HAND2 is a novel obesity-linked adipogenic transcription factor regulated by glucocorticoid signalling

Maude Giroud; Foivos Filippos Tsokanos; Giorgio Caratti; Stefan Kotschi; Sajjad Khani; Céline Jouffe; Elena S. Vogl; Martin Irmler; Christina Glantschnig; Manuel Gil-Lozano; Daniela Hass; Asrar Ali Khan; Marcos Rios Garcia; Frits Mattijssen; Adriano Maida; Daniel Tews; Pamela Fischer-Posovszky; Annette Feuchtinger; Kirsi A. Virtanen; Johannes Beckers; Martin Wabitsch; Henriette Uhlenhaut; Matthias Blüher; Jan Tuckermann; Marcel Scheideler; Alexander Bartelt; Stephan Herzig

doi:10.1007/s00125-021-05470-y

HAND2 is a novel obesity-linked adipogenic transcription factor regulated by glucocorticoid signalling

Maude Giroud
, Foivos Filippos Tsokanos
, Giorgio Caratti
, Stefan Kotschi
, Sajjad Khani
, Céline Jouffe
, Elena S. Vogl
, Martin Irmler
, Christina Glantschnig
, Manuel Gil-Lozano
, Daniela Hass
, Asrar Ali Khan
, Marcos Rios Garcia
, Frits Mattijssen
, Adriano Maida
, Daniel Tews
, Pamela Fischer-Posovszky
, Annette Feuchtinger
, Kirsi A. Virtanen
, Johannes Beckers

Martin Wabitsch, Henriette Uhlenhaut, Matthias Blüher, Jan Tuckermann, Marcel Scheideler, Alexander Bartelt, Stephan Herzig

Helmholtz Zentrum München German Research Center for Environmental Health
German Centre for Diabetes Research (DZD)
University Hospital Heidelberg
Ludwig-Maximilians-Universität München
University of Ulm
University Medical Center Ulm and Center of Excellence 'Metabolic Disorders'
Turku University Hospital
University Hospital Leipzig
Partner Site Munich Heart Alliance
Harvard T.H. Chan School of Public Health

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

Aims/hypothesis: Adipocytes are critical cornerstones of energy metabolism. While obesity-induced adipocyte dysfunction is associated with insulin resistance and systemic metabolic disturbances, adipogenesis, the formation of new adipocytes and healthy adipose tissue expansion are associated with metabolic benefits. Understanding the molecular mechanisms governing adipogenesis is of great clinical potential to efficiently restore metabolic health in obesity. Here we investigate the role of heart and neural crest derivatives-expressed 2 (HAND2) in adipogenesis. Methods: Human white adipose tissue (WAT) was collected from two cross-sectional studies of 318 and 96 individuals. In vitro, for mechanistic experiments we used primary adipocytes from humans and mice as well as human multipotent adipose-derived stem (hMADS) cells. Gene silencing was performed using siRNA or genetic inactivation in primary adipocytes from loxP and or tamoxifen-inducible Cre-ERT2 mouse models with Cre-encoding mRNA or tamoxifen, respectively. Adipogenesis and adipocyte metabolism were measured by Oil Red O staining, quantitative PCR (qPCR), microarray, glucose uptake assay, western blot and lipolysis assay. A combinatorial RNA sequencing (RNAseq) and ChIP qPCR approach was used to identify target genes regulated by HAND2. In vivo, we created a conditional adipocyte Hand2 deletion mouse model using Cre under control of the Adipoq promoter (Hand2^AdipoqCre) and performed a large panel of metabolic tests. Results: We found that HAND2 is an obesity-linked white adipocyte transcription factor regulated by glucocorticoids that was necessary but insufficient for adipocyte differentiation in vitro. In a large cohort of humans, WAT HAND2 expression was correlated to BMI. The HAND2 gene was enriched in white adipocytes compared with brown, induced early in differentiation and responded to dexamethasone (DEX), a typical glucocorticoid receptor (GR, encoded by NR3C1) agonist. Silencing of NR3C1 in hMADS cells or deletion of GR in a transgenic conditional mouse model results in diminished HAND2 expression, establishing that adipocyte HAND2 is regulated by glucocorticoids via GR in vitro and in vivo. Furthermore, we identified gene clusters indirectly regulated by the GR–HAND2 pathway. Interestingly, silencing of HAND2 impaired adipocyte differentiation in hMADS and primary mouse adipocytes. However, a conditional adipocyte Hand2 deletion mouse model using Cre under control of the Adipoq promoter did not mirror these effects on adipose tissue differentiation, indicating that HAND2 was required at stages prior to Adipoq expression. Conclusions/interpretation: In summary, our study identifies HAND2 as a novel obesity-linked adipocyte transcription factor, highlighting new mechanisms of GR-dependent adipogenesis in humans and mice. Data availability: Array data have been submitted to the GEO database at NCBI (GSE148699). Graphical abstract: [Figure not available: see fulltext.]

