Your search keyword '"Bos, Trijnie"' showing total 26 results

1. Precision-cut liver slices as an ex vivo model to assess impaired hepatic glucose production

Author

Kiyuna, Ligia Akemi, Krishnamurthy, Kishore Alagere, Homan, Esther B., Langelaar-Makkinje, Miriam, Gerding, Albert, Bos, Trijnie, Oosterhuis, Dorenda, Overduin, Ruben J., Schreuder, Andrea B., de Meijer, Vincent E., Olinga, Peter, Derks, Terry G. J., van Eunen, Karen, Bakker, Barbara M., and Oosterveer, Maaike H.

Published

2024

2. Hepatic glucokinase regulatory protein and carbohydrate response element binding protein attenuation reduce de novo lipogenesis but do not mitigate intrahepatic triglyceride accumulation in Aldob deficiency

Author

Buziau, Amée M., Oosterveer, Maaike H., Wouters, Kristiaan, Bos, Trijnie, Tolan, Dean R., Agius, Loranne, Ford, Brian E., Cassiman, David, Stehouwer, Coen D.A., Schalkwijk, Casper G., and Brouwers, Martijn C.G.J.

Published

2024

3. Normalization of hepatic ChREBP activity does not protect against liver disease progression in a mouse model for Glycogen Storage Disease type Ia

Author

Rutten, Martijn G. S., Lei, Yu, Hoogerland, Joanne H., Bloks, Vincent W., Yang, Hong, Bos, Trijnie, Krishnamurthy, Kishore A., Bleeker, Aycha, Koster, Mirjam H., Thomas, Rachel E., Wolters, Justina C., van den Bos, Hilda, Mithieux, Gilles, Rajas, Fabienne, Mardinoglu, Adil, Spierings, Diana C. J., de Bruin, Alain, van de Sluis, Bart, and Oosterveer, Maaike H.

Published

2023

4. Precision-cut liver slices as an ex vivo model to assess impaired hepatic glucose production

Author

Bakker, Barbara, primary, Kiyuna, Ligia Akemi, additional, Krishnamurthy, Kishore Alagere, additional, Langelaar-Makkinje, Miriam, additional, Gerding, Albert, additional, Bos, Trijnie, additional, Oosterhuis, Dorenda, additional, Overduin, Ruben, additional, Schreuder, Andrea B., additional, De Meijer, Vincent, additional, Olinga, Peter, additional, Derks, Terry G.J., additional, Eunen, Karen van, additional, and Oosterveer, Maaike H., additional

Published

2023

5. Normalization of hepatic ChREBP activity does not protect against liver disease progression in a mouse model for Glycogen Storage Disease type Ia

Author

Rutten, Martijn G S, Lei, Yu, Hoogerland, Joanne H, Bloks, Vincent W, Yang, Hong, Bos, Trijnie, Krishnamurthy, Kishore A, Bleeker, Aycha, Koster, Mirjam H, Thomas, Rachel E, Wolters, Justina C, van den Bos, Hilda, Mithieux, Gilles, Rajas, Fabienne, Mardinoglu, Adil, Spierings, Diana C J, de Bruin, Alain, van de Sluis, Bart, Oosterveer, Maaike H, Rutten, Martijn G S, Lei, Yu, Hoogerland, Joanne H, Bloks, Vincent W, Yang, Hong, Bos, Trijnie, Krishnamurthy, Kishore A, Bleeker, Aycha, Koster, Mirjam H, Thomas, Rachel E, Wolters, Justina C, van den Bos, Hilda, Mithieux, Gilles, Rajas, Fabienne, Mardinoglu, Adil, Spierings, Diana C J, de Bruin, Alain, van de Sluis, Bart, and Oosterveer, Maaike H

