Search

Your search keyword '"Schönke, Milena"' showing total 137 results
Start Over Author "Schönke, Milena"
137 results on '"Schönke, Milena"'

1. FGF21 protects against hepatic lipotoxicity and macrophage activation to attenuate fibrogenesis in nonalcoholic steatohepatitis.

Author

Liu, Cong, Schönke, Milena, Spoorenberg, Borah, Lambooij, Joost, van der Zande, Hendrik, Zhou, Enchen, Tushuizen, Maarten, Andreasson, Anne-Christine, Park, Andrew, Oldham, Stephanie, Uhrbom, Martin, Ahlstedt, Ingela, Ikeda, Yasuhiro, Wallenius, Kristina, Peng, Xiao-Rong, Guigas, Bruno, Boon, Mariëtte, Wang, Yanan, and Rensen, Patrick

Subjects
fibroblast growth factor 21, immunology, inflammation, lipid/scar-associated macrophages, liver-adipose tissue crosstalk, medicine, mouse, steatohepatitis, Mice, Humans, Animals, Non-alcoholic Fatty Liver Disease, Diabetes Mellitus, Type 2, Macrophage Activation, Cicatrix, Liver, Inflammation, Diet, High-Fat, Cholesterol, Lipids, Mice, Inbred C57BL, Disease Models, Animal
Abstract

Analogues of the hepatokine fibroblast growth factor 21 (FGF21) are in clinical development for type 2 diabetes and nonalcoholic steatohepatitis (NASH) treatment. Although their glucose-lowering and insulin-sensitizing effects have been largely unraveled, the mechanisms by which they alleviate liver injury have only been scarcely addressed. Here, we aimed to unveil the mechanisms underlying the protective effects of FGF21 on NASH using APOE*3-Leiden.CETP mice, a well-established model for human-like metabolic diseases. Liver-specific FGF21 overexpression was achieved in mice, followed by administration of a high-fat high-cholesterol diet for 23 weeks. FGF21 prevented hepatic lipotoxicity, accompanied by activation of thermogenic tissues and attenuation of adipose tissue inflammation, improvement of hyperglycemia and hypertriglyceridemia, and upregulation of hepatic programs involved in fatty acid oxidation and cholesterol removal. Furthermore, FGF21 inhibited hepatic inflammation, as evidenced by reduced Kupffer cell (KC) activation, diminished monocyte infiltration, and lowered accumulation of monocyte-derived macrophages. Moreover, FGF21 decreased lipid- and scar-associated macrophages, which correlated with less hepatic fibrosis as demonstrated by reduced collagen accumulation. Collectively, hepatic FGF21 overexpression limits hepatic lipotoxicity, inflammation, and fibrogenesis. Mechanistically, FGF21 blocks hepatic lipid influx and accumulation through combined endocrine and autocrine signaling, respectively, which prevents KC activation and lowers the presence of lipid- and scar-associated macrophages to inhibit fibrogenesis.

Published
2023

2. Pharmacological treatment with FGF21 strongly improves plasma cholesterol metabolism to reduce atherosclerosis.

Author

Liu, Cong, Schönke, Milena, Zhou, Enchen, Li, Zhuang, Kooijman, Sander, Boon, Mariëtte, Larsson, Mikael, Wallenius, Kristina, Dekker, Niek, Barlind, Louise, Peng, Xiao-Rong, Wang, Yanan, and Rensen, Patrick

Subjects
Adipose-liver axis, Atherosclerotic cardiovascular disease, Brown adipose tissue, Dyslipidaemia, Lipoprotein metabolism, Adipose Tissue, Brown, Adipose Tissue, White, Adiposity, Animals, Anticholesteremic Agents, Apolipoprotein E3, Atherosclerosis, Biomarkers, Cholesterol, Disease Models, Animal, Energy Metabolism, Fibroblast Growth Factors, Hypercholesterolemia, Lipid Metabolism, Lipoproteins, VLDL, Liver, Mice, Transgenic, Plaque, Atherosclerotic, Recombinant Proteins, Triglycerides
Abstract

AIMS: Fibroblast growth factor (FGF) 21, a key regulator of energy metabolism, is currently evaluated in humans for treatment of type 2 diabetes and non-alcoholic steatohepatitis. However, the effects of FGF21 on cardiovascular benefit, particularly on lipoprotein metabolism in relation to atherogenesis, remain elusive. METHODS AND RESULTS: Here, the role of FGF21 in lipoprotein metabolism in relation to atherosclerosis development was investigated by pharmacological administration of a half-life extended recombinant FGF21 protein to hypercholesterolaemic APOE*3-Leiden.CETP mice, a well-established model mimicking atherosclerosis initiation and development in humans. FGF21 reduced plasma total cholesterol, explained by a reduction in non-HDL-cholesterol. Mechanistically, FGF21 promoted brown adipose tissue (BAT) activation and white adipose tissue (WAT) browning, thereby enhancing the selective uptake of fatty acids from triglyceride-rich lipoproteins into BAT and into browned WAT, consequently accelerating the clearance of the cholesterol-enriched remnants by the liver. In addition, FGF21 reduced body fat, ameliorated glucose tolerance and markedly reduced hepatic steatosis, related to up-regulated hepatic expression of genes involved in fatty acid oxidation and increased hepatic VLDL-triglyceride secretion. Ultimately, FGF21 largely decreased atherosclerotic lesion area, which was mainly explained by the reduction in non-HDL-cholesterol as shown by linear regression analysis, decreased lesion severity, and increased atherosclerotic plaque stability index. CONCLUSION: FGF21 improves hypercholesterolaemia by accelerating triglyceride-rich lipoprotein turnover as a result of activating BAT and browning of WAT, thereby reducing atherosclerotic lesion severity and increasing atherosclerotic lesion stability index. We have thus provided additional support for the clinical use of FGF21 in the treatment of atherosclerotic cardiovascular disease.

