Your search keyword '"Sassoon, David"' showing total 10 results

1. Hypoxia promotes a perinatal-like progenitor state in the adult murine epicardium.

Author

Sayed, Angeliqua, Turoczi, Szimonetta, Soares-da-Silva, Francisca, Marazzi, Giovanna, Hulot, Jean-Sebastien, Sassoon, David, and Valente, Mariana

Subjects

PERICARDIUM, HYPOXEMIA, CELL culture, PROGENITOR cells, CELL cycle, ADULTS

Abstract

The epicardium is a reservoir of progenitors that give rise to coronary vasculature and stroma during development and mediates cardiac vascular repair. However, its role as a source of progenitors in the adult mammalian heart remains unclear due to lack of clear lineage markers and single-cell culture systems to elucidate epicardial progeny cell fate. We found that in vivo exposure of mice to physiological hypoxia induced adult epicardial cells to re-enter the cell cycle and to express a subset of developmental genes. Multiplex single cell transcriptional profiling revealed a lineage relationship between epicardial cells and smooth muscle, stromal cells, as well as cells with an endothelial-like fate. We found that physiological hypoxia promoted a perinatal-like progenitor state in the adult murine epicardium. In vitro clonal analyses of purified epicardial cells showed that cell growth and subsequent differentiation is dependent upon hypoxia, and that resident epicardial cells retain progenitor identity in the adult mammalian heart with self-renewal and multilineage differentiation potential. These results point to a source of progenitor cells in the adult heart that can be stimulated in vivo and provide an in vitro model for further studies. [ABSTRACT FROM AUTHOR]

Published

2022

2. Anti-integrin αv therapy improves cardiac fibrosis after myocardial infarction by blunting cardiac PW1+ stromal cells.

Author

Bouvet, Marion, Claude, Olivier, Roux, Maguelonne, Skelly, Dan, Masurkar, Nihar, Mougenot, Nathalie, Nadaud, Sophie, Blanc, Catherine, Delacroix, Clément, Chardonnet, Solenne, Pionneau, Cédric, Perret, Claire, Yaniz-Galende, Elisa, Rosenthal, Nadia, Trégouët, David-Alexandre, Marazzi, Giovanna, Silvestre, Jean-Sébastien, Sassoon, David, and Hulot, Jean-Sébastien

Subjects

HEART fibrosis, MYOCARDIAL infarction, HEART cells, CELL adhesion, ISCHEMIA

Abstract

There is currently no therapy to limit the development of cardiac fibrosis and consequent heart failure. We have recently shown that cardiac fibrosis post-myocardial infarction (MI) can be regulated by resident cardiac cells with a fibrogenic signature and identified by the expression of PW1 (Peg3). Here we identify αV-integrin (CD51) as an essential regulator of cardiac PW1+ cells fibrogenic behavior. We used transcriptomic and proteomic approaches to identify specific cell-surface markers for cardiac PW1+ cells and found that αV-integrin (CD51) was expressed in almost all cardiac PW1+ cells (93% ± 1%), predominantly as the αVβ1 complex. αV-integrin is a subunit member of the integrin family of cell adhesion receptors and was found to activate complex of latent transforming growth factor beta (TGFβ at the surface of cardiac PW1+ cells. Pharmacological inhibition of αV-integrin reduced the profibrotic action of cardiac PW1+CD51+ cells and was associated with improved cardiac function and animal survival following MI coupled with a reduced infarct size and fibrotic lesion. These data identify a targetable pathway that regulates cardiac fibrosis in response to an ischemic injury and demonstrate that pharmacological inhibition of αV-integrin could reduce pathological outcomes following cardiac ischemia. [ABSTRACT FROM AUTHOR]

Published

2020

3. Odd skipped-related 1 identifies a population of embryonic fibro-adipogenic progenitors regulating myogenesis during limb development.