Abstract

BACKGROUND: Glycogen storage disease type 1a (GSD Ia) is an inborn error of metabolism caused by a defect in glucose-6-phosphatase (G6PC1) activity, which induces severe hepatomegaly and increases the risk for liver cancer. Hepatic GSD Ia is characterized by constitutive activation of Carbohydrate Response Element Binding Protein (ChREBP), a glucose-sensitive transcription factor. Previously, we showed that ChREBP activation limits non-alcoholic fatty liver disease (NAFLD) in hepatic GSD Ia. As ChREBP has been proposed as a pro-oncogenic molecular switch that supports tumour progression, we hypothesized that ChREBP normalization protects against liver disease progression in hepatic GSD Ia.METHODS: Hepatocyte-specific G6pc knockout (L-G6pc -/-) mice were treated with AAV-shChREBP to normalize hepatic ChREBP activity. RESULTS: Hepatic ChREBP normalization in GSD Ia mice induced dysplastic liver growth, massively increased hepatocyte size, and was associated with increased hepatic inflammation. Furthermore, nuclear levels of the oncoprotein Yes Associated Protein (YAP) were increased and its transcriptional targets were induced in ChREBP-normalized GSD Ia mice. Hepatic ChREBP normalization furthermore induced DNA damage and mitotic activity in GSD Ia mice, while gene signatures of chromosomal instability, the cytosolic DNA-sensing cGAS-STING pathway, senescence, and hepatocyte dedifferentiation emerged.CONCLUSIONS: In conclusion, our findings indicate that ChREBP activity limits hepatomegaly while decelerating liver disease progression and protecting against chromosomal instability in hepatic GSD Ia. These results disqualify ChREBP as a therapeutic target for treatment of liver disease in GSD Ia. In addition, they underline the importance of establishing the context-specific roles of hepatic ChREBP to define its therapeutic potential to prevent or treat advanced liver disease.

Published

2023

6. Normalization of hepatic ChREBP activity does not protect against liver disease progression in a mouse model for Glycogen Storage Disease type Ia

Author

Pathobiologie, Dep Biomolecular Health Sciences, Rutten, Martijn G S, Lei, Yu, Hoogerland, Joanne H, Bloks, Vincent W, Yang, Hong, Bos, Trijnie, Krishnamurthy, Kishore A, Bleeker, Aycha, Koster, Mirjam H, Thomas, Rachel E, Wolters, Justina C, van den Bos, Hilda, Mithieux, Gilles, Rajas, Fabienne, Mardinoglu, Adil, Spierings, Diana C J, de Bruin, Alain, van de Sluis, Bart, Oosterveer, Maaike H, Pathobiologie, Dep Biomolecular Health Sciences, Rutten, Martijn G S, Lei, Yu, Hoogerland, Joanne H, Bloks, Vincent W, Yang, Hong, Bos, Trijnie, Krishnamurthy, Kishore A, Bleeker, Aycha, Koster, Mirjam H, Thomas, Rachel E, Wolters, Justina C, van den Bos, Hilda, Mithieux, Gilles, Rajas, Fabienne, Mardinoglu, Adil, Spierings, Diana C J, de Bruin, Alain, van de Sluis, Bart, and Oosterveer, Maaike H

Published

2023

7. Normalization of hepatic ChREBP activity does not protect against liver disease progression in a mouse model for Glycogen Storage Disease type Ia

Author

Rutten, Martijn G.S., primary, Lei, Yu, additional, Hoogerland, Joanne H., additional, Bloks, Vincent W., additional, Yang, Hong, additional, Bos, Trijnie, additional, Krishnamurthy, Kishore A., additional, Bleeker, Aycha, additional, Koster, Mirjam H., additional, Thomas, Rachel E., additional, Wolters, Justina C., additional, Bos, Hilda van den, additional, Mithieux, Gilles, additional, Rajas, Fabienne, additional, Mardinoglu, Adil, additional, Spierings, Diana C.J., additional, de Bruin, Alain, additional, de Sluis, Bart van, additional, and Oosterveer, Maaike H., additional

Published

2023

8. Gut microbiota inhibit Asbt-dependent intestinal bile acid reabsorption via Gata4

Author

Out, Carolien, Patankar, Jay V., Doktorova, Marcela, Boesjes, Marije, Bos, Trijnie, de Boer, Sanna, Havinga, Rick, Wolters, Henk, Boverhof, Renze, van Dijk, Theo H., Smoczek, Anna, Bleich, André, Sachdev, Vinay, Kratky, Dagmar, Kuipers, Folkert, Verkade, Henkjan J., and Groen, Albert K.