Published
2022

4. Liver-targeted Angptl4 silencing by antisense oligonucleotide treatment attenuates hyperlipidaemia and atherosclerosis development in APOE*3-Leiden.CETP mice.

Author

Modder, Melanie, Panhuis, Wietse In het, Li, Mohan, Afkir, Salwa, Dorn, Alexandra L, Pronk, Amanda C M, Streefland, Trea C M, Lalai, Reshma A, Pierrou, Stefan, Nilsson, Stefan K, Olivecrona, Gunilla, Kooijman, Sander, Rensen, Patrick C N, and Schönke, Milena

Subjects
LOW density lipoproteins, BROWN adipose tissue, BLOOD lipids, LIPOPROTEIN lipase, KRA
Abstract

Aims Angiopoietin-like 3 (ANGPTL3) and 4 (ANGPTL4) inhibit lipoprotein lipase to regulate tissue fatty acid (FA) uptake from triglyceride (TG)-rich lipoproteins such as very low density lipoproteins (VLDL). While pharmacological inhibition of ANGPTL3 is being evaluated as a lipid-lowering strategy, systemic ANGPTL4 inhibition is not pursued due to adverse effects. This study aims to compare the therapeutic potential of liver-specific Angptl3 and Angptl4 silencing to attenuate hyperlipidemia and atherosclerosis development in APOE*3-Leiden.CETP mice, a well-established humanized model for lipoprotein metabolism. Methods and results Mice were subcutaneously injected twice per week with saline or liver-targeted antisense oligonucleotides against Angptl3 , Angptl4 , both, or a scrambled oligonucleotide. Plasma lipid levels, VLDL clearance, and hepatic VLDL production were determined, and atherosclerosis development was assessed. For toxicological evaluation, cynomolgus monkeys were treated with three dosages of liver-targeted ANGPTL4 -silencing oligonucleotides. Liver-targeted Angptl4 silencing reduced plasma TGs (−48%) and total cholesterol (−56%), explained by higher VLDL-derived FA uptake by brown adipose tissue and lower VLDL production by the liver. Accordingly, Angptl4 silencing reduced atherosclerotic lesion size (−86%) and improved lesion stability. Hepatic Angptl3 silencing similarly attenuated hyperlipidemia and atherosclerosis development. While Angptl3 and Angptl4 silencing lowered plasma TGs in the refed and fasted state, respectively, combined Angptl3/4 silencing lowered plasma TGs independent of the nutritional state. In cynomolgus monkeys, anti- ANGPTL4 ASO treatment was well tolerated without adverse effects. Conclusion Liver-targeted Angptl4 silencing potently attenuates hyperlipidemia and atherosclerosis development in APOE*3-Leiden.CETP mice, and liver-targeted ANGPTL4 silencing is well tolerated in non-human primates. These data warrant further clinical development of liver-targeted ANGPTL4 silencing. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

5. Timing Matters: Late, but Not Early, Exercise Training Ameliorates MASLD in Part by Modulating the Gut‐Liver Axis in Mice.

Author

Kovynev, Artemiy, Ying, Zhixiong, Zhang, Sen, Olgiati, Emanuele, Lambooij, Joost M., Visentin, Clara, Guigas, Bruno, Ducarmon, Quinten R., Rensen, Patrick C. N., and Schönke, Milena

Subjects
EXERCISE physiology, HIGH cholesterol diet, FECAL microbiota transplantation, EXERCISE therapy, GUT microbiome
Abstract

Metabolic dysfunction‐associated steatotic liver disease (MASLD) affects two billion people worldwide and is currently mostly treatable via lifestyle interventions, such as exercise training. However, it is unclear whether the positive effects of exercise are restricted to unique circadian windows. We therefore aimed to study whether the timing of exercise training differentially modulates MASLD development. Twenty weeks old male APOE*3‐Leiden.CETP mice were fed a high fat‐high cholesterol diet to induce MASLD and treadmill‐trained for 1 h five times per week for 12 weeks either early (ZT13; E‐RUN) or late (ZT22; L‐RUN) in the dark phase while corresponding sedentary groups (E‐SED and L‐SED) did not. Late, but not early exercise training decreased the MASLD score, body weight, fat mass, and liver triglycerides, accompanied by an altered composition of the gut microbiota. Specifically, only late exercise training increased the abundance of short‐chain fatty acid‐producing bacterial families and genera, such as Akkermansia, Lachnospiraceae, and Rikenella. To assess the role of the gut microbiota in training‐induced effects, the study was repeated and trained (ZT22 only, RUN) or sedentary mice (SED) served as fecal donors for sedentary recipient mice (RUN FMT and SED FMT). Fecal microbiota transplantation reduced liver weight and plasma triglycerides in RUN FMT compared to SED FMT and tended to lower the MASLD score and liver triglycerides. Timing of exercise training is a critical factor for the positive effect on MASLD in this preclinical model, and the effect of late exercise is partially mediated via the gut‐liver axis. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

7. No evidence of brown adipose tissue activation after 24 weeks of supervised exercise training in young sedentary adults in the ACTIBATE randomized controlled trial

Author

Martinez-Tellez, Borja, Sanchez-Delgado, Guillermo, Acosta, Francisco M., Alcantara, Juan M. A., Amaro-Gahete, Francisco J., Martinez-Avila, Wendy D., Merchan-Ramirez, Elisa, Muñoz-Hernandez, Victoria, Osuna-Prieto, Francisco J., Jurado-Fasoli, Lucas, Xu, Huiwen, Ortiz-Alvarez, Lourdes, Arias-Tellez, María J., Mendez-Gutierrez, Andrea, Labayen, Idoia, Ortega, Francisco B., Schönke, Milena, Rensen, Patrick C. N., Aguilera, Concepción M., Llamas-Elvira, José M., Gil, Ángel, and Ruiz, Jonatan R.