Author

Vallecillo-García, Pedro, Orgeur, Mickael, vom Hofe-Schneider, Sophie, Stumm, Jürgen, Kappert, Verena, Ibrahim, Daniel M., Börno, Stefan T., Hayashi, Shinichiro, Relaix, Frédéric, Hildebrandt, Katrin, Sengle, Gerhard, Koch, Manuel, Timmermann, Bernd, Marazzi, Giovanna, Sassoon, David A., Duprez, Delphine, and Stricker, Sigmar

Abstract

Fibro-adipogenic progenitors (FAPs) are an interstitial cell population in adult skeletal muscle that support muscle regeneration. During development, interstitial muscle connective tissue (MCT) cells support proper muscle patterning, however the underlying molecular mechanisms are not well understood and it remains unclear whether adult FAPs and embryonic MCT cells share a common lineage. We show here that mouse embryonic limb MCT cells expressing the transcription factor Osr1, differentiate into fibrogenic and adipogenic cells in vivo and in vitro defining an embryonic FAP-like population. Genetic lineage tracing shows that developmental Osr1+ cells give rise to a subset of adult FAPs. Loss of Osr1 function leads to a reduction of myogenic progenitor proliferation and survival resulting in limb muscle patterning defects. Transcriptome and functional analyses reveal that Osr1+ cells provide a critical pro-myogenic niche via the production of MCT specific extracellular matrix components and secreted signaling factors. [ABSTRACT FROM AUTHOR]

Published

2017

4. The zinc finger transcription factor PW1/PEG3 restrains murine beta cell cycling.

Author

Sojoodi, Mozhdeh, Stradiot, Leslie, Tanaka, Karo, Heremans, Yves, Leuckx, Gunter, Besson, Vanessa, Staels, Willem, Casteele, Mark, Marazzi, Giovanna, Sassoon, David, Heimberg, Harry, and Bonfanti, Paola

Abstract

Aims/hypothesis: Pw1 or paternally-expressed gene 3 ( Peg3) encodes a zinc finger transcription factor that is widely expressed during mouse embryonic development and later restricted to multiple somatic stem cell lineages in the adult. The aim of the present study was to define Pw1 expression in the embryonic and adult pancreas and investigate its role in the beta cell cycle in Pw1 wild-type and mutant mice. Methods: We analysed PW1 expression by immunohistochemistry in pancreas of nonpregant and pregnant mice and following injury by partial duct ligation. Its role in the beta cell cycle was studied in vivo using a novel conditional knockout mouse and in vitro by lentivirus-mediated gene knockdown. Results: We showed that PW1 is expressed in early pancreatic progenitors at E9.5 but becomes progressively restricted to fully differentiated beta cells as they become established after birth and withdraw from the cell cycle. Notably, PW1 expression declines when beta cells are induced to proliferate and loss of PW1 function activates the beta cell cycle. Conclusions/interpretation: These results indicate that PW1 is a co-regulator of the beta cell cycle and can thus be considered a novel therapeutic target in diabetes. [ABSTRACT FROM AUTHOR]

Published

2016

5. Identification and characterization of a non-satellite cell muscle resident progenitor during postnatal development.

Author

Mitchell, Kathryn J., Pannérec, Alice, Cadot, Bruno, Parlakian, Ara, Besson, Vanessa, Gomes, Edgar R., Marazzi, Giovanna, and Sassoon, David A.

Subjects

SATELLITE cells, MYOBLASTS, STEM cells, MUSCLE cells, MYOGENESIS

Abstract

Satellite cells are resident myogenic progenitors in postnatal skeletal muscle involved in muscle postnatal growth and adult regenerative capacity. Here, we identify and describe a population of muscle-resident stem cells, which are located in the interstitium, that express the cell stress mediator PW1 but do not express other markers of muscle stem cells such as Pax7. PW1+/Pax7− interstitial cells (PICs) are myogenic in vitro and efficiently contribute to skeletal muscle regeneration in vivo as well as generating satellite cells and PICs. Whereas Pax7 mutant satellite cells show robust myogenic potential, Pax7 mutant PICs are unable to participate in myogenesis and accumulate during postnatal growth. Furthermore, we found that PICs are not derived from a satellite cell lineage. Taken together, our findings uncover a new and anatomically identifiable population of muscle progenitors and define a key role for Pax7 in a non-satellite cell population during postnatal muscle growth. [ABSTRACT FROM AUTHOR]

Published

2010

6. Siah ubiquitin ligase is structurally related to TRAF and modulates TNF-α signaling.

Author

Polekhina, Galina, House, Colin M., Traficante, Nadia, Mackay, Joel P., Relaix, Frédéric, Sassoon, David A., Parker, Michael W., and Bowtell, David D.L.

