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Automatic identification of informative regions with epigenomic changes associated to hematopoiesis

View ORCID ProfileEnrique Carrillo-de-Santa-Pau, View ORCID ProfileDavid Juan, View ORCID ProfileVera Pancaldi, Felipe Were, View ORCID ProfileIgnacio Martin-Subero, View ORCID ProfileDaniel Rico, View ORCID ProfileAlfonso Valencia, on behalf of The BLUEPRINT Consortium
doi: https://doi.org/10.1101/082917
Enrique Carrillo-de-Santa-Pau
1Structural Biology and BioComputing Programme, Spanish National Cancer Research Centre (CNIO)
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David Juan
1Structural Biology and BioComputing Programme, Spanish National Cancer Research Centre (CNIO)
2Institut de Biologia Evolutiva, Consejo Superior de Investigaciones Científicas–Universitat Pompeu Fabra, Parc de Recerca Biomèdica de Barcelona, Barcelona, Catalonia 08003, Spain
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Vera Pancaldi
1Structural Biology and BioComputing Programme, Spanish National Cancer Research Centre (CNIO)
3Barcelona Supercomputing Centre (BSC), Barcelona, Spain.
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Felipe Were
1Structural Biology and BioComputing Programme, Spanish National Cancer Research Centre (CNIO)
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Ignacio Martin-Subero
4Institut d’Investigacions Biomédiques August Pi i Sunyer (IDIBAPS), Department of Anatomic Pathology, Pharmacology and Microbiology, University of Barcelona, Barcelona, Spain.
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Daniel Rico
5Institute of Cellular Medicine, Newcastle University, Newcastle upon Tyne, United Kingdom.
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  • For correspondence: daniel.rico@newcastle.ac.uk alfonso.valencia@bsc.es
Alfonso Valencia
1Structural Biology and BioComputing Programme, Spanish National Cancer Research Centre (CNIO)
3Barcelona Supercomputing Centre (BSC), Barcelona, Spain.
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  • For correspondence: daniel.rico@newcastle.ac.uk alfonso.valencia@bsc.es
8Member of International Human Epigenome Consortium (IHEC). For more information, see and
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Abstract

Hematopoiesis is one of the best characterized biological systems but the connection between chromatin changes and lineage differentiation is not yet well understood. We have developed a bioinformatic workflow to generate a chromatin space that allows to classify forty-two human healthy blood epigenomes from the BLUEPRINT, NIH ROADMAP and ENCODE consortia by their cell type. This approach let us to distinguish different cells types based on their epigenomic profiles, thus recapitulating important aspects of human hematopoiesis. The analysis of the orthogonal dimension of the chromatin space identify 32,662 chromatin determinant regions (CDRs), genomic regions with different epigenetic characteristics between the cell types. Functional analysis revealed that these regions are linked with cell identities. The inclusion of leukemia epigenomes in the healthy hematological chromatin sample space gives us insights on the healthy cell types that are more epigenetically similar to the disease samples. Further analysis of tumoral epigenetic alterations in hematopoietic CDRs points to sets of genes that are tightly regulated in leukemic transformations and commonly mutated in other tumors. Our method provides an analytical approach to study the relationship between epigenomic changes and cell lineage differentiation. Method availability: https://github.com/david-juan/ChromDet

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Posted June 20, 2017.
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Automatic identification of informative regions with epigenomic changes associated to hematopoiesis
Enrique Carrillo-de-Santa-Pau, David Juan, Vera Pancaldi, Felipe Were, Ignacio Martin-Subero, Daniel Rico, Alfonso Valencia, on behalf of The BLUEPRINT Consortium
bioRxiv 082917; doi: https://doi.org/10.1101/082917
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Automatic identification of informative regions with epigenomic changes associated to hematopoiesis
Enrique Carrillo-de-Santa-Pau, David Juan, Vera Pancaldi, Felipe Were, Ignacio Martin-Subero, Daniel Rico, Alfonso Valencia, on behalf of The BLUEPRINT Consortium
bioRxiv 082917; doi: https://doi.org/10.1101/082917

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