Published
2022
Full Text
View/download PDF

8. Time-restricted feeding attenuates hypercholesterolaemia and atherosclerosis development during circadian disturbance in APOE∗3-Leiden.CETP mice

Author

In Het Panhuis, Wietse, primary, Schönke, Milena, additional, Modder, Melanie, additional, Tom, Hannah E., additional, Lalai, Reshma A., additional, Pronk, Amanda C.M., additional, Streefland, Trea C.M., additional, van Kerkhof, Linda W.M., additional, Dollé, Martijn E.T., additional, Depuydt, Marie A.C., additional, Bot, Ilze, additional, Vos, Winnie G., additional, Bosmans, Laura A., additional, van Os, Bram W., additional, Lutgens, Esther, additional, Rensen, Patrick C.N., additional, and Kooijman, Sander, additional

Published
2023
Full Text
View/download PDF

10. Time of day determines postexercise metabolism in mouse adipose tissue

Author

Pendergrast, Logan A., Lundell, Leonidas S., Ehrlich, Amy M., Ashcroft, Stephen P., Schönke, Milena, Basse, Astrid L., Krook, Anna, Treebak, Jonas T., Dollet, Lucile, Zierath, Juleen R., Pendergrast, Logan A., Lundell, Leonidas S., Ehrlich, Amy M., Ashcroft, Stephen P., Schönke, Milena, Basse, Astrid L., Krook, Anna, Treebak, Jonas T., Dollet, Lucile, and Zierath, Juleen R.

Abstract

The circadian clock is a cell-autonomous transcription–translation feedback mechanism that anticipates and adapts physiology and behavior to different phases of the day. A variety of factors including hormones, temperature, food-intake, and exercise can act on tissue-specific peripheral clocks to alter the expression of genes that influence metabolism, all in a time-of-day dependent manner. The aim of this study was to elucidate the effects of exercise timing on adipose tissue metabolism. We performed RNA sequencing on inguinal adipose tissue of mice immediately following maximal exercise or sham treatment at the early rest or early active phase. Only during the early active phase did exercise elicit an immediate increase in serum nonesterified fatty acids. Furthermore, early active phase exercise increased expression of markers of thermogenesis and mitochondrial proliferation in inguinal adipose tissue. In vitro, synchronized 3T3-L1 adipocytes showed a timing-dependent difference in Adrb2 expression, as well as a greater lipolytic activity. Thus, the response of adipose tissue to exercise is time-of-day sensitive and may be partly driven by the circadian clock. To determine the influence of feeding state on the time-of-day response to exercise, we replicated the experiment in 10-h-fasted early rest phase mice to mimic the early active phase metabolic status. A 10-h fast led to a similar lipolytic response as observed after active phase exercise but did not replicate the transcriptomic response, suggesting that the observed changes in gene expression are not driven by feeding status. In conclusion, acute exercise elicits timing-specific effects on adipose tissue to maintain metabolic homeostasis.

Published
2023

13. FGF21 protects against hepatic lipotoxicity and macrophage activation to attenuate fibrogenesis in nonalcoholic steatohepatitis

Author

Liu, Cong, primary, Schönke, Milena, additional, Spoorenberg, Borah, additional, Lambooij, Joost M, additional, van der Zande, Hendrik JP, additional, Zhou, Enchen, additional, Tushuizen, Maarten E, additional, Andreasson, Anne-Christine, additional, Park, Andrew, additional, Oldham, Stephanie, additional, Uhrbom, Martin, additional, Ahlstedt, Ingela, additional, Ikeda, Yasuhiro, additional, Wallenius, Kristina, additional, Peng, Xiao-Rong, additional, Guigas, Bruno, additional, Boon, Mariëtte R, additional, Wang, Yanan, additional, and Rensen, Patrick CN, additional

Published
2023
Full Text
View/download PDF

14. Circadian disruption impairs glucose homeostasis in male but not in female mice and is dependent on gonadal sex hormones

Author

In het Panhuis, Wietse, primary, Schönke, Milena, additional, Siebeler, Ricky, additional, Banen, Dorien, additional, Pronk, Amanda C. M., additional, Streefland, Trea C. M., additional, Afkir, Salwa, additional, Sips, Hetty C. M., additional, Kroon, Jan, additional, Rensen, Patrick C. N., additional, and Kooijman, Sander, additional

Published
2023
Full Text
View/download PDF

15. Author response: FGF21 protects against hepatic lipotoxicity and macrophage activation to attenuate fibrogenesis in nonalcoholic steatohepatitis

Author

Liu, Cong, primary, Schönke, Milena, additional, Spoorenberg, Borah, additional, Lambooij, Joost M, additional, van der Zande, Hendrik JP, additional, Zhou, Enchen, additional, Tushuizen, Maarten E, additional, Andreasson, Anne-Christine, additional, Park, Andrew, additional, Oldham, Stephanie, additional, Uhrbom, Martin, additional, Ahlstedt, Ingela, additional, Ikeda, Yasuhiro, additional, Wallenius, Kristina, additional, Peng, Xiao-Rong, additional, Guigas, Bruno, additional, Boon, Mariëtte R, additional, Wang, Yanan, additional, and Rensen, Patrick CN, additional