Published

2015

9. Precision-cut liver slices as an ex vivo model to assess impaired hepatic glucose production

Author

Krishnamurthy, Kishore Alagere, primary, Kiyuna, Ligia Akemi, additional, Langelaar, Miriam, additional, Gerding, Albert, additional, Bos, Trijnie, additional, Oosterhuis, Dorenda, additional, Olinga, Peter, additional, Van Eunen, Karen, additional, Bakker, Barbara, additional, and Oosterveer, Maaike, additional

Published

2022

10. Modeling Phenotypic Heterogeneity of Glycogen Storage Disease Type 1a Liver Disease in Mice by Somatic CRISPR/CRISPR-associated protein 9–Mediated Gene Editing

Author

Rutten, Martijn G S, Derks, Terry G J, Huijkman, Nicolette C A, Bos, Trijnie, Kloosterhuis, Niels J, van de Kolk, Kees C W A, Wolters, Justina C, Koster, Mirjam H, Bongiovanni, Laura, Thomas, Rachel E, de Bruin, Alain, van de Sluis, Bart, Oosterveer, Maaike H, LS Pathobiologie, dPB RMSC, Dep Biomolecular Health Sciences, Pathobiologie, LS Pathobiologie, dPB RMSC, Dep Biomolecular Health Sciences, Pathobiologie, Center for Liver, Digestive and Metabolic Diseases (CLDM), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

Male, INTESTINAL GLUCONEOGENESIS, G6PC, Liver tumor, GLUCOSE-PRODUCTION, Genetic Vectors, Disease, Glycogen Storage Disease Type I, Hypoglycemia, Bioinformatics, THERAPY, Steatohepatitis/Metabolic Liver Disease, Genetic Heterogeneity, Mice, Liver disease, CRISPR-Associated Protein 9, MANAGEMENT, medicine, Animals, CRISPR, Glycogen storage disease, Clustered Regularly Interspaced Short Palindromic Repeats, Gene Editing, Mice, Knockout, Hepatology, IA, Genetic heterogeneity, business.industry, INDUCTION, nutritional and metabolic diseases, Original Articles, medicine.disease, PREVENTION, Mice, Inbred C57BL, Disease Models, Animal, Phenotype, HEPATOCELLULAR ADENOMA FORMATION, Glucose-6-Phosphatase, Hepatocytes, SURVIVAL, Original Article, HEPATIC GLUCOSE-6-PHOSPHATASE-ALPHA ACTIVITY, business

Abstract

Background and Aims Patients with glycogen storage disease type 1a (GSD-1a) primarily present with life-threatening hypoglycemia and display severe liver disease characterized by hepatomegaly. Despite strict dietary management, long-term complications still occur, such as liver tumor development. Variations in residual glucose-6-phosphatase (G6PC1) activity likely contribute to phenotypic heterogeneity in biochemical symptoms and complications between patients. However, lack of insight into the relationship between G6PC1 activity and symptoms/complications and poor understanding of the underlying disease mechanisms pose major challenges to provide optimal health care and quality of life for GSD-1a patients. Currently available GSD-1a animal models are not suitable to systematically investigate the relationship between hepatic G6PC activity and phenotypic heterogeneity or the contribution of gene-gene interactions (GGIs) in the liver. Approach and Results To meet these needs, we generated and characterized a hepatocyte-specific GSD-1a mouse model using somatic CRISPR/CRISPR-associated protein 9 (Cas9)-mediated gene editing. Hepatic G6pc editing reduced hepatic G6PC activity up to 98% and resulted in failure to thrive, fasting hypoglycemia, hypertriglyceridemia, hepatomegaly, hepatic steatosis (HS), and increased liver tumor incidence. This approach was furthermore successful in simultaneously modulating hepatic G6PC and carbohydrate response element-binding protein, a transcription factor that is activated in GSD-1a and protects against HS under these conditions. Importantly, it also allowed for the modeling of a spectrum of GSD-1a phenotypes in terms of hepatic G6PC activity, fasting hypoglycemia, hypertriglyceridemia, hepatomegaly and HS. Conclusions In conclusion, we show that somatic CRISPR/Cas9-mediated gene editing allows for the modeling of a spectrum of hepatocyte-borne GSD-1a disease symptoms in mice and to efficiently study GGIs in the liver. This approach opens perspectives for translational research and will likely contribute to personalized treatments for GSD-1a and other genetic liver diseases.

