Chromatin and Single-Cell RNA-Seq Profiling Reveal Dynamic Signaling and Metabolic Transitions during Human Spermatogonial Stem Cell Development.
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IF: 25.269
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Cited by: 178
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Abstract

Human adult spermatogonial stem cells (hSSCs) must balance self-renewal and differentiation. To understand how this is achieved, we profiled DNA methylation and open chromatin (ATAC-seq) in SSEA4+ hSSCs, analyzed bulk and single-cell RNA transcriptomes (RNA-seq) in SSEA4+ hSSCs and differentiating c-KIT+ spermatogonia, and performed validation studies via immunofluorescence. First, DNA hypomethylation at embryonic developmental genes supports their epigenetic "poising" in hSSCs for future/embryonic expression, while core pluripotency genes (OCT4 and NANOG) were transcriptionally and epigenetically repressed. Interestingly, open chromatin in hSSCs was strikingly enriched in binding sites for pioneer factors (NFYA/B, DMRT1, and hormone receptors). Remarkably, single-cell RNA-seq clustering analysis identified four cellular/developmental states during hSSC differentiation, involving major transitions in cell-cycle and transcriptional regulators, splicing and signaling factors, and glucose/mitochondria regulators. Overall, our results outline the dynamic chromatin/transcription landscape operating in hSSCs and identify crucial molecular pathways that accompany the transition from quiescence to proliferation and differentiation.

Keywords

DNA methylation
hormone receptors
human spermatogonial stem cells
metabolism
open chromatin
pluripotency
single-cell RNA-seq
spermatogenesis

MeSH terms

Base Sequence
Binding Sites
Chromatin
Cluster Analysis
DNA
DNA Methylation
Genomics
Humans
Male
Meiosis
Pluripotent Stem Cells
Receptors, Cell Surface
Repetitive Sequences, Nucleic Acid
Reproducibility of Results
Seminiferous Tubules
Sequence Analysis, RNA
Signal Transduction
Single-Cell Analysis
Spermatogonia
Stage-Specific Embryonic Antigens
Stem Cells
Transcription, Genetic
Transcriptome

Authors

Guo, Jingtao
Grow, Edward J
Yi, Chongil
Mlcochova, Hana
Maher, Geoffrey J
Lindskog, Cecilia
Murphy, Patrick J
Wike, Candice L
Carrell, Douglas T
Goriely, Anne
Hotaling, James M
Cairns, Bradley R

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