Evolution of motif variants and positional bias of the cyclic-AMP response element

BACKGROUND: Transcription factors regulate gene expression by interacting with their specific DNA binding sites. Some transcription factors, particularly those involved in transcription initiation, always bind close to transcription start sites (TSS). Others have no such preference and are functiona...

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Autores principales: Smith, Brandon, Fang, Hung, Pan, Youlian, Walker, P Roy, Famili, A Fazel, Sikorska, Marianna
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2007
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1796609/
https://www.ncbi.nlm.nih.gov/pubmed/17288573
http://dx.doi.org/10.1186/1471-2148-7-S1-S15
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author Smith, Brandon
Fang, Hung
Pan, Youlian
Walker, P Roy
Famili, A Fazel
Sikorska, Marianna
author_facet Smith, Brandon
Fang, Hung
Pan, Youlian
Walker, P Roy
Famili, A Fazel
Sikorska, Marianna
author_sort Smith, Brandon
collection PubMed
description BACKGROUND: Transcription factors regulate gene expression by interacting with their specific DNA binding sites. Some transcription factors, particularly those involved in transcription initiation, always bind close to transcription start sites (TSS). Others have no such preference and are functional on sites even tens of thousands of base pairs (bp) away from the TSS. The Cyclic-AMP response element (CRE) binding protein (CREB) binds preferentially to a palindromic sequence (TGACGTCA), known as the canonical CRE, and also to other CRE variants. CREB can activate transcription at CREs thousands of bp away from the TSS, but in mammals CREs are found far more frequently within 1 to 150 bp upstream of the TSS than in any other region. This property is termed positional bias. The strength of CREB binding to DNA is dependent on the sequence of the CRE motif. The central CpG dinucleotide in the canonical CRE (TGACGTCA) is critical for strong binding of CREB dimers. Methylation of the cytosine in the CpG can inhibit binding of CREB. Deamination of the methylated cytosines causes a C to T transition, resulting in a functional, but lower affinity CRE variant, TGATGTCA. RESULTS: We performed genome-wide surveys of CREs in a number of species (from worm to human) and showed that only vertebrates exhibited a CRE positional bias. We performed pair-wise comparisons of human CREs with orthologous sequences in mouse, rat and dog genomes and found that canonical and TGATGTCA variant CREs are highly conserved in mammals. However, when orthologous sequences differ, canonical CREs in human are most frequently TGATGTCA in the other species and vice-versa. We have identified 207 human CREs showing such differences. CONCLUSION: Our data suggest that the positional bias of CREs likely evolved after the separation of urochordata and vertebrata. Although many canonical CREs are conserved among mammals, there are a number of orthologous genes that have canonical CREs in one species but the TGATGTCA variant in another. These differences are likely due to deamination of the methylated cytosines in the CpG and may contribute to differential transcriptional regulation among orthologous genes.
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spelling pubmed-17966092007-02-09 Evolution of motif variants and positional bias of the cyclic-AMP response element Smith, Brandon Fang, Hung Pan, Youlian Walker, P Roy Famili, A Fazel Sikorska, Marianna BMC Evol Biol Research BACKGROUND: Transcription factors regulate gene expression by interacting with their specific DNA binding sites. Some transcription factors, particularly those involved in transcription initiation, always bind close to transcription start sites (TSS). Others have no such preference and are functional on sites even tens of thousands of base pairs (bp) away from the TSS. The Cyclic-AMP response element (CRE) binding protein (CREB) binds preferentially to a palindromic sequence (TGACGTCA), known as the canonical CRE, and also to other CRE variants. CREB can activate transcription at CREs thousands of bp away from the TSS, but in mammals CREs are found far more frequently within 1 to 150 bp upstream of the TSS than in any other region. This property is termed positional bias. The strength of CREB binding to DNA is dependent on the sequence of the CRE motif. The central CpG dinucleotide in the canonical CRE (TGACGTCA) is critical for strong binding of CREB dimers. Methylation of the cytosine in the CpG can inhibit binding of CREB. Deamination of the methylated cytosines causes a C to T transition, resulting in a functional, but lower affinity CRE variant, TGATGTCA. RESULTS: We performed genome-wide surveys of CREs in a number of species (from worm to human) and showed that only vertebrates exhibited a CRE positional bias. We performed pair-wise comparisons of human CREs with orthologous sequences in mouse, rat and dog genomes and found that canonical and TGATGTCA variant CREs are highly conserved in mammals. However, when orthologous sequences differ, canonical CREs in human are most frequently TGATGTCA in the other species and vice-versa. We have identified 207 human CREs showing such differences. CONCLUSION: Our data suggest that the positional bias of CREs likely evolved after the separation of urochordata and vertebrata. Although many canonical CREs are conserved among mammals, there are a number of orthologous genes that have canonical CREs in one species but the TGATGTCA variant in another. These differences are likely due to deamination of the methylated cytosines in the CpG and may contribute to differential transcriptional regulation among orthologous genes. BioMed Central 2007-02-08 /pmc/articles/PMC1796609/ /pubmed/17288573 http://dx.doi.org/10.1186/1471-2148-7-S1-S15 Text en Copyright © 2007 Smith et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Smith, Brandon
Fang, Hung
Pan, Youlian
Walker, P Roy
Famili, A Fazel
Sikorska, Marianna
Evolution of motif variants and positional bias of the cyclic-AMP response element
title Evolution of motif variants and positional bias of the cyclic-AMP response element
title_full Evolution of motif variants and positional bias of the cyclic-AMP response element
title_fullStr Evolution of motif variants and positional bias of the cyclic-AMP response element
title_full_unstemmed Evolution of motif variants and positional bias of the cyclic-AMP response element
title_short Evolution of motif variants and positional bias of the cyclic-AMP response element
title_sort evolution of motif variants and positional bias of the cyclic-amp response element
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1796609/
https://www.ncbi.nlm.nih.gov/pubmed/17288573
http://dx.doi.org/10.1186/1471-2148-7-S1-S15
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