Inhibiting Gene Expression At Transcription Start Sites In Chromosomal Dna With Antigene Rnas

Bethany A. Janowski; Kenneth E. Huffman; Jacob C. Schwartz; Rosalyn Ram; Daniel Hardy; David S. Shames; John D. Minna; David R. Corey

doi:10.1038/nchembio725

Inhibiting Gene Expression At Transcription Start Sites In Chromosomal Dna With Antigene Rnas

Bethany A. Janowski, Kenneth E. Huffman, Jacob C. Schwartz, Rosalyn Ram, Daniel Hardy, David S. Shames, John D. Minna, David R. Corey

Research output: Contribution to journal › Article › peer-review

153 Scopus citations

Abstract

Transcription start sites are critical switches for converting recognition of chromosomal DNA into active synthesis of RNA. Their functional importance suggests that they may be ideal targets for regulating gene expression. Here, we report potent inhibition of gene expression by antigene RNAs (agRNAs) complementary to transcription start sites within human chromosomal DNA. Silencing does not require methylation of DNA and differs from all known mechanisms for inhibiting transcription. agRNAs overlap DNA sequences within the open complex formed by RNA polymerase, and silencing is acutely sensitive to single base shifts. agRNAs effectively silence both TATA-less and TATA-box-containing promoters. Transcription start sites occur within every gene, providing predictable targets for agRNAs. Potent inhibition of multiple genes suggests that agRNAs may represent a natural mechanism for controlling transcription, may complement siRNAs and miRNAs that target mRNA, and will be valuable agents for silencing gene expression.

Original language	English (US)
Pages (from-to)	180-184
Number of pages	5
Journal	Nature chemical biology
Volume	1
Issue number	4
DOIs	https://doi.org/10.1038/nchembio725
State	Published - Jul 2005

ASJC Scopus subject areas

Molecular Biology
Cell Biology

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title = "Inhibiting Gene Expression At Transcription Start Sites In Chromosomal Dna With Antigene Rnas",

abstract = "Transcription start sites are critical switches for converting recognition of chromosomal DNA into active synthesis of RNA. Their functional importance suggests that they may be ideal targets for regulating gene expression. Here, we report potent inhibition of gene expression by antigene RNAs (agRNAs) complementary to transcription start sites within human chromosomal DNA. Silencing does not require methylation of DNA and differs from all known mechanisms for inhibiting transcription. agRNAs overlap DNA sequences within the open complex formed by RNA polymerase, and silencing is acutely sensitive to single base shifts. agRNAs effectively silence both TATA-less and TATA-box-containing promoters. Transcription start sites occur within every gene, providing predictable targets for agRNAs. Potent inhibition of multiple genes suggests that agRNAs may represent a natural mechanism for controlling transcription, may complement siRNAs and miRNAs that target mRNA, and will be valuable agents for silencing gene expression.",

author = "Janowski, {Bethany A.} and Huffman, {Kenneth E.} and Schwartz, {Jacob C.} and Rosalyn Ram and Daniel Hardy and Shames, {David S.} and Minna, {John D.} and Corey, {David R.}",

note = "Funding Information: This work was supported by the US National Institutes of Health (NIGMS 60642 and 73042 to D.R.C. and Lung Cancer SPORE P50CA70907 to J.D.M.) and the Robert A. Welch Foundation (I-1244 to D.R.C.). We thank M. McPhaul for providing antibody to the androgen receptor.",

year = "2005",

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doi = "10.1038/nchembio725",

language = "English (US)",

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AU - Hardy, Daniel

AU - Shames, David S.

AU - Minna, John D.

AU - Corey, David R.

N1 - Funding Information: This work was supported by the US National Institutes of Health (NIGMS 60642 and 73042 to D.R.C. and Lung Cancer SPORE P50CA70907 to J.D.M.) and the Robert A. Welch Foundation (I-1244 to D.R.C.). We thank M. McPhaul for providing antibody to the androgen receptor.

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N2 - Transcription start sites are critical switches for converting recognition of chromosomal DNA into active synthesis of RNA. Their functional importance suggests that they may be ideal targets for regulating gene expression. Here, we report potent inhibition of gene expression by antigene RNAs (agRNAs) complementary to transcription start sites within human chromosomal DNA. Silencing does not require methylation of DNA and differs from all known mechanisms for inhibiting transcription. agRNAs overlap DNA sequences within the open complex formed by RNA polymerase, and silencing is acutely sensitive to single base shifts. agRNAs effectively silence both TATA-less and TATA-box-containing promoters. Transcription start sites occur within every gene, providing predictable targets for agRNAs. Potent inhibition of multiple genes suggests that agRNAs may represent a natural mechanism for controlling transcription, may complement siRNAs and miRNAs that target mRNA, and will be valuable agents for silencing gene expression.

AB - Transcription start sites are critical switches for converting recognition of chromosomal DNA into active synthesis of RNA. Their functional importance suggests that they may be ideal targets for regulating gene expression. Here, we report potent inhibition of gene expression by antigene RNAs (agRNAs) complementary to transcription start sites within human chromosomal DNA. Silencing does not require methylation of DNA and differs from all known mechanisms for inhibiting transcription. agRNAs overlap DNA sequences within the open complex formed by RNA polymerase, and silencing is acutely sensitive to single base shifts. agRNAs effectively silence both TATA-less and TATA-box-containing promoters. Transcription start sites occur within every gene, providing predictable targets for agRNAs. Potent inhibition of multiple genes suggests that agRNAs may represent a natural mechanism for controlling transcription, may complement siRNAs and miRNAs that target mRNA, and will be valuable agents for silencing gene expression.

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Inhibiting Gene Expression At Transcription Start Sites In Chromosomal Dna With Antigene Rnas

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