@article {Winick-Ng2020.04.02.020990, author = {Warren Winick-Ng and Alexander Kukalev and Izabela Harabula and Luna Zea Redondo and Mandy Meijer and Leonid Serebreni and Simona Bianco and Dominik Szabo and Andrea M. Chiariello and Ibai Irastorza Azcarate and Luca Fiorillo and Francesco Musella and Christoph Thieme and Ehsan Irani and Elena Torlai Triglia and Aleksandra A. Kolodziejczyk and Andreas Abentung and Galina Apostolova and Eleanor J. Paul and Vedran Franke and Rieke Kempfer and Altuna Akalin and Sarah Teichmann and Georg Dechant and Mark A. Ungless and Mario Nicodemi and Gon{\c c}alo Castelo-Branco and Ana Pombo}, title = {Cell-type specialization in the brain is encoded by specific long-range chromatin topologies}, elocation-id = {2020.04.02.020990}, year = {2020}, doi = {10.1101/2020.04.02.020990}, publisher = {Cold Spring Harbor Laboratory}, abstract = {Neurons and oligodendrocytes are terminally differentiated cells that perform highly specialized functions, which depend on cascades of gene activation and repression to retain homeostatic control over a lifespan. Gene expression is regulated by three-dimensional (3D) genome organisation, from local levels of chromatin compaction to the organisation of topological domains and chromosome compartments. Whereas our understanding of 3D genome architecture has vastly increased in the past decade, it remains difficult to study specialized cells in their native environment without disturbing their activity. To develop the application of Genome Architecture Mapping (GAM) in small numbers of specialized cells in complex tissues, we combined GAM with immunoselection. We applied immunoGAM to map the genome architecture of specific cell populations in the juvenile/adult mouse brain: dopaminergic neurons (DNs) from the midbrain, pyramidal glutamatergic neurons (PGNs) from the hippocampus, and oligodendrocyte lineage cells (OLGs) from the cortex. We integrate 3D genome organisation with single-cell transcriptomics data, and find specific chromatin structures that relate with cell-type specific patterns of gene expression. We discover abundant changes in compartment organisation, especially a strengthening of heterochromatin compartments which establish strong contacts spanning tens of megabases, especially in brain cells. These compartments contain olfactory and taste receptor genes, which are de-repressed in a subpopulation of PGNs with molecular signatures of long-term potentiation (LTP). We also show extensive reorganisation of topological domains where activation of neuronal or oligodendrocyte genes coincides with formation of new TAD borders. Finally, we discover loss of TAD organisation, or {\textquoteleft}TAD melting{\textquoteright}, at long (\>1Mb) neuronal genes when they are most highly expressed. Our work shows that the 3D organisation of the genome is highly cell-type specific in terminally differentiated cells of the brain, and essential to better understand brain-specific mechanisms of gene regulation.}, URL = {https://www.biorxiv.org/content/early/2020/04/02/2020.04.02.020990}, eprint = {https://www.biorxiv.org/content/early/2020/04/02/2020.04.02.020990.full.pdf}, journal = {bioRxiv} }