Original language	English
Pages (from-to)	1850-1865
Number of pages	16
Journal	Diabetologia
Volume	64
Issue number	8
DOIs	https://doi.org/10.1007/s00125-021-05470-y
State	Published - Aug 2021

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

Adipocytes
Dexamethasone
Differentiation
Glucocorticoid receptor
HAND2
Human adipose tissue
Mesenchymal stem cells
Obesity
Transcription factor
hMADS

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10.1007/s00125-021-05470-y

Cite this

Giroud, M., Tsokanos, F. F., Caratti, G., Kotschi, S., Khani, S., Jouffe, C., Vogl, E. S., Irmler, M., Glantschnig, C., Gil-Lozano, M., Hass, D., Khan, A. A., Garcia, M. R., Mattijssen, F., Maida, A., Tews, D., Fischer-Posovszky, P., Feuchtinger, A., Virtanen, K. A., ... Herzig, S. (2021). HAND2 is a novel obesity-linked adipogenic transcription factor regulated by glucocorticoid signalling. Diabetologia, 64(8), 1850-1865. https://doi.org/10.1007/s00125-021-05470-y

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title = "HAND2 is a novel obesity-linked adipogenic transcription factor regulated by glucocorticoid signalling",

abstract = "Aims/hypothesis: Adipocytes are critical cornerstones of energy metabolism. While obesity-induced adipocyte dysfunction is associated with insulin resistance and systemic metabolic disturbances, adipogenesis, the formation of new adipocytes and healthy adipose tissue expansion are associated with metabolic benefits. Understanding the molecular mechanisms governing adipogenesis is of great clinical potential to efficiently restore metabolic health in obesity. Here we investigate the role of heart and neural crest derivatives-expressed 2 (HAND2) in adipogenesis. Methods: Human white adipose tissue (WAT) was collected from two cross-sectional studies of 318 and 96 individuals. In vitro, for mechanistic experiments we used primary adipocytes from humans and mice as well as human multipotent adipose-derived stem (hMADS) cells. Gene silencing was performed using siRNA or genetic inactivation in primary adipocytes from loxP and or tamoxifen-inducible Cre-ERT2 mouse models with Cre-encoding mRNA or tamoxifen, respectively. Adipogenesis and adipocyte metabolism were measured by Oil Red O staining, quantitative PCR (qPCR), microarray, glucose uptake assay, western blot and lipolysis assay. A combinatorial RNA sequencing (RNAseq) and ChIP qPCR approach was used to identify target genes regulated by HAND2. In vivo, we created a conditional adipocyte Hand2 deletion mouse model using Cre under control of the Adipoq promoter (Hand2AdipoqCre) and performed a large panel of metabolic tests. Results: We found that HAND2 is an obesity-linked white adipocyte transcription factor regulated by glucocorticoids that was necessary but insufficient for adipocyte differentiation in vitro. In a large cohort of humans, WAT HAND2 expression was correlated to BMI. The HAND2 gene was enriched in white adipocytes compared with brown, induced early in differentiation and responded to dexamethasone (DEX), a typical glucocorticoid receptor (GR, encoded by NR3C1) agonist. Silencing of NR3C1 in hMADS cells or deletion of GR in a transgenic conditional mouse model results in diminished HAND2 expression, establishing that adipocyte HAND2 is regulated by glucocorticoids via GR in vitro and in vivo. Furthermore, we identified gene clusters indirectly regulated by the GR–HAND2 pathway. Interestingly, silencing of HAND2 impaired adipocyte differentiation in hMADS and primary mouse adipocytes. However, a conditional adipocyte Hand2 deletion mouse model using Cre under control of the Adipoq promoter did not mirror these effects on adipose tissue differentiation, indicating that HAND2 was required at stages prior to Adipoq expression. Conclusions/interpretation: In summary, our study identifies HAND2 as a novel obesity-linked adipocyte transcription factor, highlighting new mechanisms of GR-dependent adipogenesis in humans and mice. Data availability: Array data have been submitted to the GEO database at NCBI (GSE148699). Graphical abstract: [Figure not available: see fulltext.]",

keywords = "Adipocytes, Dexamethasone, Differentiation, Glucocorticoid receptor, HAND2, Human adipose tissue, Mesenchymal stem cells, Obesity, Transcription factor, hMADS",