Subjects

UBIQUITIN, PROTEINS

Abstract

Members of the Siah (seven in absentia homolog) family of RING domain proteins are components of E3 ubiquitin ligase complexes that catalyze ubiquitination of proteins. We have determined the crystal structure of the substrate-binding domain (SBD) of murine Siah1a to 2.6 Å resolution. The structure reveals that Siah is a dimeric protein and that the SBD adopts an eight-stranded β-sandwich fold that is highly similar to the TRAF-C region of TRAF (TNF-receptor associated factor) proteins. The TRAF-C region interacts with TNF-α receptors and TNF-receptor associated death-domain (TRADD) proteins; however, our findings indicate that these interactions are unlikely to be mimicked by Siah. The Siah structure also reveals two novel zinc fingers in a region with sequence similarity to TRAF. We find that the Siah1a SBD potentiates TNF-α-mediated NF-κB activation. Therefore, Siah proteins share important similarities with the TRAF family of proteins, including their overall domain architecture, three-dimensional structure and functional activity. [ABSTRACT FROM AUTHOR]

Published

2002

7. Peg3/Pw1 is an imprinted gene involved in the TNF-NFκB signal transduction pathway.

Author

Relaix, Frédéric, Wei, Xiao-Jun, Wu, Xiangwei, and Sassoon, David A.

Published

1998

8. Fetal exposure to DES results in de-regulation of Wnt7a during uterine morphogenesis.

Author

Miller, Cary, Degenhardt, Karl, and Sassoon, David A.

Subjects

FEMALE reproductive organs, LABORATORY mice

Abstract

Examines the effects of diethylstilbestrol in the female reproductive tract using mice models. Cytodifferentiation of the reproductive tract; Expression of Wnt7a gene; Morphology of female reproductive tract.

Published

1998

9. The imprinted gene Pw1/Peg3 regulates skeletal muscle growth, satellite cell metabolic state, and self-renewal.

Author

Correra, Rosa Maria, Ollitrault, David, Valente, Mariana, Mazzola, Alessia, Adalsteinsson, Bjorn T., Ferguson-Smith, Anne C., Marazzi, Giovanna, and Sassoon, David A.

Abstract

Pw1/Peg3 is an imprinted gene expressed from the paternally inherited allele. Several imprinted genes, including Pw1/Peg3, have been shown to regulate overall body size and play a role in adult stem cells. Pw1/Peg3 is expressed in muscle stem cells (satellite cells) as well as a progenitor subset of muscle interstitial cells (PICs) in adult skeletal muscle. We therefore examined the impact of loss-of-function of Pw1/Peg3 during skeletal muscle growth and in muscle stem cell behavior. We found that constitutive loss of Pw1/Peg3 function leads to a reduced muscle mass and myofiber number. In newborn mice, the reduction in fiber number is increased in homozygous mutants as compared to the deletion of only the paternal Pw1/Peg3 allele, indicating that the maternal allele is developmentally functional. Constitutive and a satellite cell-specific deletion of Pw1/Peg3, revealed impaired muscle regeneration and a reduced capacity of satellite cells for self-renewal. RNA sequencing analyses revealed a deregulation of genes that control mitochondrial function. Consistent with these observations, Pw1/Peg3 mutant satellite cells displayed increased mitochondrial activity coupled with accelerated proliferation and differentiation. Our data show that Pw1/Peg3 regulates muscle fiber number determination during fetal development in a gene-dosage manner and regulates satellite cell metabolism in the adult. [ABSTRACT FROM AUTHOR]

Published

2018

10. PW1/Peg3 expression regulates key properties that determine mesoangioblast stem cell competence.

Author

Bonfanti, Chiara, Rossi, Giuliana, Tedesco, Francesco Saverio, Giannotta, Monica, Benedetti, Sara, Tonlorenzi, Rossana, Antonini, Stefania, Marazzi, Giovanna, Dejana, Elisabetta, Sassoon, David, Cossu, Giulio, and Messina, Graziella

Published

2015