Your search keyword '"Julie Massart"' showing total 4 results

1. Regulation of glucose uptake and inflammation markers by FOXO1 and FOXO3 in skeletal muscle

Author

Leonidas S. Lundell, Julie Massart, Ali Altıntaş, Anna Krook, and Juleen R. Zierath

Subjects

Internal medicine, RC31-1245

Abstract

Objective: Forkhead box class O (FOXO) transcription factors regulate whole body energy metabolism, skeletal muscle mass, and substrate switching. FOXO1 and FOXO3 are highly abundant transcription factors, but their precise role in skeletal muscle metabolism has not been fully elucidated. Methods: To elucidate the role of FOXO in skeletal muscle, dominant negative (dn) constructs for FOXO1 (FOXO1dn) or FOXO3 (FOXO3dn) were transfected by electroporation into mouse tibialis anterior muscle and glucose uptake, signal transduction, and gene expression profiles were assessed after an oral glucose tolerance test. Results were compared against contralateral control transfected muscle. Results: FOXO1dn and FOXO3dn attenuated glucose uptake (35%, p

Published

2019

2. High-fat diet reprograms the epigenome of rat spermatozoa and transgenerationally affects metabolism of the offspring

Author

Thais de Castro Barbosa, Lars R. Ingerslev, Petter S. Alm, Soetkin Versteyhe, Julie Massart, Morten Rasmussen, Ida Donkin, Rasmus Sjögren, Jonathan M. Mudry, Laurène Vetterli, Shashank Gupta, Anna Krook, Juleen R. Zierath, and Romain Barrès

Subjects

Internal medicine, RC31-1245

Abstract

Objectives: Chronic and high consumption of fat constitutes an environmental stress that leads to metabolic diseases. We hypothesized that high-fat diet (HFD) transgenerationally remodels the epigenome of spermatozoa and metabolism of the offspring. Methods: F0-male rats fed either HFD or chow diet for 12 weeks were mated with chow-fed dams to generate F1 and F2 offspring. Motile spermatozoa were isolated from F0 and F1 breeders to determine DNA methylation and small non-coding RNA (sncRNA) expression pattern by deep sequencing. Results: Newborn offspring of HFD-fed fathers had reduced body weight and pancreatic beta-cell mass. Adult female, but not male, offspring of HFD-fed fathers were glucose intolerant and resistant to HFD-induced weight gain. This phenotype was perpetuated in the F2 progeny, indicating transgenerational epigenetic inheritance. The epigenome of spermatozoa from HFD-fed F0 and their F1 male offspring showed common DNA methylation and small non-coding RNA expression signatures. Altered expression of sperm miRNA let-7c was passed down to metabolic tissues of the offspring, inducing a transcriptomic shift of the let-7c predicted targets. Conclusion: Our results provide insight into mechanisms by which HFD transgenerationally reprograms the epigenome of sperm cells, thereby affecting metabolic tissues of offspring throughout two generations. Keywords: Epigenetics, Obesity, Spermatozoa, DNA methylation, microRNA

Published

2016

3. Bioenergetic cues shift FXR splicing towards FXRα2 to modulate hepatic lipolysis and fatty acid metabolism

Author

Jorge C. Correia, Julie Massart, Jan Freark de Boer, Margareta Porsmyr-Palmertz, Vicente Martínez-Redondo, Leandro Z. Agudelo, Indranil Sinha, David Meierhofer, Vera Ribeiro, Marie Björnholm, Sascha Sauer, Karin Dahlman-Wright, Juleen R. Zierath, Albert K. Groen, and Jorge L. Ruas

Subjects

FXR isoforms, Splicing, NAFLD, Insulin resistance, Energy metabolism, Internal medicine, RC31-1245