author = "Maude Giroud and Tsokanos, \{Foivos Filippos\} and Giorgio Caratti and Stefan Kotschi and Sajjad Khani and C{\'e}line Jouffe and Vogl, \{Elena S.\} and Martin Irmler and Christina Glantschnig and Manuel Gil-Lozano and Daniela Hass and Khan, \{Asrar Ali\} and Garcia, \{Marcos Rios\} and Frits Mattijssen and Adriano Maida and Daniel Tews and Pamela Fischer-Posovszky and Annette Feuchtinger and Virtanen, \{Kirsi A.\} and Johannes Beckers and Martin Wabitsch and Henriette Uhlenhaut and Matthias Bl{\"u}her and Jan Tuckermann and Marcel Scheideler and Alexander Bartelt and Stephan Herzig",

note = "Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2021",

month = aug,

doi = "10.1007/s00125-021-05470-y",

language = "English",

volume = "64",

pages = "1850--1865",

journal = "Diabetologia",

issn = "0012-186X",

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Giroud, M, Tsokanos, FF, Caratti, G, Kotschi, S, Khani, S, Jouffe, C, Vogl, ES, Irmler, M, Glantschnig, C, Gil-Lozano, M, Hass, D, Khan, AA, Garcia, MR, Mattijssen, F, Maida, A, Tews, D, Fischer-Posovszky, P, Feuchtinger, A, Virtanen, KA, Beckers, J, Wabitsch, M, Uhlenhaut, H, Blüher, M, Tuckermann, J, Scheideler, M, Bartelt, A & Herzig, S 2021, 'HAND2 is a novel obesity-linked adipogenic transcription factor regulated by glucocorticoid signalling', Diabetologia, vol. 64, no. 8, pp. 1850-1865. https://doi.org/10.1007/s00125-021-05470-y

TY - JOUR

T1 - HAND2 is a novel obesity-linked adipogenic transcription factor regulated by glucocorticoid signalling

AU - Giroud, Maude

AU - Tsokanos, Foivos Filippos

AU - Caratti, Giorgio

AU - Kotschi, Stefan

AU - Khani, Sajjad

AU - Jouffe, Céline

AU - Vogl, Elena S.

AU - Irmler, Martin

AU - Glantschnig, Christina

AU - Gil-Lozano, Manuel

AU - Hass, Daniela

AU - Khan, Asrar Ali

AU - Garcia, Marcos Rios

AU - Mattijssen, Frits

AU - Maida, Adriano

AU - Tews, Daniel

AU - Fischer-Posovszky, Pamela

AU - Feuchtinger, Annette

AU - Virtanen, Kirsi A.

AU - Beckers, Johannes

AU - Wabitsch, Martin

AU - Uhlenhaut, Henriette

AU - Blüher, Matthias

AU - Tuckermann, Jan

AU - Scheideler, Marcel

AU - Bartelt, Alexander

AU - Herzig, Stephan

PY - 2021/8

Y1 - 2021/8

N2 - Aims/hypothesis: Adipocytes are critical cornerstones of energy metabolism. While obesity-induced adipocyte dysfunction is associated with insulin resistance and systemic metabolic disturbances, adipogenesis, the formation of new adipocytes and healthy adipose tissue expansion are associated with metabolic benefits. Understanding the molecular mechanisms governing adipogenesis is of great clinical potential to efficiently restore metabolic health in obesity. Here we investigate the role of heart and neural crest derivatives-expressed 2 (HAND2) in adipogenesis. Methods: Human white adipose tissue (WAT) was collected from two cross-sectional studies of 318 and 96 individuals. In vitro, for mechanistic experiments we used primary adipocytes from humans and mice as well as human multipotent adipose-derived stem (hMADS) cells. Gene silencing was performed using siRNA or genetic inactivation in primary adipocytes from loxP and or tamoxifen-inducible Cre-ERT2 mouse models with Cre-encoding mRNA or tamoxifen, respectively. Adipogenesis and adipocyte metabolism were measured by Oil Red O staining, quantitative PCR (qPCR), microarray, glucose uptake assay, western blot and lipolysis assay. A combinatorial RNA sequencing (RNAseq) and ChIP qPCR approach was used to identify target genes regulated by HAND2. In vivo, we created a conditional adipocyte Hand2 deletion mouse model using Cre under control of the Adipoq promoter (Hand2AdipoqCre) and performed a large panel of metabolic tests. Results: We found that HAND2 is an obesity-linked white adipocyte transcription factor regulated by glucocorticoids that was necessary but insufficient for adipocyte differentiation in vitro. In a large cohort of humans, WAT HAND2 expression was correlated to BMI. The HAND2 gene was enriched in white adipocytes compared with brown, induced early in differentiation and responded to dexamethasone (DEX), a typical glucocorticoid receptor (GR, encoded by NR3C1) agonist. Silencing of NR3C1 in hMADS cells or deletion of GR in a transgenic conditional mouse model results in diminished HAND2 expression, establishing that adipocyte HAND2 is regulated by glucocorticoids via GR in vitro and in vivo. Furthermore, we identified gene clusters indirectly regulated by the GR–HAND2 pathway. Interestingly, silencing of HAND2 impaired adipocyte differentiation in hMADS and primary mouse adipocytes. However, a conditional adipocyte Hand2 deletion mouse model using Cre under control of the Adipoq promoter did not mirror these effects on adipose tissue differentiation, indicating that HAND2 was required at stages prior to Adipoq expression. Conclusions/interpretation: In summary, our study identifies HAND2 as a novel obesity-linked adipocyte transcription factor, highlighting new mechanisms of GR-dependent adipogenesis in humans and mice. Data availability: Array data have been submitted to the GEO database at NCBI (GSE148699). Graphical abstract: [Figure not available: see fulltext.]

