HIV-1-encoded antisense RNA suppresses viral replication for a prolonged period

HIV-1-encoded antisense RNA suppresses viral replication for a prolonged period

<p>Abstract</p> <p>Background</p> <p>Recent evidence proposes a novel concept that mammalian natural antisense RNAs play important roles in cellular homeostasis by regulating the expression of several genes. Identification and characterization of retroviral antisense RN...

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Main Authors: Kobayashi-Ishihara Mie, Yamagishi Makoto, Hara Takuma, Matsuda Yuka, Takahashi Ryutaro, Miyake Ariko, Nakano Kazumi, Yamochi Tadanori, Ishida Takaomi, Watanabe Toshiki
Format: Article
Language:English
Published: BMC 2012-05-01
Series:Retrovirology
Online Access:http://www.retrovirology.com/content/9/1/38
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spelling doaj-53ec0b8beab0410ea5cfeb2e40921f372020-11-25T00:35:00ZengBMCRetrovirology1742-46902012-05-01913810.1186/1742-4690-9-38HIV-1-encoded antisense RNA suppresses viral replication for a prolonged periodKobayashi-Ishihara MieYamagishi MakotoHara TakumaMatsuda YukaTakahashi RyutaroMiyake ArikoNakano KazumiYamochi TadanoriIshida TakaomiWatanabe Toshiki<p>Abstract</p> <p>Background</p> <p>Recent evidence proposes a novel concept that mammalian natural antisense RNAs play important roles in cellular homeostasis by regulating the expression of several genes. Identification and characterization of retroviral antisense RNA would provide new insights into mechanisms of replication and pathogenesis. HIV-1 encoded-antisense RNAs have been reported, although their structures and functions remain to be studied. We have tried to identify and characterize antisense RNAs of HIV-1 and their function in viral infection.</p> <p>Results</p> <p>Characterization of transcripts of HEK293T cells that were transiently transfected with an expression plasmid with HIV-1<sub>NL4–3</sub> DNA in the antisense orientation showed that various antisense transcripts can be expressed. By screening and characterizing antisense RNAs in HIV-1<sub>NL4–3</sub>-infected cells, we defined the primary structure of a major form of HIV-1 antisense RNAs, which corresponds to a variant of previously reported <it>ASP</it> mRNA. This 2.6 kb RNA was transcribed from the U3 region of the 3′ LTR and terminated at the <it>env</it> region in acutely or chronically infected cell lines and acutely infected human peripheral blood mononuclear cells. Reporter assays clearly demonstrated that the HIV-1 LTR harbours promoter activity in the reverse orientation. Mutation analyses suggested the involvement of NF-κΒ binding sites in the regulation of antisense transcription. The antisense RNA was localized in the nuclei of the infected cells. The expression of this antisense RNA suppressed HIV-1 replication for more than one month. Furthermore, the specific knockdown of this antisense RNA enhanced HIV-1 gene expression and replication.</p> <p>Conclusions</p> <p>The results of the present study identified an accurate structure of the major form of antisense RNAs expressed from the HIV-1<sub>NL4–3</sub> provirus and demonstrated its nuclear localization. Functional studies collectively demonstrated a new role of the antisense RNA in viral replication. Thus, we suggest a novel viral mechanism that self-limits HIV-1 replication and provides new insight into the viral life cycle.</p> http://www.retrovirology.com/content/9/1/38
collection DOAJ
language English
format Article
sources DOAJ
author Kobayashi-Ishihara Mie
Yamagishi Makoto
Hara Takuma
Matsuda Yuka
Takahashi Ryutaro
Miyake Ariko
Nakano Kazumi
Yamochi Tadanori
Ishida Takaomi
Watanabe Toshiki
spellingShingle Kobayashi-Ishihara Mie
Yamagishi Makoto
Hara Takuma
Matsuda Yuka
Takahashi Ryutaro
Miyake Ariko
Nakano Kazumi
Yamochi Tadanori
Ishida Takaomi
Watanabe Toshiki
HIV-1-encoded antisense RNA suppresses viral replication for a prolonged period
Retrovirology
author_facet Kobayashi-Ishihara Mie
Yamagishi Makoto
Hara Takuma
Matsuda Yuka
Takahashi Ryutaro
Miyake Ariko
Nakano Kazumi
Yamochi Tadanori
Ishida Takaomi
Watanabe Toshiki
author_sort Kobayashi-Ishihara Mie
title HIV-1-encoded antisense RNA suppresses viral replication for a prolonged period
title_short HIV-1-encoded antisense RNA suppresses viral replication for a prolonged period
title_full HIV-1-encoded antisense RNA suppresses viral replication for a prolonged period
title_fullStr HIV-1-encoded antisense RNA suppresses viral replication for a prolonged period
title_full_unstemmed HIV-1-encoded antisense RNA suppresses viral replication for a prolonged period
title_sort hiv-1-encoded antisense rna suppresses viral replication for a prolonged period
publisher BMC
series Retrovirology
issn 1742-4690
publishDate 2012-05-01
description <p>Abstract</p> <p>Background</p> <p>Recent evidence proposes a novel concept that mammalian natural antisense RNAs play important roles in cellular homeostasis by regulating the expression of several genes. Identification and characterization of retroviral antisense RNA would provide new insights into mechanisms of replication and pathogenesis. HIV-1 encoded-antisense RNAs have been reported, although their structures and functions remain to be studied. We have tried to identify and characterize antisense RNAs of HIV-1 and their function in viral infection.</p> <p>Results</p> <p>Characterization of transcripts of HEK293T cells that were transiently transfected with an expression plasmid with HIV-1<sub>NL4–3</sub> DNA in the antisense orientation showed that various antisense transcripts can be expressed. By screening and characterizing antisense RNAs in HIV-1<sub>NL4–3</sub>-infected cells, we defined the primary structure of a major form of HIV-1 antisense RNAs, which corresponds to a variant of previously reported <it>ASP</it> mRNA. This 2.6 kb RNA was transcribed from the U3 region of the 3′ LTR and terminated at the <it>env</it> region in acutely or chronically infected cell lines and acutely infected human peripheral blood mononuclear cells. Reporter assays clearly demonstrated that the HIV-1 LTR harbours promoter activity in the reverse orientation. Mutation analyses suggested the involvement of NF-κΒ binding sites in the regulation of antisense transcription. The antisense RNA was localized in the nuclei of the infected cells. The expression of this antisense RNA suppressed HIV-1 replication for more than one month. Furthermore, the specific knockdown of this antisense RNA enhanced HIV-1 gene expression and replication.</p> <p>Conclusions</p> <p>The results of the present study identified an accurate structure of the major form of antisense RNAs expressed from the HIV-1<sub>NL4–3</sub> provirus and demonstrated its nuclear localization. Functional studies collectively demonstrated a new role of the antisense RNA in viral replication. Thus, we suggest a novel viral mechanism that self-limits HIV-1 replication and provides new insight into the viral life cycle.</p>
url http://www.retrovirology.com/content/9/1/38
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