Published
2023
Full Text
View/download PDF

16. Time to run: Late rather than early exercise training in mice remodels the gut microbiome and reduces atherosclerosis development

Author

Schönke, Milena, primary, Ying, Zhixiong, additional, Kovynev, Artemiy, additional, In het Panhuis, Wietse, additional, Binnendijk, Anne, additional, van der Poel, Sabine, additional, Pronk, Amanda C. M., additional, Streefland, Trea C. M., additional, Hoekstra, Menno, additional, Kooijman, Sander, additional, and Rensen, Patrick C. N., additional

Published
2022
Full Text
View/download PDF

19. Acute and long-term exercise differently modulate plasma levels of oxylipins, endocannabinoids, and their analogues in young sedentary adults: A sub-study and secondary analyses from the ACTIBATE randomized controlled-trial

Author

Jurado-Fasoli, Lucas, primary, Di, Xinyu, additional, Sanchez-Delgado, Guillermo, additional, Yang, Wei, additional, Osuna-Prieto, Francisco J., additional, Ortiz-Alvarez, Lourdes, additional, Krekels, Elke, additional, Harms, Amy C., additional, Hankemeier, Thomas, additional, Schönke, Milena, additional, Aguilera, Concepcion M., additional, Llamas-Elvira, Jose M., additional, Kohler, Isabelle, additional, Rensen, Patrick C.N., additional, Ruiz, Jonatan R., additional, and Martinez-Tellez, Borja, additional

Published
2022
Full Text
View/download PDF

20. Aging attenuates diurnal lipid uptake by brown adipose tissue

Author

In het Panhuis, Wietse, primary, Schönke, Milena, additional, Siebeler, Ricky, additional, Afkir, Salwa, additional, Baelde, Rianne, additional, Pronk, Amanda C.M., additional, Streefland, Trea C.M., additional, Sips, Hetty C.M., additional, Lalai, Reshma A., additional, Rensen, Patrick C.N., additional, and Kooijman, Sander, additional

Published
2022
Full Text
View/download PDF

21. FGF21 protects against hepatic lipotoxicity and macrophage activation to attenuate fibrogenesis in nonalcoholic steatohepatitis

Author

Liu, Cong, primary, Schönke, Milena, additional, Spoorenberg, Borah, additional, Lambooij, Joost M., additional, van der Zande, Hendrik J.P., additional, Zhou, Enchen, additional, Tushuizen, Maarten E., additional, Andréasson, Anne-Christine, additional, Park, Andrew, additional, Oldham, Stephanie, additional, Uhrbom, Martin, additional, Ahlstedt, Ingela, additional, Ikeda, Yasuhiro, additional, Wallenius, Kristina, additional, Peng, Xiao-Rong, additional, Guigas, Bruno, additional, Boon, Mariëtte R., additional, Wang, Yanan, additional, and Rensen, Patrick C.N., additional

Published
2022
Full Text
View/download PDF

23. Sexual Dimorphism in Transcriptional and Functional Glucocorticoid Effects on Mouse Skeletal Muscle

Author

Li, Sheng, primary, Schönke, Milena, additional, Buurstede, Jacobus C., additional, Moll, Tijmen J.A., additional, Gentenaar, Max, additional, Schilperoort, Maaike, additional, Visser, Jenny A., additional, Kaikaew, Kasiphak, additional, van de Vijver, Davy, additional, Abbassi-Daloii, Tooba, additional, Raz, Vered, additional, Aartsma-Rus, Annemieke, additional, van Putten, Maaike, additional, Meijer, Onno C., additional, and Kroon, Jan, additional

Published
2022
Full Text
View/download PDF

24. Angiopoietin-like 4 governs diurnal lipoprotein lipase activity in brown adipose tissue

Author

van Eenige, Robin, primary, In het Panhuis, Wietse, additional, Schönke, Milena, additional, Jouffe, Céline, additional, Devilee, Thomas H., additional, Siebeler, Ricky, additional, Streefland, Trea C.M., additional, Sips, Hetty C.M., additional, Pronk, Amanda C.M., additional, Vorderman, Ruben H.P., additional, Mei, Hailiang, additional, van Klinken, Jan Bert, additional, van Weeghel, Michel, additional, Uhlenhaut, Nina H., additional, Kersten, Sander, additional, Rensen, Patrick C.N., additional, and Kooijman, Sander, additional

Published
2022
Full Text
View/download PDF

26. Sexual Dimorphism in Transcriptional and Functional Glucocorticoid Effects on Mouse Skeletal Muscle

Author

Li, Sheng, Schönke, Milena, Buurstede, Jacobus C., Moll, Tijmen J.A., Gentenaar, Max, Schilperoort, Maaike, Visser, Jenny A., Kaikaew, Kasiphak, van de Vijver, Davy, Abbassi-Daloii, Tooba, Raz, Vered, Aartsma-Rus, Annemieke, van Putten, Maaike, Meijer, Onno C., Kroon, Jan, Li, Sheng, Schönke, Milena, Buurstede, Jacobus C., Moll, Tijmen J.A., Gentenaar, Max, Schilperoort, Maaike, Visser, Jenny A., Kaikaew, Kasiphak, van de Vijver, Davy, Abbassi-Daloii, Tooba, Raz, Vered, Aartsma-Rus, Annemieke, van Putten, Maaike, Meijer, Onno C., and Kroon, Jan

Abstract

Muscle atrophy is common in patients with increased glucocorticoid exposure. Glucocorticoid effects are often sex-specific, and while different glucocorticoid responses between male and female subjects are reported, it is unclear why this is. In this study, we evaluated the effects of corticosterone and synthetic glucocorticoid treatment on muscle atrophy in male and female mice. We found that corticosterone treatment reduced grip strength in female mice only, whereas muscle mass was reduced in both sexes. Skeletal muscle transcriptional responses to corticosterone treatment were more pronounced and widespread in male mice. Synthetic glucocorticoid treatment reduced grip strength in both sexes, while female mice were more sensitive to muscle atrophy than male mice. To evaluate the role of androgens, chemically-castrated male mice were treated with synthetic glucocorticoids. We observed additively reduced muscle mass, but did not observe any interaction effects. Although sex differences in glucocorticoid responses in skeletal muscle are partly influenced by androgen signaling, further studies are warranted to fully delineate the underlying mechanisms.