Published

2021

11. Disrupted glucose-6-phosphate-ChREBP signalling aggravates hepatomegaly and accelerates liver disease progression in a mouse model for Glycogen Storage Disease type 1a

Author

Rutten, Martijn, Lei, Yu, Hoogerland, Joanne, Bos, Trijnie, Bleeker, Aycha, Thomas, Rachel, Mithieux, Gilles, Rajas, Fabienne, de Bruin, Alain, van de Sluis, Bart, Oosterveer, Maaike, Center for Liver, Digestive and Metabolic Diseases (CLDM), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Published

2021

12. Modeling Phenotypic Heterogeneity of Glycogen Storage Disease Type 1a Liver Disease in Mice by Somatic CRISPR/CRISPR-associated protein 9–Mediated Gene Editing

Author

LS Pathobiologie, dPB RMSC, Dep Biomolecular Health Sciences, Pathobiologie, Rutten, Martijn G S, Derks, Terry G J, Huijkman, Nicolette C A, Bos, Trijnie, Kloosterhuis, Niels J, van de Kolk, Kees C W A, Wolters, Justina C, Koster, Mirjam H, Bongiovanni, Laura, Thomas, Rachel E, de Bruin, Alain, van de Sluis, Bart, Oosterveer, Maaike H, LS Pathobiologie, dPB RMSC, Dep Biomolecular Health Sciences, Pathobiologie, Rutten, Martijn G S, Derks, Terry G J, Huijkman, Nicolette C A, Bos, Trijnie, Kloosterhuis, Niels J, van de Kolk, Kees C W A, Wolters, Justina C, Koster, Mirjam H, Bongiovanni, Laura, Thomas, Rachel E, de Bruin, Alain, van de Sluis, Bart, and Oosterveer, Maaike H

Published

2021

13. Impaired Very‐Low‐Density Lipoprotein catabolism links hypoglycemia to hypertriglyceridemia in Glycogen Storage Disease type Ia

Author

Hoogerland, Joanne A., primary, Peeks, Fabian, additional, Hijmans, Brenda S., additional, Wolters, Justina C., additional, Kooijman, Sander, additional, Bos, Trijnie, additional, Bleeker, Aycha, additional, Dijk, Theo H., additional, Wolters, Henk, additional, Gerding, Albert, additional, Eunen, Karen, additional, Havinga, Rick, additional, Pronk, Amanda C. M., additional, Rensen, Patrick C. N., additional, Mithieux, Gilles, additional, Rajas, Fabienne, additional, Kuipers, Folkert, additional, Reijngoud, Dirk‐Jan, additional, Derks, Terry G. J., additional, and Oosterveer, Maaike H., additional

Published

2021

14. Hepatic ChREBP activation limits NAFLD development in a mouse model for Glycogen Storage Disease type Ia

Author

Lei, Yu, Hoogerland, Joanne A, Bloks, Vincent W, Bos, Trijnie, Bleeker, Aycha, Wolters, Henk, Wolters, Justina C, Hijmans, Brenda S, van Dijk, Theo H, Thomas, Rachel, van Weeghel, Michel, Mithieux, Gilles, Houtkooper, Riekelt H, de Bruin, Alain, Rajas, Fabienne, Kuipers, Folkert, Oosterveer, Maaike H, Lei, Yu, Hoogerland, Joanne A, Bloks, Vincent W, Bos, Trijnie, Bleeker, Aycha, Wolters, Henk, Wolters, Justina C, Hijmans, Brenda S, van Dijk, Theo H, Thomas, Rachel, van Weeghel, Michel, Mithieux, Gilles, Houtkooper, Riekelt H, de Bruin, Alain, Rajas, Fabienne, Kuipers, Folkert, and Oosterveer, Maaike H

