| Literature DB >> 31152164 |
Kevin Grosselin1,2,3, Adeline Durand4,5, Justine Marsolier4,5, Adeline Poitou1,6, Elisabetta Marangoni5, Fariba Nemati5, Ahmed Dahmani5, Sonia Lameiras7, Fabien Reyal5,8,9, Olivia Frenoy1,10, Yannick Pousse1, Marcel Reichen1,11, Adam Woolfe1, Colin Brenan1,12, Andrew D Griffiths13, Céline Vallot14,15, Annabelle Gérard16.
Abstract
Modulation of chromatin structure via histone modification is a major epigenetic mechanism and regulator of gene expression. However, the contribution of chromatin features to tumor heterogeneity and evolution remains unknown. Here we describe a high-throughput droplet microfluidics platform to profile chromatin landscapes of thousands of cells at single-cell resolution. Using patient-derived xenograft models of acquired resistance to chemotherapy and targeted therapy in breast cancer, we found that a subset of cells within untreated drug-sensitive tumors share a common chromatin signature with resistant cells, undetectable using bulk approaches. These cells, and cells from the resistant tumors, have lost chromatin marks-H3K27me3, which is associated with stable transcriptional repression-for genes known to promote resistance to treatment. This single-cell chromatin immunoprecipitation followed by sequencing approach paves the way to study the role of chromatin heterogeneity, not just in cancer but in other diseases and healthy systems, notably during cellular differentiation and development.Entities:
Mesh:
Substances:
Year: 2019 PMID: 31152164 DOI: 10.1038/s41588-019-0424-9
Source DB: PubMed Journal: Nat Genet ISSN: 1061-4036 Impact factor: 38.330