Abstract

Objective: Farnesoid X receptor (FXR) plays a prominent role in hepatic lipid metabolism. The FXR gene encodes four proteins with structural differences suggestive of discrete biological functions about which little is known. Methods: We expressed each FXR variant in primary hepatocytes and evaluated global gene expression, lipid profile, and metabolic fluxes. Gene delivery of FXR variants to Fxr−/− mouse liver was performed to evaluate their role in vivo. The effects of fasting and physical exercise on hepatic Fxr splicing were determined. Results: We show that FXR splice isoforms regulate largely different gene sets and have specific effects on hepatic metabolism. FXRα2 (but not α1) activates a broad transcriptional program in hepatocytes conducive to lipolysis, fatty acid oxidation, and ketogenesis. Consequently, FXRα2 decreases cellular lipid accumulation and improves cellular insulin signaling to AKT. FXRα2 expression in Fxr−/− mouse liver activates a similar gene program and robustly decreases hepatic triglyceride levels. On the other hand, FXRα1 reduces hepatic triglyceride content to a lesser extent and does so through regulation of lipogenic gene expression. Bioenergetic cues, such as fasting and exercise, dynamically regulate Fxr splicing in mouse liver to increase Fxrα2 expression. Conclusions: Our results show that the main FXR variants in human liver (α1 and α2) reduce hepatic lipid accumulation through distinct mechanisms and to different degrees. Taking this novel mechanism into account could greatly improve the pharmacological targeting and therapeutic efficacy of FXR agonists.

Published

2015

4. High-fat diet reprograms the epigenome of rat spermatozoa and transgenerationally affects metabolism of the offspring

Author

Jonathan M. Mudry, Morten Arendt Rasmussen, Petter S. Alm, Shashank Gupta, Juleen R. Zierath, Romain Barrès, Julie Massart, Rasmus J. O. Sjögren, Lars R. Ingerslev, Thais de Castro Barbosa, Laurène Vetterli, Ida Donkin, Soetkin Versteyhe, and Anna Krook

Subjects

0301 basic medicine, lcsh:Internal medicine, Offspring, 030209 endocrinology & metabolism, Biology, Transcriptome, Andrology, 03 medical and health sciences, 0302 clinical medicine, microRNA, medicine, Obesity, Epigenetics, lcsh:RC31-1245, Molecular Biology, 2. Zero hunger, Genetics, DNA methylation, digestive, oral, and skin physiology, food and beverages, Cell Biology, Epigenome, Spermatozoa, Sperm, 030104 developmental biology, Original Article, medicine.symptom, Weight gain

Abstract

Objectives Chronic and high consumption of fat constitutes an environmental stress that leads to metabolic diseases. We hypothesized that high-fat diet (HFD) transgenerationally remodels the epigenome of spermatozoa and metabolism of the offspring. Methods F0-male rats fed either HFD or chow diet for 12 weeks were mated with chow-fed dams to generate F1 and F2 offspring. Motile spermatozoa were isolated from F0 and F1 breeders to determine DNA methylation and small non-coding RNA (sncRNA) expression pattern by deep sequencing. Results Newborn offspring of HFD-fed fathers had reduced body weight and pancreatic beta-cell mass. Adult female, but not male, offspring of HFD-fed fathers were glucose intolerant and resistant to HFD-induced weight gain. This phenotype was perpetuated in the F2 progeny, indicating transgenerational epigenetic inheritance. The epigenome of spermatozoa from HFD-fed F0 and their F1 male offspring showed common DNA methylation and small non-coding RNA expression signatures. Altered expression of sperm miRNA let-7c was passed down to metabolic tissues of the offspring, inducing a transcriptomic shift of the let-7c predicted targets. Conclusion Our results provide insight into mechanisms by which HFD transgenerationally reprograms the epigenome of sperm cells, thereby affecting metabolic tissues of offspring throughout two generations., Highlights • Body weight and glucose metabolism are altered in F1 and F2 offspring of F0-HFD fathers. • High-fat diet reprograms the epigenome of sperm cells. • Spermatozoa from F0-HFD fathers and F1 offspring share common epigenetic signatures. • Expression of let-7c is changed in sperm of founders and in the adipose tissue of the offspring.

Published

2016