Abstract

Glycogen storage disease type Ia (GSD Ia) is an inborn error of metabolism caused by defective glucose-6-phosphatase (G6PC) activity. GSD Ia patients exhibit severe hepatomegaly due to glycogen and triglyceride (TG) accumulation in the liver. We have previously shown that the activity of Carbohydrate Response Element Binding Protein (ChREBP), a key regulator of glycolysis and de novo lipogenesis, is increased in GSD Ia. In the current study we assessed the contribution of ChREBP to non-alcoholic fatty liver disease (NAFLD) development in a mouse model for hepatic GSD Ia. Liver-specific G6pc knockout (L-G6pc-/- ) mice were treated with AAV2/8-shChREBP to normalize hepatic ChREBP activity to levels observed in wildtype (L-G6pc+/+ ) mice receiving AAV8-shScramble. Hepatic ChREBP knockdown markedly increased liver weight and hepatocyte size in L-G6pc-/- mice. This was associated with hepatic accumulation of G6P, glycogen and lipids, while the expression of glycolytic and lipogenic genes was reduced. Enzyme activities, flux measurements, hepatic metabolite analysis and VLDL-TG secretion assays revealed that hepatic ChREBP knockdown reduced downstream glycolysis and de novo lipogenesis, but also strongly suppressed hepatic VLDL lipidation hence promoting the storage of 'old fat'. Interestingly, enhanced VLDL-TG secretion in shScramble-treated L-G6pc-/- mice associated with a ChREBP-dependent induction of the VLDL lipidation proteins MTTP and TM6SF2, the latter being confirmed by ChIP-PCR. CONCLUSION: Attenuation of hepatic ChREBP induction in GSD Ia liver aggravates hepatomegaly due to further accumulation of glycogen and lipids as a result of reduced glycolysis and suppressed VLDL-TG secretion. TM6SF2, critical for VLDL formation, was identified as a novel ChREBP target in mouse liver. Altogether, our data show that enhanced ChREBP activity limits NAFLD development in GSD Ia by balancing hepatic TG production and -secretion.

Published

2020

15. Hepatic ChREBP activation limits NAFLD development in a mouse model for Glycogen Storage Disease type Ia

Author

Pathobiologie, dPB RMSC, Dep Biomolecular Health Sciences, Lei, Yu, Hoogerland, Joanne A, Bloks, Vincent W, Bos, Trijnie, Bleeker, Aycha, Wolters, Henk, Wolters, Justina C, Hijmans, Brenda S, van Dijk, Theo H, Thomas, Rachel, van Weeghel, Michel, Mithieux, Gilles, Houtkooper, Riekelt H, de Bruin, Alain, Rajas, Fabienne, Kuipers, Folkert, Oosterveer, Maaike H, Pathobiologie, dPB RMSC, Dep Biomolecular Health Sciences, Lei, Yu, Hoogerland, Joanne A, Bloks, Vincent W, Bos, Trijnie, Bleeker, Aycha, Wolters, Henk, Wolters, Justina C, Hijmans, Brenda S, van Dijk, Theo H, Thomas, Rachel, van Weeghel, Michel, Mithieux, Gilles, Houtkooper, Riekelt H, de Bruin, Alain, Rajas, Fabienne, Kuipers, Folkert, and Oosterveer, Maaike H

Published

2020

16. Essential fatty acid deficiency in mice is associated with hepatic steatosis and secretion of large VLDL particles

Author

Werner, Anniek, Havinga, Rick, Bos, Trijnie, Bloks, Vincent W., Kuipers, Folkert, and Verkade, Henkjan J.

Subjects

Mice -- Research, Mice -- Physiological aspects, Essential fatty acids -- Research, Essential fatty acids -- Physiological aspects, Biological sciences

Abstract

Essential fatty acid (EFA) deficiency in mice decreases plasma triglyceride (TG) concentrations and increases hepatic TG content. We evaluated in vivo and in vitro whether decreased hepatic secretion of TG-rich very low-density lipoprotein (VLDL) contributes to this consequence of EFA deficiency. EFA deficiency was induced in mice by feeding an EFA-deficient (EFAD) diet for 8 wk. Hepatic VLDL secretion was quantified in fasted EFAD and EFA-sufficient (EFAS) mice using the Triton WR-1339 method. In cultured hepatocytes from EFAD and EFAS mice, VLDL secretion into medium was measured by quantifying [[sup.3]H]-labeled glycerol incorporation into TG and phospholipids. Hepatic expression of genes involved in VLDL synthesis and clearance was measured, as were plasma activities of lipolytic enzymes. TG secretion rates were quantitatively similar in EFAD and EFAS mice in vivo and in primary hepatocytes from EFAD and EFAS mice in vitro. However, EFA deficiency increased the size of secreted VLDL particles, as determined by calculation of particle diameter, particle sizing by light scattering, and evaluation of the TG-to-apoB ratio. EFA deficiency did not inhibit hepatic lipase and lipoprotein lipase activities in plasma, but increased hepatic mRNA levels of apoAV and apoCII, both involved in control of lipolytic degradation of TG-rich lipoproteins. EFA deficiency does not affect hepatic TG secretion rate in mice, but increases the size of secreted VLDL particles. Present data suggest that hypotriglyceridemia during EFA deficiency is related to enhanced clearance of altered VLDL particles. hepatic lipoprotein secretion: lipoprotein clearance; hypotriglyceridemia

