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4 research outputs found

The transcription factor SOX6 contributes to the developmental origins of obesity by promoting adipogenesis

Author: Asim Shabbir
Craig McFarlane
Gluckman Peter D.
Jeremie Poschmann
Juan Yin
Lee Yung Seng
Leow Shi Chi
Melvin K. S. Leow
Ng Kai Lyn
Peh Gek Too
Philip W. Ingham
Roy Joseph
Shaillay Dogra
Shyam Prabhakar
Walter Stunkel
Yap Seng Chong
Publication venue: 'The Company of Biologists'
Publication date: 01/01/2016
Field of study

10.1242/dev.131573Development (Cambridge, England)1436950-961GUSTO (Growing up towards Healthy Outcomes

ScholarBank@NUS

ACSL1 is associated with fetal programming of insulin sensitivity and cellular lipid content

Author: Chong Yap Seng
Gluckman Peter D.
Holbrook Joanna D
Joseph Roy
Julien Sofi G.
Ng Kai Lyn
Poschmann Jeremie
Prabhakar Shyam
Stünkel Walter
Sukarieh Rami
Teh Ai Ling
Too Peh Gek
Xu Feng
Publication venue: 'The Endocrine Society'
Publication date: 01/06/2015
Field of study

10.1210/me.2015-1020Molecular Endocrinology296909-920GUSTO (Growing up towards Healthy Outcomes

The transcription factor SOX6 contributes to the developmental origins of obesity by promoting adipogenesis

Author: Chong Yap Seng
Dogra Shaillay
Gluckman Peter
Ingham Philip
Joseph Roy
Lee Yung Seng
Leow Melvin
Leow Shi Chi
Mcfarlane Craig
Ng Kai Lyn
Poschmann Jérémie
Prabhakar Shyam
Shabbir Asim
Stünkel Walter
Too Peh Gek
Yin Juan
Publication venue: 'The Company of Biologists'
Publication date: 01/01/2016
Field of study

International audienceAn association between impaired fetal growth and the postnatal development of obesity has been established. Here, by comparing adipocytes differentiated from mesenchymal stem cells (MSCs) taken from the umbilical cord and derived from normal and growth-restricted neonates, we identified the transcription factor SOX6 as highly expressed only in growth-restricted individuals. We found that SOX6 regulates adipogenesis in vertebrate species by activating adipogenic regulators including PPARγ, C/EBPα and MEST. We further show that SOX6 interacts with β-catenin in adipocytes, suggesting an inhibition of WNT/β-catenin signaling, thereby promoting adipogenesis. The upstream regulatory region of the MEST gene in MSCs from growth-restricted subjects harbors hypomethylated CpGs next to SOX6 binding motifs, and we found that SOX6 binding is impaired by adjacent CpG methylation. In summary, we report that SOX6 is a novel regulator of adipogenesis synergizing with epigenetic mechanisms

Crossref

HAL-Inserm

ResearchOnline at James Cook University

HAL Descartes

DR-NTU (Digital Repository of NTU)

The transcription factor SOX6 contributes to the developmental origins of obesity by promoting adipogenesis

Author: Chong Yap Seng
Dogra Shaillay
Gluckman Peter D.
Ingham Philip W.
Joseph Roy
Lee Yung Seng
Leow Melvin K.S.
Leow Shi Chi
McFarlane Craig
Ng Kai Lyn
Poschmann Jeremie
Prabhakar Shyam
Shabbir Asim
Stünkel Walter
Too Peh Gek
Yin Juan
Publication venue: The Company of Biologists Ltd
Publication date: 01/01/2016
Field of study

An association between impaired fetal growth and the postnatal development of obesity has been established. Here, by comparing adipocytes differentiated from mesenchymal stem cells (MSCs) taken from the umbilical cord and derived from normal and growth-restricted neonates, we identified the transcription factor SOX6 as highly expressed only in growth-restricted individuals. We found that SOX6 regulates adipogenesis in vertebrate species by activating adipogenic regulators including PPARγ, C/EBPα and MEST. We further show that SOX6 interacts with β-catenin in adipocytes, suggesting an inhibition of WNT/β-catenin signaling, thereby promoting adipogenesis. The upstream regulatory region of the MEST gene in MSCs from growth-restricted subjects harbors hypomethylated CpGs next to SOX6 binding motifs, and we found that SOX6 binding is impaired by adjacent CpG methylation. In summary, we report that SOX6 is a novel regulator of adipogenesis synergizing with epigenetic mechanisms

ResearchOnline@JCU