A neurogenic signature involving monoamine Oxidase-A controls human thermogenic adipose tissue development

Solivan-Rivera, Javier; Loureiro, Zinger Yang; DeSouza, Tiffany; Desai, Anand; Pallat, Sabine; Yang, Qin; Rojas-Rodriguez, Raziel; Ziegler, Rachel; Skritakis, Pantos; Joyce, Shannon; Zhong, Denise; Nguyen, Tammy; Corvera, Silvia

doi:10.7554/elife.78945

Cited by 10 publications

(5 citation statements)

References 70 publications

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“…6a ) and generate a functional human/mouse hybrid adipose depot (Fig. 6b ) 33 . Analysis of human transcript-specific reads in adipose tissue formed 8 weeks after implantation revealed expected expression of human adipocyte genes, as well as expression of mesenchymal progenitor markers and canonical Wnt target genes (Fig.…”

Section: Resultsmentioning

confidence: 99%

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Wnt signaling preserves progenitor cell multipotency during adipose tissue development

et al. 2023

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Mesenchymal stem/progenitor cells are essential for tissue development and repair throughout life, but how they are maintained under chronic differentiation pressure is not known. Using single-cell transcriptomics of human progenitor cells we find that adipose differentiation stimuli elicit two cellular trajectories: one toward mature adipocytes and another toward a pool of non-differentiated cells that maintain progenitor characteristics. These cells are induced by transient Wnt pathway activation and express numerous extracellular matrix genes and are therefore named structural Wnt-regulated adipose tissue cells. We find that the genetic signature of structural Wnt-regulated adipose tissue cells is present in adult human adipose tissue and adipose tissue developed from human progenitor cells in mice. Our results suggest a mechanism whereby adipose differentiation occurs concurrently with the maintenance of a mesenchymal progenitor cell pool, ensuring tissue development, repair and appropriate metabolic control over the lifetime.

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Section: Resultsmentioning

confidence: 99%

“…Methods for the collection and culture of adipose tissue explants were previously published 33 . In brief, ~10 7 passage 3 human adipose tissue derived progenitor cells were thawed into 150-mm plate and after 72 h they were split 1:2 at a dense seeding density of ~8 × 10 6 cells per 150-mm plate.…”

Section: Methodsmentioning

confidence: 99%

Wnt signaling preserves progenitor cell multipotency during adipose tissue development

et al. 2023

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“…An et al [31] discovered that regardless of genetic and other clinical factors, methylation variation in the MAOA gene promoter is related to fasting plasma glucose. Solivan-Rivera et al [32] identifed mechanisms that regulate the formation of thermogenic adipose tissue and suggested that human adipocyte MAOA could serve as a potential therapeutic target for metabolic disorders. Our molecular docking analysis of eugenol and MAOA refected that the hypoglycemic mechanism may be bound up with inhibiting MAOA by eugenol after a high-fat diet.…”

Section: Discussionmentioning

confidence: 99%

Network Pharmacology Prediction and Metabolomics Validation of the Novel Targets of Morus alba L. against High-Fat Diet-Induced Diabetes Mellitus in C57/6J Mice

Qiu,

Chen,

et al. 2024

Journal of Food Biochemistry

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Diabetes mellitus (DM) is an endocrine-metabolic disorder that has limited approaches to treat effectively. Morus alba L., also known as mulberry, is a well-known medicinal plant, and its branch bark has shown hypoglycemic activity. It is rich in antioxidant and anti-inflammatory ingredients. In this study, we used metabolomics combined with network pharmacology to investigate the molecular mechanism and potential key targets of mulberry branch bark powder (MBBP) for treating DM. Serum metabolomics was performed to analyze the differences in metabolites and enrich metabolic pathways. Network pharmacology, based on systems biology tools, was applied to generate the pathway-target-compound network. Integrated analyses were then used to screen for key targets. To verify the obtained key targets, we used a molecular docking method and experimental validation. Our findings revealed that thirty-five endogenous metabolites contributed to the therapeutic impact of MBBP against DM. The analysis of 10 hub genes in the compound-target network partially supported the enrichment of metabolic pathways. Further analysis focused on two compounds (eugenol and mulberrofuran A) and three key targets (NOS2, MAOA, and CYP1A1). This study explores the active compounds of MBBP against DM and provides a novel perspective for improving DM treatment based on key targets.

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“…It is well established that humans are born with classical brown adipose tissue localized to the interscapular and perirenal regions 49 with the interscapular depot regressing in the first and second decade of life 17,20 and the perirenal depot slowly transforming into a white adipose tissue depot 50 . Since thermogenic adipose tissue increases insulin sensitivity and energy expenditure to suppress the development of diabetes and obesity, there are currently numerous efforts to find therapeutic approaches to induce the formation of beige adipose tissue [51][52][53] . However, an alternative approach would be to prevent the regression of brown adipocytes that are present at birth.…”

Section: Discussionmentioning

confidence: 99%

Involution of brown adipose tissue through a Syntaxin 4 dependent pyroptosis pathway

Yu,

Benitez,

Wei

et al. 2024

Nat Commun

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Aging, chronic high-fat diet feeding, or housing at thermoneutrality induces brown adipose tissue (BAT) involution, a process characterized by reduction of BAT mass and function with increased lipid droplet size. Single nuclei RNA sequencing of aged mice identifies a specific brown adipocyte population of Ucp1-low cells that are pyroptotic and display a reduction in the longevity gene syntaxin 4 (Stx4a). Similar to aged brown adipocytes, Ucp1-STX4KO mice display loss of brown adipose tissue mass and thermogenic dysfunction concomitant with increased pyroptosis. Restoration of STX4 expression or suppression of pyroptosis activation protects against the decline in both mass and thermogenic activity in the aged and Ucp1-STX4KO mice. Mechanistically, STX4 deficiency reduces oxidative phosphorylation, glucose uptake, and glycolysis leading to reduced ATP levels, a known triggering signal for pyroptosis. Together, these data demonstrate an understanding of rapid brown adipocyte involution and that physiologic aging and thermogenic dysfunction result from pyroptotic signaling activation.

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A neurogenic signature involving monoamine Oxidase-A controls human thermogenic adipose tissue development

Cited by 10 publications

References 70 publications

Wnt signaling preserves progenitor cell multipotency during adipose tissue development

Wnt signaling preserves progenitor cell multipotency during adipose tissue development

Network Pharmacology Prediction and Metabolomics Validation of the Novel Targets of Morus alba L. against High-Fat Diet-Induced Diabetes Mellitus in C57/6J Mice

Involution of brown adipose tissue through a Syntaxin 4 dependent pyroptosis pathway

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