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Down regulation of human immunodeficiency virus type-1 (HIV-1) expression by Vif antisense RNA expression vectors in transfected cells.

作者信息

Barnor Jacob Samson, Miyano-Kurosaki Naoko, Yamaguchi Kazuya, Kobayashi Hiroki, Ishikawa Koichi, Osei-Kwasi Mubarak, Ampofo William Kwabina, Ofori-Adjei David, Inagaki Yoshio, Yamamoto Naoki, Takaku Hiroshi

机构信息

Department of Industrial Chemistry, Chiba Institute of Technology, Tsudanuma, Narashino, Chiba 275-0016, Japan.

出版信息

Nucleic Acids Res Suppl. 2002(2):123-4. doi: 10.1093/nass/2.1.123.

Abstract

The HIV-1 vif gene is a potential candidate in the quest for anti-retroviral interventions, due to its unique role in the target cell infection. We employed the antisense RNA strategy to determine the antiviral activity of intracellularly expressed anti-sense RNAs of various lengths complementary to the targeted HIV-1 vif gene. Expression vectors mediating the delivery of the vif-ORF, 5'-Vif, M-vif, and 3'-vif antisense RNAs under the CMV promoter were constructed using pcDNA 3.1. The COS cells transfected with the antisense vectors showed a steady-state of antisense RNA expression levels. In contrast, those co-transfected with the Infectious molecular clone, pNL-E, exhibited a significant reduction in the steady-state antisense RNA levels, which correlated with a significant reduction in p24 antigen production. Thus, this expression method for these antisense RNAs provides a promising gene therapy strategy for HIV-1.

摘要

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