<i>Irx3</i> promotes gap junction communication between uterine stromal cells to regulate vascularization during embryo implantation

Brown, Roger; Wang, Linda; Fu, Anqi; Kannan, Athilakshmi; Mussar, Michael; Bagchi, Indrani C.; Jorgensen, Joan S.

doi:10.1093/biolre/ioac015

Cited by 4 publications

(1 citation statement)

References 32 publications

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“…For example, our data show that Irx3 controls genes in the Wnt/β-catenin and Hippo signaling pathways in preadipocytes, and these pathways have been shown by others to also be regulated by Irx3 and/or Irx5 in kidney development [41]. Thus our data may help understand how IRX3 mediates its effects in several other conditions in which IRX3 has been implicated, including type 2 diabetes [10], metabolic inflammation [42], fertility [43], neurogenesis [44,45], glioblastoma [46], acute myeloid leukemia [47–50], microvascularization [51] and heart development and function [52– 57].…”

Section: Discussionmentioning

confidence: 70%

Mechanisms of theFTOlocus association with obesity: Irx3 controls a sumoylation-dependent switch between adipogenesis and osteogenesis

Bjune,

Laber,

Lawrence-Archer

et al. 2023

Preprint

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Background: IRX3 is implicated in genetic predisposition to obesity via theFTOvariant locus.IRX3showsFTOrisk allele-dependent upregulation specifically during early adipogenesis, leading to a shift from energy-dissipation to fat storage in mature adipocytes. However, how changes inIRX3expression at one developmental stage affect cellular phenotype at a later stage remains unclear. We here hypothesize that IRX3 regulates adipocyte development via transcriptional modulation of epigenetic reprogramming factors. Methods: We combined ChIP-, ATAC- and RNA-sequencing to map direct Irx3 target genes in regions of open chromatin during early adipogenesis of wild-type andIrx3-KO preadipocytes. Gene ontology analyses was performed to identify significantly enriched biological pathways. Denaturing western blotting was used to assess sumoylation levels, and the inhibitor ML-792 was used to specifically block sumoylation. Luciferase assays were performed to estimate effects of ML-792 on Pparγ activity. Bodipy lipid staining, immunofluorescence and qPCR were employed to assess adipogenic differentiation in 3D culture. Alkaline phosphatase and Alizarine Red S staining, as well as immunofluorescence and qPCR were used to assess osteogenic differentiation in 3D culture. Results: We identified more than 300 Irx3 binding sites in preadipocytes, and these were almost exclusively restricted to promoter regions, with a strong enrichment of genes related to sumoylation, histone modifications and chromatin remodeling. Genes from every step of the sumoylation cycle were bound by Irx3 and differentially expressed in response toIrx3-KO, leading to increased global sumoylation levels in the KO cells. Irx3 ablation and elevated sumoylation inhibited Pparγ activity and adipogenic differentiation in preadipocytes, both of which could be restored by pharmacological inhibition of sumoylation. The Irx3-KO cells demonstrated reduced epigenetic suppression against osteogenesis, resulting in increased osteogenesis in 3D culture. Finally, osteogenesis induced by Irx3 ablation could partially be reversed by inhibition of sumoylation. Conclusions: Our study has uncovered IRX3 as a novel upstream regulator of sumoylation, and a potent controller of epigenetic regulators, both directly and indirectly via suppressing global sumoylation levels. This study indicates that theFTOlocus promotes obesity via IRX3-mediated suppression of sumoylation, which promotes adipogenic commitment and differentiation through epigenetic programming.

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Section: Discussionmentioning

confidence: 70%

Mechanisms of theFTOlocus association with obesity: Irx3 controls a sumoylation-dependent switch between adipogenesis and osteogenesis

Bjune,

Laber,

Lawrence-Archer

et al. 2023

Preprint

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Gene Regulatory Network Analysis of Decidual Stromal Cells and Natural Killer Cells

Rytkönen,

Adossa,

Zúñiga Norman

et al. 2024

Reprod. Sci.

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Human reproductive success relies on the proper differentiation of the uterine endometrium to facilitate implantation, formation of the placenta, and pregnancy. This process involves two critical types of decidual uterine cells: endometrial/decidual stromal cells (dS) and uterine/decidual natural killer (dNK) cells. To better understand the transcription factors governing the in vivo functions of these cells, we analyzed single-cell transcriptomics data from first-trimester terminations of pregnancy, and for the first time conducted gene regulatory network analysis of dS and dNK cell subpopulations. Our analysis revealed stromal cell populations that corresponded to previously described in vitro decidualized cells and senescent decidual cells. We discovered new decidualization driving transcription factors of stromal cells for early pregnancy, including DDIT3 and BRF2, which regulate oxidative stress protection. For dNK cells, we identified transcription factors involved in the immunotolerant (dNK1) subpopulation, including IRX3 and RELB, which repress the NFKB pathway. In contrast, for the less immunotolerant (dNK3) population we predicted TBX21 (T-bet) and IRF2-mediated upregulation of the interferon pathway. To determine the clinical relevance of our findings, we tested the overrepresentation of the predicted transcription factors target genes among cell type-specific regulated genes from pregnancy disorders, such as recurrent pregnancy loss and preeclampsia. We observed that the predicted decidualized stromal and dNK1-specific transcription factor target genes were enriched with the genes downregulated in pregnancy disorders, whereas the predicted dNK3-specific targets were enriched with genes upregulated in pregnancy disorders. Our findings emphasize the importance of stress tolerance pathways in stromal cell decidualization and immunotolerance promoting regulators in dNK differentiation.

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Defining high confidence targets of differential CpG methylation in response to in utero arsenic exposure and implications for cancer risk

Lumour-Mensah,

Lemos

2024

Toxicology and Applied Pharmacology

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Irx3 promotes gap junction communication between uterine stromal cells to regulate vascularization during embryo implantation

Cited by 4 publications

References 32 publications

Mechanisms of theFTOlocus association with obesity: Irx3 controls a sumoylation-dependent switch between adipogenesis and osteogenesis

Mechanisms of theFTOlocus association with obesity: Irx3 controls a sumoylation-dependent switch between adipogenesis and osteogenesis

Gene Regulatory Network Analysis of Decidual Stromal Cells and Natural Killer Cells

Defining high confidence targets of differential CpG methylation in response to in utero arsenic exposure and implications for cancer risk

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