| Literature DB >> 30811995 |
Nicolas Merienne1, Cécile Meunier2, Anne Schneider3, Jonathan Seguin3, Satish S Nair4, Anne B Rocher5, Stéphanie Le Gras6, Céline Keime6, Richard Faull7, Luc Pellerin8, Jean-Yves Chatton9, Christian Neri4, Karine Merienne3, Nicole Déglon10.
Abstract
The role of brain cell-type-specific functions and profiles in pathological and non-pathological contexts is still poorly defined. Such cell-type-specific gene expression profiles in solid, adult tissues would benefit from approaches that avoid cellular stress during isolation. Here, we developed such an approach and identified highly selective transcriptomic signatures in adult mouse striatal direct and indirect spiny projection neurons, astrocytes, and microglia. Integrating transcriptomic and epigenetic data, we obtained a comprehensive model for cell-type-specific regulation of gene expression in the mouse striatum. A cross-analysis with transcriptomic and epigenomic data generated from mouse and human Huntington's disease (HD) brains shows that opposite epigenetic mechanisms govern the transcriptional regulation of striatal neurons and glial cells and may contribute to pathogenic and compensatory mechanisms. Overall, these data validate this less stressful method for the investigation of cellular specificity in the adult mouse brain and demonstrate the potential of integrative studies using multiple databases.Entities:
Keywords: HD patients; HD transgenic mice; Huntington’s disease; cell-type-specific profiling; epigenetics; striatum; transcriptomics
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Year: 2019 PMID: 30811995 DOI: 10.1016/j.celrep.2019.02.003
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423