Published
2022

27. Atlas of exercise metabolism reveals time-dependent signatures of metabolic homeostasis

Author

Sato, Shogo, Dyar, Kenneth A, Treebak, Jonas T, Jepsen, Sara L, Ehrlich, Amy M, Ashcroft, Stephen P, Trost, Kajetan, Kunzke, Thomas, Prade, Verena M, Small, Lewin, Basse, Astrid Linde, Schönke, Milena, Chen, Siwei, Samad, Muntaha, Baldi, Pierre, Barrès, Romain, Walch, Axel, Moritz, Thomas, Holst, Jens J, Lutter, Dominik, Zierath, Juleen R., Sassone-Corsi, Paolo, Sato, Shogo, Dyar, Kenneth A, Treebak, Jonas T, Jepsen, Sara L, Ehrlich, Amy M, Ashcroft, Stephen P, Trost, Kajetan, Kunzke, Thomas, Prade, Verena M, Small, Lewin, Basse, Astrid Linde, Schönke, Milena, Chen, Siwei, Samad, Muntaha, Baldi, Pierre, Barrès, Romain, Walch, Axel, Moritz, Thomas, Holst, Jens J, Lutter, Dominik, Zierath, Juleen R., and Sassone-Corsi, Paolo

Abstract

Tissue sensitivity and response to exercise vary according to the time of day and alignment of circadian clocks, but the optimal exercise time to elicit a desired metabolic outcome is not fully defined. To understand how tissues independently and collectively respond to timed exercise, we applied a systems biology approach. We mapped and compared global metabolite responses of seven different mouse tissues and serum after an acute exercise bout performed at different times of the day. Comparative analyses of intra- and inter-tissue metabolite dynamics, including temporal profiling and blood sampling across liver and hindlimb muscles, uncovered an unbiased view of local and systemic metabolic responses to exercise unique to time of day. This comprehensive atlas of exercise metabolism provides clarity and physiological context regarding the production and distribution of canonical and novel time-dependent exerkine metabolites, such as 2-hydroxybutyrate (2-HB), and reveals insight into the health-promoting benefits of exercise on metabolism.

Published
2022

29. Rev1 deficiency induces replication stress to cause metabolic dysfunction differently in males and females

Author

In het Panhuis, Wietse, primary, Tsaalbi-Shtylik, Anastasia, additional, Schönke, Milena, additional, van Harmelen, Vanessa, additional, Pronk, Amanda C. M., additional, Streefland, Trea C. M., additional, Sips, Hetty C. M., additional, Afkir, Salwa, additional, Willems van Dijk, Ko, additional, Rensen, Patrick C. N., additional, de Wind, Niels, additional, and Kooijman, Sander, additional

Published
2022
Full Text
View/download PDF

30. Atlas of exercise metabolism reveals time-dependent signatures of metabolic homeostasis

Author

Sato, Shogo, primary, Dyar, Kenneth A., additional, Treebak, Jonas T., additional, Jepsen, Sara L., additional, Ehrlich, Amy M., additional, Ashcroft, Stephen P., additional, Trost, Kajetan, additional, Kunzke, Thomas, additional, Prade, Verena M., additional, Small, Lewin, additional, Basse, Astrid Linde, additional, Schönke, Milena, additional, Chen, Siwei, additional, Samad, Muntaha, additional, Baldi, Pierre, additional, Barrès, Romain, additional, Walch, Axel, additional, Moritz, Thomas, additional, Holst, Jens J., additional, Lutter, Dominik, additional, Zierath, Juleen R., additional, and Sassone-Corsi, Paolo, additional

Published
2022
Full Text
View/download PDF

31. FGF21 protects against hepatic lipotoxicity and macrophage activation to attenuate fibrogenesis in nonalcoholic steatohepatitis.

Author

Cong Liu, Schönke, Milena, Spoorenberg, Borah, Lambooij, Joost M., van der Zande, Hendrik J. P., Enchen Zhou, Tushuizen, Maarten E., Andreasson, Anne-Christine, Park, Andrew, Oldham, Stephanie, Uhrbom, Martin, Ahlstedt, Ingela, Yasuhiro Ikeda, Wallenius, Kristina, Xiao-Rong Peng, Guigas, Bruno, Boon, Mariëtte R., Yanan Wang, and Rensen, Patrick C. N.

