长末端重复序列的转录并在功能上与Tat合作
3. cAMP Signaling Enhances HIV-1 Long Terminal Repeat (LTR)-directed Transcription and Viral Replication in Bone Marrow Progenitor Cells [J] . Anupam Banerjee, Luna Li, Vanessa Pirrone, Clinical Medicine Insights: Pathology . 2017,第8期

机译：cAMP信号增强了骨髓祖细胞中HIV-1长末端重复（LTR）定向转录和病毒复制。
4. cAMP signaling enhances HIV-1 long terminal repeat (LTR)-directed transcription and viral replication in human bone marrow progenitor cells [J] . Banerjee Anupam, Li Luna, Pirrone Vanessa, Journal of neurovirology . 2016,第Suppla1期

机译：cAMP信号增强人类骨髓祖细胞中HIV-1长末端重复（LTR）定向的转录和病毒复制
5. Down-regulation of HIV-1 long terminal repeat controlled viral transcription by DNA-binding,arginine-rich fusion proteins derived from HIV-1 TAT for the direct delivery into the nucleus [C] . Stefan R.K.Hoffmann the International Peptide Symposium . 2001

机译：通过DNA结合的HIV-1长末端重复受控病毒转录的下调，从HIV-1 TAT衍生的精氨酸富融合蛋白，用于直接输送到细胞核中
6. Incorporation of integrase-LexA fusion proteins into HIV-1 and analysis of resulting virions, a strategy for achieving site-directed integration in vivo. [D] . Holmes, Michelle Lynne. 2000

机译：将整合酶-LexA融合蛋白整合到HIV-1中并分析所得病毒体，这是在体内实现定点整合的一种策略。
7. Kaposis sarcoma associated herpes virus-encoded viral FLICE inhibitory protein activates transcription from HIV-1 Long Terminal Repeat via the classical NF-κB pathway and functionally cooperates with Tat [O] . Qinmiao Sun, Hittu Matta, Preet M Chaudhary 2005

机译：卡波济氏肉瘤相关疱疹病毒编码的病毒FLICE抑制蛋白通过经典的NF-κB途径激活HIV-1长末端重复序列的转录并在功能上与Tat合作
8. Kaposi's sarcoma associated herpes virus-encoded viral FLICE inhibitory protein activates transcription from HIV-1 Long Terminal Repeat via the classical NF-κB pathway and functionally cooperates with Tat [O] . Sun, Qinmiao, Matta, Hittu, Chaudhary, Preet M 2005

机译：卡波济氏肉瘤相关疱疹病毒编码的病毒FLICE抑制蛋白通过经典的NF-κB途径激活HIV-1长末端重复序列的转录并在功能上与Tat合作
9. Enhanced HIV-1 Replication in Retinoid-Treated Monocytes. Retinoid EffectsMediated through Mechanisms Related to Cell Differentiation and to a Direct Transcriptional Action on Viral Gene Expression [R] . Turpin, J. A., Meltzer, M. S. 1992

机译：维甲酸处理的单核细胞中HIV-1复制增强。通过与细胞分化相关的机制介导的类视黄醇效应和对病毒基因表达的直接转录作用

Down-regulation of HIV-1 long terminal repeat controlled viral transcription by DNA-binding,arginine-rich fusion proteins derived from HIV-1 TAT for the direct delivery into the nucleus

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