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Genome-wide CTCF distribution in vertebrates defines equivalent sites that aid the identification of disease-associated genes

Author: A Achiron
A Alcina
A Barski
A Ragvin
AE Handel
AI Su
AM Bushey
Ana Fernández Miñán
Antonio Alcina
B Hemmer
B Rhead
Christian Valdes-Quezada
Cristina Pantoja
D Blankenberg
D Blankenberg
D Martin
DA Hafler
DA Kleinjan
David Martin
DJ Epstein
ED Rubio
Eduardo Moltó
Elisa de la Calle-Mustienes
F Hsu
F Recillas-Targa
F Recillas-Targa
F Zambelli
Fernando Casares
Fuencisla Matesanz
Félix Recillas-Targa
G Elgar
GN Filippova
H Rincón-Arano
H Yao
I Ovcharenko
IA Hoppenbrouwers
Ivan Ovcharenko
J Bessa
J Dekker
JA Wallace
JD Phelan
JE Phillips
José Luis Gómez-Skarmeta
JR Oksenberg
K Ishihara
KS Wendt
L Guelen
Leila Taher
Lluís Montoliu
M Escamilla-Del-Arenal
Manuel Serrano
María A Blasco
María Fedetz
Mayra Furlan-Magaril
Miguel Manzanares
MJ Pikaart
N Nègre
N Shubin
NK Wilson
Orlando Domínguez
Ozren Bogdanović
Paulo S Pereira
R Jothi
R Ohlsson
Roderic Guigó
S Cuddapah
S Gonzalez
S Hoffjan
Susana Cañón
T Ravasi
TA Manolio
TL Bailey
TS Mikkelsen
V Matys
V Parelho
VV Lunyak
X Chen
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2011
Field of study

Many genomic alterations associated with human diseases localize in noncoding regulatory elements located far from the promoters they regulate, making it challenging to link noncoding mutations or risk-associated variants with target genes. The range of action of a given set of enhancers is thought to be defined by insulator elements bound by the 11 zinc-finger nuclear factor CCCTC-binding protein (CTCF). Here we analyzed the genomic distribution of CTCF in various human, mouse and chicken cell types, demonstrating the existence of evolutionarily conserved CTCF-bound sites beyond mammals. These sites preferentially flank transcription factor–encoding genes, often associated with human diseases, and function as enhancer blockers in vivo, suggesting that they act as evolutionarily invariant gene boundaries. We then applied this concept to predict and functionally demonstrate that the polymorphic variants associated with multiple sclerosis located within the EVI5 gene impinge on the adjacent gene GFI1.This research was supported by the following grants: BFU2007-60042/BMC, BFU2010-14839, Petri PET2007_0158, CONSOLIDER CSD2007-00008 (Spanish Ministerio de Ciencia e Innovación (MICINN)) and Proyecto de Excelencia CVI-3488 (Junta de Andalucía) to J.L.G.-S.; BFU2009-07044 (MICINN) and Proyecto de Excelencia CVI 2658 (Junta de Andalucía) to F.C.; FIS PI081636 (ISCIII) to F.M.; PN-SAF2009-11491 (MICINN) and Proyecto de Excelencia P07-CVI-02551 (Junta de Andalucía) to A.A.; BFU2008-00838, CONSOLIDER CSD2007-00008 (MICINN), Regional Government of Madrid (CAM S-SAL-0190-2006) and the Pro-CNIC Foundation to M.M.; BFU2006-12185 and BIO2009-12697 (MICINN) to L.M.; Dirección General de Asuntos del Personal Académico, Universidad Nacional Autónoma de México (IN209403, IN214407 and IN203811) and Consejo Nacional de Ciencia y Tecnología, México (CONACyT: 42653-Q, 58767 and 128464) to F.R.-T.; Intramural Research Program of the US NCBI (NIH) to I.O. and BIO2006-03380, CONSOLIDER CSD2007-00050 (MICINN) and RETICS RD07/0067/0012 (Spanish MICINN) to R.G. L.M. thanks A. Fernández for technical assistance and L. Barrios for statistical analysis. F.R.-T. thanks G.G. Avendaño for technical assistance

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