Subjects
*MACROPHAGE activation, *NON-alcoholic fatty liver disease, *HYPERTROPHIC scars, *FATTY acid oxidation, *HIGH cholesterol diet, *KUPFFER cells, *FIBROBLAST growth factors
Abstract

Analogues of the hepatokine fibroblast growth factor 21 (FGF21) are in clinical development for type 2 diabetes and nonalcoholic steatohepatitis (NASH) treatment. Although their glucose-lowering and insulin-sensitizing effects have been largely unraveled, the mechanisms by which they alleviate liver injury have only been scarcely addressed. Here, we aimed to unveil the mechanisms underlying the protective effects of FGF21 on NASH using APOE*3-Leiden. CETP mice, a well-established model for human-like metabolic diseases. Liver-specific FGF21 overexpression was achieved in mice, followed by administration of a high-fat high-cholesterol diet for 23 weeks. FGF21 prevented hepatic lipotoxicity, accompanied by activation of thermogenic tissues and attenuation of adipose tissue inflammation, improvement of hyperglycemia and hypertriglyceridemia, and upregulation of hepatic programs involved in fatty acid oxidation and cholesterol removal. Furthermore, FGF21 inhibited hepatic inflammation, as evidenced by reduced Kupffer cell (KC) activation, diminished monocyte infiltration, and lowered accumulation of monocyte-derived macrophages. Moreover, FGF21 decreased lipid- and scar-associated macrophages, which correlated with less hepatic fibrosis as demonstrated by reduced collagen accumulation. Collectively, hepatic FGF21 overexpression limits hepatic lipotoxicity, inflammation, and fibrogenesis. Mechanistically, FGF21 blocks hepatic lipid influx and accumulation through combined endocrine and autocrine signaling, respectively, which prevents KC activation and lowers the presence of lipid- and scar-associated macrophages to inhibit fibrogenesis. [ABSTRACT FROM AUTHOR]

Published
2023
Full Text
View/download PDF

32. Time to run: Late rather than early exercise training in mice remodels the gut microbiome and reduces atherosclerosis development.

Author

Schönke, Milena, Ying, Zhixiong, Kovynev, Artemiy, In het Panhuis, Wietse, Binnendijk, Anne, van der Poel, Sabine, Pronk, Amanda C. M., Streefland, Trea C. M., Hoekstra, Menno, Kooijman, Sander, and Rensen, Patrick C. N.

Abstract

The metabolic and inflammatory processes that are implicated in the development of cardiovascular diseases are under control of the biological clock. While skeletal muscle function exhibits circadian rhythms, it is unclear to what extent the beneficial health effects of exercise are restricted to unique time windows. We aimed to study whether the timing of exercise training differentially modulates the development of atherosclerosis and elucidate underlying mechanisms. We endurance‐trained atherosclerosis‐prone female APOE*3‐Leiden.CETP mice fed a Western‐type diet, a well‐established human‐like model for cardiometabolic diseases, for 1 h five times a week for 4 weeks either in their early or in their late active phase on a treadmill. We monitored metabolic parameters, the development of atherosclerotic lesions in the aortic root and assessed the composition of the gut microbiota. Late, but not early, exercise training reduced fat mass by 19% and the size of early‐stage atherosclerotic lesions by as much as 29% compared to sedentary animals. No correlation between cholesterol exposure and lesion size was evident, as no differences in plasma lipid levels were observed, but circulating levels of the pro‐inflammatory markers ICAM‐1 and VCAM‐1 were reduced with late exercise. Strikingly, we observed a time‐of‐day‐dependent effect of exercise training on the composition of the gut microbiota as only late training increased the abundance of gut bacteria producing short‐chain fatty acids with proposed anti‐inflammatory properties. Together, these findings indicate that timing is a critical factor to the beneficial anti‐atherosclerotic effects of exercise with a great potential to further optimize training recommendations for patients. [ABSTRACT FROM AUTHOR]

Published
2023
Full Text
View/download PDF

33. The ZBED6–IGF2 axis has a major effect on growth of skeletal muscle and internal organs in placental mammals

Author

Younis, Shady, Schönke, Milena, Massart, Julie, Hjortebjerg, Rikke, Sundström, Elisabeth, Gustafson, Ulla, Björnholm, Marie, Krook, Anna, Frystyk, Jan, Zierath, Juleen R., and Andersson, Leif

Subjects
Male, animal structures, endocrine system diseases, Mouse, Cell- och molekylärbiologi, Mice, Transgenic, Mice, Insulin-Like Growth Factor II, Metabolic regulation, parasitic diseases, Journal Article, Genetics, Animals, Muscle, Skeletal, Promoter Regions, Genetic, mouse, Alleles, Conserved Sequence, Mice, Knockout, Repressor Proteins/genetics, Binding Sites, Insulin-Like Growth Factor II/physiology, Sequence Analysis, RNA, ZBED6, IGF2, Biological Sciences, female genital diseases and pregnancy complications, Up-Regulation, Mice, Inbred C57BL, Repressor Proteins, Phenotype, PNAS Plus, DNA Transposable Elements, Muscle growth, CpG Islands, Female, metabolic regulation, muscle growth, Muscle, Skeletal/growth & development, Transcriptome, Cell and Molecular Biology
Abstract

Significance Insulin-like growth factor 2 (IGF2) is an important growth factor with a critical role for fetal growth in mammals. The ZBED6 transcription factor is unique to placental mammals and has evolved from a domesticated DNA transposon. This study shows that ZBED6 and its interaction with the Igf2 locus play a prominent role in regulating postnatal growth of skeletal muscle and internal organs (kidney, liver, and heart) in placental mammals. This prominent role in mammalian biology provides a reasonable explanation why ZBED6 is highly conserved among all families of placental mammals and why 16 base pairs encompassing the ZBED6 binding site in an intron of Igf2 are conserved among the great majority of, if not all, placental mammals., A single nucleotide substitution in the third intron of insulin-like growth factor 2 (IGF2) is associated with increased muscle mass and reduced subcutaneous fat in domestic pigs. This mutation disrupts the binding of the ZBED6 transcription factor and leads to a threefold up-regulation of IGF2 expression in pig skeletal muscle. Here, we investigated the biological significance of ZBED6–IGF2 interaction in the growth of placental mammals using two mouse models, ZBED6 knock-out (Zbed6−/−) and Igf2 knock-in mice that carry the pig IGF2 mutation. These transgenic mice exhibit markedly higher serum IGF2 concentrations, higher growth rate, increased lean mass, and larger heart, kidney, and liver; no significant changes were observed for white adipose tissues. The changes in body and lean mass were most pronounced in female mice. The phenotypic changes were concomitant with a remarkable up-regulation of Igf2 expression in adult tissues. Transcriptome analysis of skeletal muscle identified differential expression of genes belonging to the extracellular region category. Expression analysis using fetal muscles indicated a minor role of ZBED6 in regulating Igf2 expression prenatally. Furthermore, transcriptome analysis of the adult skeletal muscle revealed that this elevated expression of Igf2 was derived from the P1 and P2 promoters. The results revealed very similar phenotypic effects in the Zbed6 knock-out mouse and in the Igf2 knock-in mouse, showing that the effect of ZBED6 on growth of muscle and internal organs is mediated through the binding site in the Igf2 gene. The results explain why this ZBED6 binding site is extremely well conserved among placental mammals.