Published

2005

17. Liver receptor homolog-1 is critical for adequate up-regulation of Cyp7a1 gene transcription and bile salt synthesis during bile salt sequestration

Author

Out, Carolien, Hageman, Jurre, Bloks, Vincent W., Gerrits, Han, Gelpke, Maarten D. Sollewijn, Bos, Trijnie, Havinga, Rick, Smit, Martin J., Kuipers, Folkert, and Groen, Albert K.

Published

2011

18. Hepatic Carbohydrate Response Element Binding Protein Activation Limits Nonalcoholic Fatty Liver Disease Development in a Mouse Model for Glycogen Storage Disease Type 1a

Author

Lei, Yu, primary, Hoogerland, Joanne A., additional, Bloks, Vincent W., additional, Bos, Trijnie, additional, Bleeker, Aycha, additional, Wolters, Henk, additional, Wolters, Justina C., additional, Hijmans, Brenda S., additional, Dijk, Theo H., additional, Thomas, Rachel, additional, Weeghel, Michel, additional, Mithieux, Gilles, additional, Houtkooper, Riekelt H., additional, Bruin, Alain, additional, Rajas, Fabienne, additional, Kuipers, Folkert, additional, and Oosterveer, Maaike H., additional

Published

2020

19. Glucose‐6‐Phosphate Regulates Hepatic Bile Acid Synthesis in Mice

Author

Hoogerland, Joanne A., primary, Lei, Yu, additional, Wolters, Justina C., additional, de Boer, Jan Freark, additional, Bos, Trijnie, additional, Bleeker, Aycha, additional, Mulder, Niels L., additional, van Dijk, Theo H., additional, Kuivenhoven, Jan A., additional, Rajas, Fabienne, additional, Mithieux, Gilles, additional, Haeusler, Rebecca A., additional, Verkade, Henkjan J., additional, Bloks, Vincent W., additional, Kuipers, Folkert, additional, and Oosterveer, Maaike H., additional

Published

2019

20. Resistance to diet-induced adiposity in cannabinoid receptor-1 deficient mice is not due to impaired adipocyte function

Author

Oosterveer Maaike H, Koolman Anniek H, de Boer Pieter T, Bos Trijnie, Bleeker Aycha, van Dijk Theo H, Bloks Vincent W, Kuipers Folkert, Sauer Pieter JJ, and van Dijk Gertjan

Subjects

CB1-receptor, diet-induced adiposity, fat tissue, lipogenesis, lipolysis, Nutrition. Foods and food supply, TX341-641, Nutritional diseases. Deficiency diseases, RC620-627

Abstract

Abstract Background Overactivity and/or dysregulation of the endocannabinoid system (ECS) contribute to development of obesity. In vitro studies indicate a regulatory role for the cannabinoid receptor 1 (CB1) in adipocyte function and CB1-receptor deficient (CB1-/-) mice are resistant to high fat diet-induced obesity. Whether this phenotype of CB1-/- mice is related to altered fat metabolism in adipose tissue is unknown. Methods We evaluated adipose tissue differentiation/proliferation markers and quantified lipogenic and lipolytic activities in fat tissues of CB1-/- and CB1+/+ mice fed a high-fat (HF) or a high-fat/fish oil (HF/FO) diet as compared to animals receiving a low-fat chow diet. Comparison between HF diet and HF/FO diet allowed to investigate the influence of dietary fat quality on adipose tissue biology in relation to CB1 functioning. Results The adiposity-resistant phenotype of the CB1-/- mice was characterized by reduced fat mass and adipocyte size in HF and HF/FO-fed CB1-/- mice in parallel to a significant increase in energy expenditure as compared to CB1+/+ mice. The expression levels of adipocyte differentiation and proliferation markers were however maintained in these animals. Consistent with unaltered lipogenic gene expression, the fatty acid synthesis rates in adipose tissues from CB1-/- and CB1+/+ mice were unchanged. Whole-body and adipose-specific lipoprotein lipase (LPL) activities were also not altered in CB1-/- mice. Conclusions These findings indicate that protection against diet-induced adiposity in CB1-deficient mice is not related to changes in adipocyte function per se, but rather results from increased energy dissipation by oxidative and non-oxidative pathways.

