Cell-type specific profiling of histone post-translational modifications in the adult mouse striatum

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Abstract

Epigenetic gene regulation in the heterogeneous brain remains challenging to decipher with current strategies. Bulk tissue analysis from pooled subjects reflects the average of cell-type specific changes across cell-types and individuals, which obscures causal relationships between epigenetic modifications, regulation of gene expression, and complex pathology. To address these limitations, we optimized a hybrid protocol, ICuRuS, for the isolation of nuclei tagged in specific cell-types and histone post translational modification profiling from the striatum of a single mouse. We combined affinity-based isolation of the medium spiny neuron subtypes, Adenosine 2a Receptor or Dopamine Receptor D1, with cleavage of histone-DNA complexes using an antibody-targeted micrococcal nuclease to release DNA complexes for paired end sequencing. Unlike fluorescence activated cell sorting paired with chromatin immunoprecipitation, ICuRuS allowed for robust epigenetic profiling at cell-type specific resolution. Our analysis provides a framework to understand combinatorial relationships between neuronal-subtype-specific epigenetic modifications and gene expression.

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Carpenter, M. D., Fischer, D. K., Zhang, S., Bond, A. M., Czarnecki, K. S., Woolf, M. T., … Heller, E. A. (2022). Cell-type specific profiling of histone post-translational modifications in the adult mouse striatum. Nature Communications, 13(1). https://doi.org/10.1038/s41467-022-35384-1

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