Transcriptional Pathways in cPGI2-Induced Adipocyte Progenitor Activation for Browning

Bayindir, Irem; Babaeikelishomi, Rohollah; Kočanová, Silvia; Sousa, Isabel; Lerch, Sarah; Hardt, Olaf; Wild, Stefan; Bosio, Andreas; Bystricky, Kerstin; Herzig, Stephan; Vegiopoulos, Alexandros

doi:10.3389/fendo.2015.00129

Cited by 30 publications

(41 citation statements)

References 40 publications

(63 reference statements)

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“…Aside from these limitations, the physiological relevance of an undocumented but presumably substantially augmented (Bol et al, 2002) and sustained increase in prostaglandin biosynthesis in COX-2 overexpressing mice is, at best, arguable. Similar constraints apply to the reports that micromolar concentrations of carbaprostacyclin, a synthetic analog of the COX-2 product, prostacyclin, promote browning of adipocytes in in vitro cell-culture models (Bayindir et al, 2015; Ghandour et al, 2016). Endogenous prostanoids, such as prostacyclin, are formed transiently and, at femtomolar to picomolar quantities, to act locally (FitzGerald et al, 1981).…”

Section: Resultsmentioning

confidence: 59%

Cold-Induced Browning of Inguinal White Adipose Tissue Is Independent of Adipose Tissue Cyclooxygenase-2

et al. 2018

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SUMMARY Previous studies using genetic mouse models have implicated COX-2 in the browning of white adipose tissues (WATs) in mice during cold exposure. However, COX-2 is important during development, and conventional knockouts (KOs) exhibit many defects, conditioned by genetic background. Similarly, the physiological relevance of transgenic overexpression of COX-2 is questionable. In the present study, we utilized mice in which COX-2 was deleted postnatally, bypassing the consequences of enzyme deficiency during development. Despite activation of thermogenesis and browning of inguinal WAT, cold exposure failed to increase COX-2 expression in the adipose tissues of mice with different genetic backgrounds, and the body temperature response to cold was unaltered in postnatal global COX-2 KOs. Selective disruption of COX-2 in adipose tissues also failed detectably to impact systemic prostaglandin biosynthesis. Browning of inguinal WATs induced by exposure to cold is independent of adipose tissue COX-2.

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Section: Resultsmentioning

confidence: 59%

Cold-Induced Browning of Inguinal White Adipose Tissue Is Independent of Adipose Tissue Cyclooxygenase-2

et al. 2018

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“…Adipose progenitors were isolated by magnetic-activated cell sorting (MACS) approach, as previously described (17,18). Briefly, the SVF …”

Section: Progenitor Isolation By Macsmentioning

confidence: 99%

“…Sorting of adipose tissue cell populations was performed as previously described (18). Briefly, adipocytes and SVF were separated by centrifugation of digested and strained adipose tissue.…”

Section: Isolation Of Adipose Tissue Cell Populations By Facsmentioning

confidence: 99%

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Jak-TGFβ cross-talk links transient adipose tissue inflammation to beige adipogenesis

et al. 2018

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The transient activation of inflammatory networks is required for adipose tissue remodeling including the "browning" of white fat in response to stimuli such as 3-adrenergic receptor activation. In this process, white adipose tissue acquires thermogenic characteristics through the recruitment of so-called beige adipocytes. We investigated the downstream signaling pathways impinging on adipocyte progenitors that promote de novo formation of adipocytes. We showed that the Jak family of kinases controlled TGF signaling in the adipose tissue microenvironment through Stat3 and thereby adipogenic commitment, a function that was required for beige adipocyte differentiation of murine and human progenitors. Jak/Stat3 inhibited TGF signaling to the transcription factors Srf and Smad3 by repressing local Tgfb3 and Tgfb1 expression before the core transcriptional adipogenic cascade was activated. This pathway cross-talk was triggered in stromal cells by ATGL-dependent adipocyte lipolysis and a transient wave of IL-6 family cytokines at the onset of adipose tissue remodeling induced by 3-adrenergic receptor stimulation. Our results provide insight into the activation of adipocyte progenitors and are relevant for the therapeutic targeting of adipose tissue inflammatory pathways.

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“…3) [44,46]. L'engagement des préadipocytes dans la voie de différenciation en adipocytes brites serait dépendante du récepteur IP et pourrait mettre en jeu des réorganisations du cytosquelette et/ou de la chromatine [46,50]. De même, l'effet de cPGI2 sur la conversion des adipocytes blancs en brites est dépendant des voies faisant intervenir des variations des niveaux d'AMPc [44].…”

Section: Acide Arachidonique Et Recrutement Des Adipocytes Britesunclassified

Acide arachidonique et prostaglandines : impact sur la formation des adipocytes blancs, bruns et brites/beiges

Ghandour

Pisani

Amri

2016

Obes

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Les adipocytes blancs stockent et libèrent l'énergie à la demande alors que les adipocytes brites (ou beiges) et bruns la dissipent sous forme de chaleur. Nous décrivons ici les effets de l'acide arachidonique (ARA) et de ses métabolites sur la formation de ces adipocytes, en mettant en avant la complexité et la dualité de ces effets. Ces données démontrent l'importance de la biodisponibilité de l'ARA dans la biologie du tissu adipeux et les pathologies qui lui sont associées. Mots clés Acides gras · Prostacycline · PGF2α · PGE2 · AdipogenèseAbstract White adipocytes store and release energy upon request whereas brown and brite (or beige) adipocytes dissipate it as heat. Herein, we describe the effects of arachidonic acid (ARA) and its metabolites on the formation of white and brites adipocytes, highlighting the complexity and duality of these effects. These observations demonstrate the importance of the bioavailability of ARA in the adipose tissue biology and its associated diseases.

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Transcriptional Pathways in cPGI2-Induced Adipocyte Progenitor Activation for Browning

Cited by 30 publications

References 40 publications

Cold-Induced Browning of Inguinal White Adipose Tissue Is Independent of Adipose Tissue Cyclooxygenase-2

Cold-Induced Browning of Inguinal White Adipose Tissue Is Independent of Adipose Tissue Cyclooxygenase-2

Jak-TGFβ cross-talk links transient adipose tissue inflammation to beige adipogenesis

Acide arachidonique et prostaglandines : impact sur la formation des adipocytes blancs, bruns et brites/beiges

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