Mapping the Effects of Genetic Variation on Chromatin State and Gene Expression Reveals Loci That Control Ground State Pluripotency

Skelly, Daniel A.; Czechanski, Anne; Byers, Candice; Aydin, Selcan; Spruce, Catrina; Olivier, Chris; Choi, Kwangbom; Gatti, Daniel M.; Raghupathy, Narayanan; Keele, Gregory R.; Stanton, Alexander R.; Vincent, Matthew; Dion, Stephanie; Greenstein, Ian; Pankratz, Matthew; Porter, Devin K.; Martin, Whitney; O’Connor, Callan; Qin, Wenning; Harrill, Alison H.; Choi, Tae-Young; Churchill, Gary A.; Munger, Steven C.; Baker, Christopher L.; Reinholdt, Laura G.

doi:10.1016/j.stem.2020.07.005

Cited by 35 publications

(80 citation statements)

References 73 publications

(81 reference statements)

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“…This approach showed that chromatin accessibility at pluripotent TF motifs are higher in B6 compared to D2, indicating other trans acting chromatin regulation may determine pluripotent spectrum. We identified 6 QTL hotspots that alter binding of naïve 57 , as well as association with differences in priming sites of meiotic recombination 49 and stabilization of ground state pluripotency 14 . Notably, a single KZFP contained within our Chr 13 hotspot QTL interval was shown to be causal in the progression of a lupus phenotype 57 .…”

Section: Genetic Background Biases Differentiation Propensitymentioning

confidence: 99%

“…For each biological replicate ESC ChIP-seq library, 10 million cells were harvested and fixed as previously described 14 . Cell lysis, chromatin fragmentation, dialysis, and immunoprecipitation was performed as described 67 .…”

Section: Atac-seq and Chip-seq Sample Prep And Sequencingmentioning

confidence: 99%

“…Further, success in derivation and differentiation of human induced PSCs (hiPSCs) and ESCs (hESCs) are influenced by genetic background [8][9][10][11][12][13] . While we 14 and others 15 have recently investigated how genetic variation impacts pluripotency, less is understood about how genetic backgrounds influence cell state transitions.…”

Section: Introductionmentioning

confidence: 99%

“…Transit through formative pluripotency is required for multi-lineage competency [21][22][23] , and this state can be modeled in vitro by EpiLCs 21 . While culture conditions can provide external signaling cues that positions a cell along the pluripotency spectrum 22 , variability in acquisition of desired pluripotent states is, in part, dependent on the ESC's strain of origin 6,14,15,[24][25][26][27] . Importantly, differentiation propensity to specific germ layers has been linked to the origin of ESCs within this pluripotency spectrum 28 .…”

Section: Introductionmentioning

confidence: 99%

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Genetic control of pluripotency epigenome determines differentiation bias in mouse embryonic stem cells

Byers

Spruce

Fortin

et al. 2021

Preprint

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Genetically diverse pluripotent stem cells (PSCs) display varied, heritable responses to differentiation cues in the culture environment. By harnessing these disparities through derivation of embryonic stem cells (ESCs) from the BXD mouse genetic reference panel, along with C57BL/6J (B6) and DBA/2J (D2) parental strains, we demonstrate genetically determined biases in lineage commitment and identify major regulators of the pluripotency epigenome. Upon transition to formative pluripotency using epiblast-like cells (EpiLCs), B6 quickly dissolves naïve networks adopting gene expression modules indicative of neuroectoderm lineages; whereas D2 retains aspects of naïve pluripotency with little bias in differentiation. Genetic mapping identifies 6 major trans-acting loci co-regulating chromatin accessibility and gene expression in ESCs and EpiLCs, indicating a common regulatory system impacting cell state transition. These loci distally modulate occupancy of pluripotency factors, including TRIM28, P300, and POU5F1, at hundreds of regulatory elements. One trans-acting locus on Chr 12 primarily impacts chromatin accessibility in ESCs; while in EpiLCs the same locus subsequently influences gene expression, suggesting early chromatin priming. Consequently, the distal gene targets of this locus are enriched for neurogenesis genes and were more highly expressed when cells carried B6 haplotypes at this Chr 12 locus, supporting genetic regulation of biases in cell fate. Spontaneous formation of embryoid bodies validated this with B6 showing a propensity towards neuroectoderm differentiation and D2 towards definitive endoderm, confirming the fundamental importance of genetic variation influencing cell fate decisions.

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Section: Genetic Background Biases Differentiation Propensitymentioning

confidence: 99%

Section: Atac-seq and Chip-seq Sample Prep And Sequencingmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Genetic control of pluripotency epigenome determines differentiation bias in mouse embryonic stem cells

Byers

Spruce

Fortin

et al. 2021

Preprint

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“…Applications of mediation analysis to large scale genetic and molecular profiling data have used modified versions of the traditional tests described above. Approximations to CS have been used in the multi-parent Collaborative Cross (CC [12,6,13]) and Diversity Outbred mouse populations (DO [14,5,15,16]). These studies identified QTL for gene expression (eQTL), protein abundance (pQTL), and chromatin accessibility (cQTL).…”

Section: Introductionmentioning

confidence: 99%

A Bayesian model selection approach to mediation analysis

Crouse

Keele

Gastonguay

et al. 2021

Preprint

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Mediation analysis is a powerful tool for discovery of causal relationships. We describe a Bayesian model selection approach to mediation analysis that is implemented in our bmediatR software. Using simulations, we show that bmediatR performs as well or better than established methods including the Sobel test, while allowing greater flexibility in both model specification and in the types of inference that are possible. We applied bmediatR to genetic data from mice and human cell lines to demonstrate its ability to derive biologically meaningful findings. The Bayesian model selection framework is extensible to support a wide variety of mediation models.

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Inherent genomic properties underlie the epigenomic heterogeneity of human induced pluripotent stem cells

et al. 2021

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Mapping the Effects of Genetic Variation on Chromatin State and Gene Expression Reveals Loci That Control Ground State Pluripotency

Cited by 35 publications

References 73 publications

Genetic control of pluripotency epigenome determines differentiation bias in mouse embryonic stem cells

Genetic control of pluripotency epigenome determines differentiation bias in mouse embryonic stem cells

A Bayesian model selection approach to mediation analysis

Inherent genomic properties underlie the epigenomic heterogeneity of human induced pluripotent stem cells

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