Unknown

Dataset Information

0

Integrating transcription-factor abundance with chromatin accessibility in human erythroid lineage commitment.

ABSTRACT: Master transcription factors (TFs) directly regulate present and future cell states by binding DNA regulatory elements and driving gene-expression programs. Their abundance influences epigenetic priming to different cell fates at the chromatin level, especially in the context of differentiation. In order to link TF protein abundance to changes in TF motif accessibility and open chromatin, we developed InTAC-seq, a method for simultaneous quantification of genome-wide chromatin accessibility and intracellular protein abundance in fixed cells. Our method produces high-quality data and is a cost-effective alternative to single-cell techniques. We showcase our method by purifying bone marrow (BM) progenitor cells based on GATA-1 protein levels and establish high GATA-1-expressing BM cells as both epigenetically and functionally similar to erythroid-committed progenitors.

SUBMITTER: Baskar R 

PROVIDER: S-EPMC9017139 | biostudies-literature | 2022 Mar

REPOSITORIES: biostudies-literature

Json Xml
altmetric image

Publications

Integrating transcription-factor abundance with chromatin accessibility in human erythroid lineage commitment.

Baskar Reema R   Chen Amy F AF   Favaro Patricia P   Reynolds Warren W   Mueller Fabian F   Borges Luciene L   Jiang Sizun S   Park Hyun Shin HS   Kool Eric T ET   Greenleaf William J WJ   Bendall Sean C SC  

Cell reports methods 20220321 3

Master transcription factors (TFs) directly regulate present and future cell states by binding DNA regulatory elements and driving gene-expression programs. Their abundance influences epigenetic priming to different cell fates at the chromatin level, especially in the context of differentiation. In order to link TF protein abundance to changes in TF motif accessibility and open chromatin, we developed InTAC-seq, a method for simultaneous quantification of genome-wide chromatin accessibility and  ...[more]

Similar Datasets

Genomics Integrating transcription factor abundance with chromatin accessibility in human erythroid lineage commitment
2022-03-10 | GSE167934 | GEO
Genomics Integrating transcription factor abundance with chromatin accessibility in human erythroid lineage commitment
| PRJNA705610 | ENA
Unknown Setd1a and NURF mediate chromatin dynamics and gene regulation during erythroid lineage commitment and differentiation.
| S-EPMC5009724 | biostudies-literature
Unknown Genome-Wide Association between Transcription Factor Expression and Chromatin Accessibility Reveals Regulators of Chromatin Accessibility.
| S-EPMC5261565 | biostudies-literature
Unknown Erythroid lineage chromatin accessibility maps facilitate identification and validation of NFIX as a fetal hemoglobin repressor.
| S-EPMC10267139 | biostudies-literature
Unknown Transcription factor AP1 potentiates chromatin accessibility and glucocorticoid receptor binding.
| S-EPMC3138120 | biostudies-literature
Unknown Functional definition of a transcription factor hierarchy regulating T cell lineage commitment.
| S-EPMC7400773 | biostudies-literature
Unknown TRACE: transcription factor footprinting using chromatin accessibility data and DNA sequence.
| S-EPMC7397869 | biostudies-literature
Unknown Quantitative dissection of transcription in development yields evidence for transcription-factor-driven chromatin accessibility.
| S-EPMC7738189 | biostudies-literature
Unknown The transcription factor TCF-1 enforces commitment to the innate lymphoid cell lineage.
| S-EPMC6707869 | biostudies-literature