Genome-wide cancer-specific chromatin accessibility patterns derived from archival processed xenograft tumors

Author:

Marcel Shelsa S.ORCID,Quimby Austin L.,Noel Melodie P.,Jaimes Oscar C.,Mehrab-Mohseni Marjan,Ashur Suud A.,Velasco Brian,Tsuruta James K.,Kasoji Sandeep K.,Santos Charlene M.,Dayton Paul A.ORCID,Parker Joel S.ORCID,Davis Ian J.ORCID,Pattenden Samantha G.ORCID

Abstract

Chromatin accessibility states that influence gene expression and other nuclear processes can be altered in disease. The constellation of transcription factors and chromatin regulatory complexes in cells results in characteristic patterns of chromatin accessibility. The study of these patterns in tissues has been limited because existing chromatin accessibility assays are ineffective for archival formalin-fixed, paraffin-embedded (FFPE) tissues. We have developed a method to efficiently extract intact chromatin from archival tissue via enhanced cavitation with a nanodroplet reagent consisting of a lipid shell with a liquid perfluorocarbon core. Inclusion of nanodroplets during the extraction of chromatin from FFPE tissues enhances the recovery of intact accessible and nucleosome-bound chromatin. We show that the addition of nanodroplets to the chromatin accessibility assay formaldehyde-assisted isolation of regulatory elements (FAIRE), does not affect the accessible chromatin signal. Applying the technique to FFPE human tumor xenografts, we identified tumor-relevant regions of accessible chromatin shared with those identified in primary tumors. Further, we deconvoluted non-tumor signal to identify cellular components of the tumor microenvironment. Incorporation of this method of enhanced cavitation into FAIRE offers the potential for extending chromatin accessibility to clinical diagnosis and personalized medicine, while also enabling the exploration of gene regulatory mechanisms in archival samples.

Funder

National Cancer Institute

NCI

National Institutes of Health

National Institute of Environmental Health Sciences

University Cancer Research Fund, and North Carolina Biotechnology Center

NIH

National Institute of General Medical Sciences

North Carolina Translational and Clinical Sciences Institute

North Carolina Biotechnology Center

Publisher

Cold Spring Harbor Laboratory

Subject

Genetics(clinical),Genetics

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