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

Reema Baskar,A.F. Chen,P.M.B. Favaro,W. Reynolds,F. Muller,Luciene Borges,S Jiang,H. Shin Park,E. T. Kool,William J. Greenleaf,Sean C. Bendall

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

2021

Reema Baskar
A.F. Chen
P.M.B. Favaro
W. Reynolds
F. Muller
Luciene Borges
S Jiang
H. Shin Park
E. T. Kool
William J. Greenleaf
Sean C. Bendall

We present InTAC-seq, a method for simultaneous quantification of genome-wide open chromatin and intracellular protein abundance in fixed cells. Using InTAC we directly observe variation in chromatin accessibility and transcription factor motif occupancy driven by differences in transcription factor protein abundance. By purifying bone marrow progenitor cells based on GATA1 protein expression, we establish its role in both functional and epigenetic restriction of erythroid cell identity in human hematopoiesis.

Keywords:

bone marrow progenitor cells
Chromatin
Haematopoiesis
Biology
Cell biology
Epigenetics
Abundance (ecology)
GATA1
Transcription factor
lineage commitment

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