Published
2018
Full Text
View/download PDF

34. Pharmacological treatment with FGF21 strongly improves plasma cholesterol metabolism to reduce atherosclerosis

Author

Liu, Cong, primary, Schönke, Milena, additional, Zhou, Enchen, additional, Li, Zhuang, additional, Kooijman, Sander, additional, Boon, Mariëtte R, additional, Larsson, Mikael, additional, Wallenius, Kristina, additional, Dekker, Niek, additional, Barlind, Louise, additional, Peng, Xiao-Rong, additional, Wang, Yanan, additional, and Rensen, Patrick C N, additional

Published
2021
Full Text
View/download PDF

35. Sexual Dimorphism in Transcriptional and Functional Glucocorticoid Effects on Mouse Skeletal Muscle.

Author

Sheng Li, Schönke, Milena, Buurstede, Jacobus C., Moll, Tijmen J. A., Gentenaar, Max, Schilperoort, Maaike, Visser, Jenny A., Kaikaew, Kasiphak, van de Vijver, Davy, Abbassi-Daloii, Tooba, Raz, Vered, Aartsma-Rus, Annemieke, van Putten, Maaike, Meijer, Onno C., and Kroon, Jan

Subjects
SEXUAL dimorphism, SKELETAL muscle, GLUCOCORTICOIDS, MUSCULAR atrophy, MUSCLE mass
Abstract

Muscle atrophy is common in patients with increased glucocorticoid exposure. Glucocorticoid effects are often sex-specific, and while different glucocorticoid responses between male and female subjects are reported, it is unclear why this is. In this study, we evaluated the effects of corticosterone and synthetic glucocorticoid treatment on muscle atrophy in male and female mice. We found that corticosterone treatment reduced grip strength in female mice only, whereas muscle mass was reduced in both sexes. Skeletal muscle transcriptional responses to corticosterone treatment were more pronounced and widespread in male mice. Synthetic glucocorticoid treatment reduced grip strength in both sexes, while femalemiceweremore sensitive tomuscle atrophy thanmalemice. To evaluate the role of androgens, chemically-castrated male mice were treated with synthetic glucocorticoids. We observed additively reduced muscle mass, but did not observe any interaction effects. Although sex differences in glucocorticoid responses in skeletal muscle are partly influenced by androgen signaling, further studies are warranted to fully delineate the underlying mechanisms. [ABSTRACT FROM AUTHOR]

Published
2022
Full Text
View/download PDF

38. Rev1 deficiency induces replication stress to cause metabolic dysfunction differently in males and females.

Author

Panhuis, Wietse In het, Tsaalbi-Shtylik, Anastasia, Schönke, Milena, van Harmelen, Vanessa, Pronk, Amanda C. M., Streefland, Trea C. M., Sips, Hetty C. M., Afkir, Salwa, van Dijk, Ko Willems, Rensen, Patrick C. N., de Wind, Niels, and Kooijman, Sander

Subjects
NAD (Coenzyme), DNA polymerases, METABOLIC disorders, GLUCOSE-6-phosphate dehydrogenase, ADIPOSE tissues, WEIGHT gain, DNA replication, BLOOD lactate
Abstract

DNA damage responses compete for cellular resources with metabolic pathways, but little is known about the metabolic consequences of impaired DNA replication, a process called replication stress. Here we characterized the metabolic consequences of DNA replication stress at endogenous DNA lesions by using mice with a disruption of Rev1, a translesion DNA polymerase specialized in the mutagenic replication of damaged DNA. Male and female Rev1 knockout (KO) mice were compared with wild-type (WT) mice and followed over time to study the natural course of body weight gain and glucose tolerance. Follow-up measurements were performed in female mice for in-depth metabolic characterization. Body weight and fat mass were only increased in female KO mice versus WT mice, whereas glucose intolerance and a reduction in lean mass were observed in both sexes. Female KO mice showed reduced locomotor activity while male KO mice showed increased activity as compared with their WT littermates. Further characterization of female mice revealed that lipid handling was unaffected by Rev1 deletion. An increased respiratory exchange ratio, combined with elevated plasma lactate levels and increased hepatic gluconeogenesis indicated problems with aerobic oxidation and increased reliance on anaerobic glycolysis. Supplementation with the NAD+ precursor nicotinamide riboside to stimulate aerobic respiration failed to restore the metabolic phenotype. In conclusion, replication stress at endogenous DNA lesions induces a complex metabolic phenotype, most likely initiated by muscular metabolic dysfunction and increased dependence on anaerobic glycolysis. Nicotinamide riboside supplementation after the onset of the metabolic impairment did not rescue this phenotype. [ABSTRACT FROM AUTHOR]