Published

2011

21. Hepatic Carbohydrate Response Element Binding Protein Activation Limits Nonalcoholic Fatty Liver Disease Development in a Mouse Model for Glycogen Storage Disease Type 1a.

Author

Yu Lei, Hoogerland, Joanne A., Bloks, Vincent W., Bos, Trijnie, Bleeker, Aycha, Wolters, Henk, Wolters, Justina C., Hijmans, Brenda S., van Dijk, Theo H., Thomas, Rachel, van Weeghel, Michel, Mithieux, Gilles, Houtkooper, Riekelt H., de Bruin, Alain, Rajas, Fabienne, Kuipers, Folkert, and Oosterveer, Maaike H.

Published

2020

22. Intestinal Farnesoid X Receptor Controls Transintestinal Cholesterol Excretion in Mice

Author

de Boer, Jan Freark, primary, Schonewille, Marleen, additional, Boesjes, Marije, additional, Wolters, Henk, additional, Bloks, Vincent W., additional, Bos, Trijnie, additional, van Dijk, Theo H., additional, Jurdzinski, Angelika, additional, Boverhof, Renze, additional, Wolters, Justina C., additional, Kuivenhoven, Jan A., additional, van Deursen, Jan M., additional, Oude Elferink, Ronald P.J., additional, Moschetta, Antonio, additional, Kremoser, Claus, additional, Verkade, Henkjan J., additional, Kuipers, Folkert, additional, and Groen, Albert K., additional

Published

2017

23. Abstract 424: Transintestinal Cholesterol Excretion Can Drive Massive Cholesterol Elimination in Mice

Author

De Boer, Jan F, primary, Schonewille, Marleen, additional, Boesjes, Marije, additional, Wolters, Henk, additional, Bloks, Vincent W, additional, Bos, Trijnie, additional, Van Dijk, Theo H, additional, Jurdzinski, Angelika, additional, Boverhof, Renze, additional, Van Deursen, Jan M, additional, Oude Elferink, Ronald P, additional, Moschetta, Antonio, additional, Kremoser, Claus, additional, Verkade, Henkjan J, additional, Kuipers, Folkert, additional, and Groen, Albert K, additional

Published

2016

24. Hepatic Farnesoid X-Receptor Isoforms α2 and α4 Differentially Modulate Bile Salt and Lipoprotein Metabolism in Mice

Author

Boesjes, Marije, primary, Bloks, Vincent W., additional, Hageman, Jurre, additional, Bos, Trijnie, additional, van Dijk, Theo H., additional, Havinga, Rick, additional, Wolters, Henk, additional, Jonker, Johan W., additional, Kuipers, Folkert, additional, and Groen, Albert K., additional

Published

2014

25. Resistance to diet-induced adiposity in cannabinoid receptor-1 deficient mice is not due to impaired adipocyte function

Author

Oosterveer, Maaike H., Koolman, Anniek H., de Boer, Pieter T., Bos, Trijnie, Bleeker, Aycha, Bloks, Vincent W., Kuipers, Folkert, Sauer, Pieter J. J., van Dijk, Gertjan, Oosterveer, Maaike H., Koolman, Anniek H., de Boer, Pieter T., Bos, Trijnie, Bleeker, Aycha, Bloks, Vincent W., Kuipers, Folkert, Sauer, Pieter J. J., and van Dijk, Gertjan