AB - Aims/hypothesis: Adipocytes are critical cornerstones of energy metabolism. While obesity-induced adipocyte dysfunction is associated with insulin resistance and systemic metabolic disturbances, adipogenesis, the formation of new adipocytes and healthy adipose tissue expansion are associated with metabolic benefits. Understanding the molecular mechanisms governing adipogenesis is of great clinical potential to efficiently restore metabolic health in obesity. Here we investigate the role of heart and neural crest derivatives-expressed 2 (HAND2) in adipogenesis. Methods: Human white adipose tissue (WAT) was collected from two cross-sectional studies of 318 and 96 individuals. In vitro, for mechanistic experiments we used primary adipocytes from humans and mice as well as human multipotent adipose-derived stem (hMADS) cells. Gene silencing was performed using siRNA or genetic inactivation in primary adipocytes from loxP and or tamoxifen-inducible Cre-ERT2 mouse models with Cre-encoding mRNA or tamoxifen, respectively. Adipogenesis and adipocyte metabolism were measured by Oil Red O staining, quantitative PCR (qPCR), microarray, glucose uptake assay, western blot and lipolysis assay. A combinatorial RNA sequencing (RNAseq) and ChIP qPCR approach was used to identify target genes regulated by HAND2. In vivo, we created a conditional adipocyte Hand2 deletion mouse model using Cre under control of the Adipoq promoter (Hand2AdipoqCre) and performed a large panel of metabolic tests. Results: We found that HAND2 is an obesity-linked white adipocyte transcription factor regulated by glucocorticoids that was necessary but insufficient for adipocyte differentiation in vitro. In a large cohort of humans, WAT HAND2 expression was correlated to BMI. The HAND2 gene was enriched in white adipocytes compared with brown, induced early in differentiation and responded to dexamethasone (DEX), a typical glucocorticoid receptor (GR, encoded by NR3C1) agonist. Silencing of NR3C1 in hMADS cells or deletion of GR in a transgenic conditional mouse model results in diminished HAND2 expression, establishing that adipocyte HAND2 is regulated by glucocorticoids via GR in vitro and in vivo. Furthermore, we identified gene clusters indirectly regulated by the GR–HAND2 pathway. Interestingly, silencing of HAND2 impaired adipocyte differentiation in hMADS and primary mouse adipocytes. However, a conditional adipocyte Hand2 deletion mouse model using Cre under control of the Adipoq promoter did not mirror these effects on adipose tissue differentiation, indicating that HAND2 was required at stages prior to Adipoq expression. Conclusions/interpretation: In summary, our study identifies HAND2 as a novel obesity-linked adipocyte transcription factor, highlighting new mechanisms of GR-dependent adipogenesis in humans and mice. Data availability: Array data have been submitted to the GEO database at NCBI (GSE148699). Graphical abstract: [Figure not available: see fulltext.]

KW - Adipocytes

KW - Dexamethasone

KW - Differentiation

KW - Glucocorticoid receptor

KW - HAND2

KW - Human adipose tissue

KW - Mesenchymal stem cells

KW - Obesity

KW - Transcription factor

KW - hMADS

UR - https://www.scopus.com/pages/publications/85105991851

U2 - 10.1007/s00125-021-05470-y

DO - 10.1007/s00125-021-05470-y

M3 - Article

C2 - 34014371

AN - SCOPUS:85105991851

SN - 0012-186X

VL - 64

SP - 1850

EP - 1865

JO - Diabetologia

JF - Diabetologia

IS - 8

ER -

HAND2 is a novel obesity-linked adipogenic transcription factor regulated by glucocorticoid signalling

Abstract

UN SDGs

Keywords

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