JunD Regulates Pancreatic β-Cells Function by Altering Lipid Accumulation

Wang, Kexin; Cui, Yixin; Lin, Pei; Yao, Zhina; Sun, Yu

doi:10.3389/fendo.2021.689845

Cited by 9 publications

(10 citation statements)

References 56 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…This could explain the absence of well-established pancreas TFs such as MAFA (Olbrot et al 2002), MNX1 (Flanagan et al 2014), NEUROG3 (Krentz et al 2017), FOXA2 (Lee et al 2019) and NKX2-2 (Mastracci et al 2011) in this analysis. Nevertheless, in support of the validity of our findings, ATAC-seq, the literature and immunohistochemistry of human pancreas sections corroborate several pySCENIC predictions reported here such as BHLHE41, JUND and HEYL (Gomez et al 2015; Good et al 2019; K. Wang et al 2021).…”

Section: Discussionsupporting

confidence: 92%

“…EGR1 (but not EGR4) has been shown to transcriptionally regulate GCG (Leung-Theung-Long et al 2005) as well as the PDX1 promoter in beta cells (Eto, Kaur, and Thomas 2007). STAT4 and JUND have been described respectively in pancreatic tissue in general and in beta cells but not in alpha cells (Yu and Kim 2012; Good et al 2019; K. Wang et al 2021) (Figure 3B,C) .…”

Section: Resultsmentioning

confidence: 97%

“…To examine the effect of perturbation of candidate TFs in the human adult pancreas, we selected two TFs for targeting with siRNAs in hiPSC-derived islet cells, an in vitro pancreatic islet model (Balboa et al 2022). JUND was identified as a regulator of oxidative stress and lipotoxicity in beta cells (K. Wang et al 2021; Good et al 2019) but its potential role in alpha cells remains unknown. BHLHE41 was of interest due to its role in circadian rhythm regulation (Hamaguchi et al 2004) but its putative impact on cell identity in the human pancreas has not yet been investigated.…”

Section: Resultsmentioning

confidence: 99%

See 2 more Smart Citations

Predicting the Key Regulators of Cell Identity in Human Adult Pancreas

Vanheer¹,

Schiavo

Haele

et al. 2020

Preprint

View full text Add to dashboard Cite

SUMMARYCellular identity during development is under the control of transcription factors that form gene regulatory networks. However, the transcription factors and gene regulatory networks underlying cellular identity in the human adult pancreas remain largely unexplored. Here, we integrate multiple single-cell RNA sequencing datasets of the human adult pancreas, totaling 7393 cells, and comprehensively reconstruct gene regulatory networks. We show that a network of 142 transcription factors forms distinct regulatory modules that characterize pancreatic cell types. We present evidence that our approach identifies key regulators of cell identity in the human adult pancreas. We predict that HEYL and JUND are active in acinar and alpha cells, respectively, and show that these proteins are present in the human adult pancreas as well as in human induced pluripotent stem cell-derived pancreatic cells. The comprehensive gene regulatory network atlas can be explored interactively online. We anticipate our analysis to be the starting point for a more sophisticated dissection of how transcription factors regulate cell identity in the human adult pancreas. Furthermore, given that transcription factors are major regulators of embryo development and are often perturbed in diseases, a comprehensive understanding of how transcription factors work will be relevant in development and disease biology.HIGHLIGHTS-Reconstruction of gene regulatory networks for human adult pancreatic cell types-An interactive resource to explore and visualize gene expression and regulatory states-Predicting putative transcription factors driving pancreatic cell identity-HEYL and JUND as candidate regulators of acinar and alpha cell identity, respectively

show abstract

Section: Discussionsupporting

confidence: 92%

Section: Resultsmentioning

confidence: 97%

Section: Resultsmentioning

confidence: 99%

See 1 more Smart Citation

Predicting the Key Regulators of Cell Identity in Human Adult Pancreas

Vanheer¹,

Schiavo

Haele

et al. 2020

Preprint

View full text Add to dashboard Cite

show abstract

“…RXRA was predicted to cooperate with the bile acid receptor NR1H4 in SC-β-cell and SC-EC gene regulation ( Figure 2J ), identifying a possible mechanism for the role of bile acids in insulin secretion (Vettorazzi et al, 2016). Of interest is also the SC-β-cell-specific interaction between BACH2 and JUND ( Figure 2K ), which have both been reported to contribute to β-cell dysfunction in type 2 diabetes (Good et al, 2019; Son et al, 2021; Wang et al, 2021). In summary, our GRN provides a resource for interrogating gene regulatory mechanisms in SC-islet cell types and their precursors.…”

Section: Resultsmentioning

confidence: 99%

Improving stem cell-derived pancreatic islets using single-cell multiome-inferred regulomes

Zhu

Wang

Nguyen-Ngoc

et al. 2022

Preprint

View full text Add to dashboard Cite

Pancreatic islet cells derived from human pluripotent stem cells hold great promise for modeling and treating diabetes. Differences between stem cell-derived and primary islets remain, but molecular insights to inform improvements are limited. Here, we acquire single-cell transcriptomes and accessible chromatin profiles during in vitro islet differentiation and pancreas from childhood and adult donors for comparison. We delineate major cell types, define their regulomes, and describe spatiotemporal gene regulatory relationships between transcription factors. CDX2 emerged as a regulator of enterochromaffin-like cells, which we show resemble a transient, previously unrecognized, CDX2+ pre-β-cell population in fetal pancreas, arguing against a proposed non-pancreatic origin. Furthermore, we observe insufficient activation of signal-dependent transcriptional programs during in vitro β-cell maturation and identify sex hormones as drivers of β-cell proliferation in childhood. Altogether, our analysis provides a comprehensive understanding of cell fate acquisition in stem cell-derived islets and a framework for manipulating cell identities and maturity.

show abstract

“…Especially, JUND are assigned with high weights on the models of multiple target genes, and also tend to form clockwise curve (Supplementary Figure 2c). Early studies have reported that JUND modulates cell differentiation, proliferation, and apoptosis [30], further confirming the regulation mechanisms of JUND in pancreatic cells [31,32].…”

Section: Tfvelo Can Model Cell Differentiation Process On Pancreas Da...mentioning

confidence: 64%

TFvelo: gene regulation inspired RNA velocity estimation

Pan

Yuan

et al. 2023

Preprint

View full text Add to dashboard Cite

RNA velocity is closely related with cell fate and is an important indicator for the prediction of cell states with elegant physical explanation derived from single-cell RNA-seq data. However, most existing RNA velocity models can only be applied to datasets with unspliced/spliced or new/total RNA abundance information. Moreover, the dynamics constructed by these models can not fit the co-expression of spliced and unspliced RNAs well. Motivated by the finding that RNA velocity could be driven by the transcriptional regulation, we propose TFvelo, which expands RNA velocity concept to various single-cell datasets without splicing information, by introducing gene regulatory network information. Our experiments on synthetic data and scRNA-Seq data demonstrate that TFvelo can better model the gene dynamics, infer cell pseudo-time and trajectory, and also detect the key TF-target regulation simultaneously. TFvelo opens a novel, robust and accurate avenue for modeling RNA velocity for single cell data.

show abstract

JunD Regulates Pancreatic β-Cells Function by Altering Lipid Accumulation

Cited by 9 publications

References 56 publications

Predicting the Key Regulators of Cell Identity in Human Adult Pancreas

Predicting the Key Regulators of Cell Identity in Human Adult Pancreas

Improving stem cell-derived pancreatic islets using single-cell multiome-inferred regulomes

TFvelo: gene regulation inspired RNA velocity estimation

Contact Info

Product

Resources

About