Abstract

Background: Overactivity and/or dysregulation of the endocannabinoid system (ECS) contribute to development of obesity. In vitro studies indicate a regulatory role for the cannabinoid receptor 1 (CB1) in adipocyte function and CB1-receptor deficient (CB1-/-) mice are resistant to high fat diet-induced obesity. Whether this phenotype of CB1-/- mice is related to altered fat metabolism in adipose tissue is unknown.Methods: We evaluated adipose tissue differentiation/proliferation markers and quantified lipogenic and lipolytic activities in fat tissues of CB1-/- and CB1+/+ mice fed a high-fat (HF) or a high-fat/fish oil (HF/FO) diet as compared to animals receiving a low-fat chow diet. Comparison between HF diet and HF/FO diet allowed to investigate the influence of dietary fat quality on adipose tissue biology in relation to CB1 functioning.Results: The adiposity-resistant phenotype of the CB1-/- mice was characterized by reduced fat mass and adipocyte size in HF and HF/FO-fed CB1-/- mice in parallel to a significant increase in energy expenditure as compared to CB1+/+ mice. The expression levels of adipocyte differentiation and proliferation markers were however maintained in these animals. Consistent with unaltered lipogenic gene expression, the fatty acid synthesis rates in adipose tissues from CB1-/- and CB1+/+ mice were unchanged. Whole-body and adipose-specific lipoprotein lipase (LPL) activities were also not altered in CB1-/- mice.Conclusions: These findings indicate that protection against diet-induced adiposity in CB1-deficient mice is not related to changes in adipocyte function per se, but rather results from increased energy dissipation by oxidative and non-oxidative pathways.

Published

2011

26. Modeling Phenotypic Heterogeneity of Glycogen Storage Disease Type 1a Liver Disease in Mice by Somatic CRISPR/CRISPR-associated protein 9-Mediated Gene Editing.

Author

Rutten MGS, Derks TGJ, Huijkman NCA, Bos T, Kloosterhuis NJ, van de Kolk KCWA, Wolters JC, Koster MH, Bongiovanni L, Thomas RE, de Bruin A, van de Sluis B, and Oosterveer MH

Subjects

Animals, Genetic Vectors, Glucose-6-Phosphatase genetics, Glucose-6-Phosphatase metabolism, Hepatocytes enzymology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, CRISPR-Associated Protein 9 genetics, Clustered Regularly Interspaced Short Palindromic Repeats genetics, Disease Models, Animal, Gene Editing methods, Genetic Heterogeneity, Glycogen Storage Disease Type I genetics, Phenotype

Abstract

Background and Aims: Patients with glycogen storage disease type 1a (GSD-1a) primarily present with life-threatening hypoglycemia and display severe liver disease characterized by hepatomegaly. Despite strict dietary management, long-term complications still occur, such as liver tumor development. Variations in residual glucose-6-phosphatase (G6PC1) activity likely contribute to phenotypic heterogeneity in biochemical symptoms and complications between patients. However, lack of insight into the relationship between G6PC1 activity and symptoms/complications and poor understanding of the underlying disease mechanisms pose major challenges to provide optimal health care and quality of life for GSD-1a patients. Currently available GSD-1a animal models are not suitable to systematically investigate the relationship between hepatic G6PC activity and phenotypic heterogeneity or the contribution of gene-gene interactions (GGIs) in the liver., Approach and Results: To meet these needs, we generated and characterized a hepatocyte-specific GSD-1a mouse model using somatic CRISPR/CRISPR-associated protein 9 (Cas9)-mediated gene editing. Hepatic G6pc editing reduced hepatic G6PC activity up to 98% and resulted in failure to thrive, fasting hypoglycemia, hypertriglyceridemia, hepatomegaly, hepatic steatosis (HS), and increased liver tumor incidence. This approach was furthermore successful in simultaneously modulating hepatic G6PC and carbohydrate response element-binding protein, a transcription factor that is activated in GSD-1a and protects against HS under these conditions. Importantly, it also allowed for the modeling of a spectrum of GSD-1a phenotypes in terms of hepatic G6PC activity, fasting hypoglycemia, hypertriglyceridemia, hepatomegaly and HS., Conclusions: In conclusion, we show that somatic CRISPR/Cas9-mediated gene editing allows for the modeling of a spectrum of hepatocyte-borne GSD-1a disease symptoms in mice and to efficiently study GGIs in the liver. This approach opens perspectives for translational research and will likely contribute to personalized treatments for GSD-1a and other genetic liver diseases., (© 2021 The Authors. Hepatology published by Wiley Periodicals LLC on behalf of American Association for the Study of Liver Diseases.)

Published

2021