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High-capacity sample multiplexing for single cell chromatin accessibility profiling.


ABSTRACT: Single-cell chromatin accessibility has emerged as a powerful means of understanding the epigenetic landscape of diverse tissues and cell types, but profiling cells from many independent specimens is challenging and costly. Here we describe a novel approach, sciPlex-ATAC-seq, which uses unmodified DNA oligos as sample-specific nuclear labels, enabling the concurrent profiling of chromatin accessibility within single nuclei from virtually unlimited specimens or experimental conditions. We first demonstrate our method with a chemical epigenomics screen, in which we identify drug-altered distal regulatory sites predictive of compound- and dose-dependent effects on transcription. We then analyze cell type-specific chromatin changes in PBMCs from multiple donors responding to synthetic and allogeneic immune stimulation. We quantify stimulation-altered immune cell compositions and isolate the unique effects of allogeneic stimulation on chromatin accessibility specific to T-lymphocytes. Finally, we observe that impaired global chromatin decondensation often coincides with chemical inhibition of allogeneic T-cell activation.

SUBMITTER: Booth GT 

PROVIDER: S-EPMC10696879 | biostudies-literature | 2023 Dec

REPOSITORIES: biostudies-literature

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High-capacity sample multiplexing for single cell chromatin accessibility profiling.

Booth Gregory T GT   Daza Riza M RM   Srivatsan Sanjay R SR   McFaline-Figueroa José L JL   Gladden Rula Green RG   Mullen Andrew C AC   Furlan Scott N SN   Shendure Jay J   Trapnell Cole C  

BMC genomics 20231204 1


Single-cell chromatin accessibility has emerged as a powerful means of understanding the epigenetic landscape of diverse tissues and cell types, but profiling cells from many independent specimens is challenging and costly. Here we describe a novel approach, sciPlex-ATAC-seq, which uses unmodified DNA oligos as sample-specific nuclear labels, enabling the concurrent profiling of chromatin accessibility within single nuclei from virtually unlimited specimens or experimental conditions. We first d  ...[more]

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