Published
2022
Full Text
View/download PDF

40. Time of Exercise Specifies the Impact on Muscle Metabolic Pathways and Systemic Energy Homeostasis

Author

Sato, Shogo, primary, Basse, Astrid Linde, additional, Schönke, Milena, additional, Chen, Siwei, additional, Samad, Muntaha, additional, Altıntaş, Ali, additional, Laker, Rhianna C., additional, Dalbram, Emilie, additional, Barrès, Romain, additional, Baldi, Pierre, additional, Treebak, Jonas T., additional, Zierath, Juleen R., additional, and Sassone-Corsi, Paolo, additional

Published
2019
Full Text
View/download PDF

41. Modified UCN2 Peptide Acts as an Insulin Sensitizer in Skeletal Muscle of Obese Mice

Author

Borg, Melissa L., primary, Massart, Julie, additional, Schönke, Milena, additional, De Castro Barbosa, Thais, additional, Guo, Lili, additional, Wade, Mark, additional, Alsina-Fernandez, Jorge, additional, Miles, Rebecca, additional, Ryan, Andrew, additional, Bauer, Steve, additional, Coskun, Tamer, additional, O’Farrell, Elizabeth, additional, Niemeier, Evan M., additional, Chibalin, Alexander V., additional, Krook, Anna, additional, Karlsson, Håkan K., additional, Brozinick, Joseph T., additional, and Zierath, Juleen R., additional

Published
2019
Full Text
View/download PDF

42. Acute sleep loss results in tissue-specific alterations in genome-wide DNA methylation state and metabolic fuel utilization in humans

Author

Cedernaes, Jonathan, primary, Schönke, Milena, additional, Westholm, Jakub Orzechowski, additional, Mi, Jia, additional, Chibalin, Alexander, additional, Voisin, Sarah, additional, Osler, Megan, additional, Vogel, Heike, additional, Hörnaeus, Katarina, additional, Dickson, Suzanne L., additional, Lind, Sara Bergström, additional, Bergquist, Jonas, additional, Schiöth, Helgi B, additional, Zierath, Juleen R., additional, and Benedict, Christian, additional

Published
2018
Full Text
View/download PDF

44. Proteomics Analysis of Skeletal Muscle from Leptin-Deficient ob/ob Mice Reveals Adaptive Remodeling of Metabolic Characteristics and Fiber Type Composition

Author

Schönke, Milena, Björnholm, Marie, Chibalin, Alexander V., Zierath, Juleen R., Deshmukh, Atul S., Schönke, Milena, Björnholm, Marie, Chibalin, Alexander V., Zierath, Juleen R., and Deshmukh, Atul S.

Abstract

Skeletal muscle insulin resistance, an early metabolic defect in the pathogenesis of type 2 diabetes (T2D), may be a cause or consequence of altered protein expression profiles. Proteomics technology offers enormous promise to investigate molecular mechanisms underlying pathologies, however, the analysis of skeletal muscle is challenging. Using state-of-the-art multienzyme digestion and filter-aided sample preparation (MED-FASP) and a mass spectrometry (MS)-based workflow, we performed a global proteomics analysis of skeletal muscle from leptin-deficient, obese, insulin resistant (ob/ob) and lean mice in mere two fractions in a short time (8 h per sample). We identified more than 6000 proteins with 118 proteins differentially regulated in obesity. This included protein kinases, phosphatases, and secreted and fiber type associated proteins. Enzymes involved in lipid metabolism in skeletal muscle from ob/ob mice were increased, providing evidence against reduced fatty acid oxidation in lipid-induced insulin resistance. Mitochondrial and peroxisomal proteins, as well as components of pyruvate and lactate metabolism, were increased. Finally, the skeletal muscle proteome from ob/ob mice displayed a shift toward the "slow fiber type." This detailed characterization of an obese rodent model of T2D demonstrates an efficient workflow for skeletal muscle proteomics, which may easily be adapted to other complex tissues.

Published
2018

48. Altered DNA methylation of glycolytic and lipogenic genes in liver from obese and type 2 diabetic patients

Author

Kirchner, Henriette, Sinha, Indranil, Gao, Hui, Ruby, Maxwell A, Schönke, Milena, Lindvall, Jessica M, Barrès, Romain, Krook, Anna, Näslund, Erik, Dahlman-Wright, Karin, Zierath, Juleen R, Kirchner, Henriette, Sinha, Indranil, Gao, Hui, Ruby, Maxwell A, Schönke, Milena, Lindvall, Jessica M, Barrès, Romain, Krook, Anna, Näslund, Erik, Dahlman-Wright, Karin, and Zierath, Juleen R

Abstract

OBJECTIVE: Epigenetic modifications contribute to the etiology of type 2 diabetes.METHOD: We performed genome-wide methylome and transcriptome analysis in liver from severely obese men with or without type 2 diabetes and non-obese men to discover aberrant pathways underlying the development of insulin resistance. Results were validated by pyrosequencing.RESULT: We identified hypomethylation of genes involved in hepatic glycolysis and insulin resistance, concomitant with increased mRNA expression and protein levels. Pyrosequencing revealed the CpG-site within ATF-motifs was hypomethylated in four of these genes in liver of severely obese non-diabetic and type 2 diabetic patients, suggesting epigenetic regulation of transcription by altered ATF-DNA binding.CONCLUSION: Severely obese non-diabetic and type 2 diabetic patients have distinct alterations in the hepatic methylome and transcriptome, with hypomethylation of several genes controlling glucose metabolism within the ATF-motif regulatory site. Obesity appears to shift the epigenetic program of the liver towards increased glycolysis and lipogenesis, which may exacerbate the development of insulin resistance.

Published
2016

Catalog

Books, media, physical & digital resources
See catalog results