Your search keyword '"Solberg, Rigmor"' showing total 4 results

1. The Cysteine Protease Legumain Is Upregulated by Vitamin D and Is a Regulator of Vitamin D Metabolism in Mice.

Author

Forbord, Karl Martin, Okla, Meshail, Lunde, Ngoc Nguyen, Bosnjak-Olsen, Tatjana, Arnekleiv, Guro, Hesselson, Daniel, Johansen, Harald Thidemann, Tang, Jonathan C. Y., Kassem, Moustapha, Solberg, Rigmor, and Jafari, Abbas

Subjects

VITAMIN D metabolism, VITAMIN D receptors, VITAMIN D, MESENCHYMAL stem cells, CYSTEINE, MICE

Abstract

Legumain is a lysosomal cysteine protease that has been implicated in an increasing amount of physiological and pathophysiological processes. However, the upstream mechanisms regulating the expression and function of legumain are not well understood. Here, we provide in vitro and in vivo data showing that vitamin D3 (VD3) enhances legumain expression and function. In turn, legumain alters VD3 bioavailability, possibly through proteolytic cleavage of vitamin D binding protein (VDBP). Active VD3 (1,25(OH)2D3) increased legumain expression, activity, and secretion in osteogenic cultures of human bone marrow stromal cells. Upregulation of legumain was also observed in vivo, evidenced by increased legumain mRNA in the liver and spleen, as well as increased legumain activity in kidneys from wild-type mice treated with 25(OH)D3 (50 µg/kg, subcutaneously) for 8 days compared to a control. In addition, the serum level of legumain was also increased. We further showed that active legumain cleaved purified VDBP (55 kDa) in vitro, forming a 45 kDa fragment. In vivo, no VDBP cleavage was found in kidneys or liver from legumain-deficient mice (Lgmn−/−), whereas VDBP was cleaved in wild-type control mice (Lgmn+/+). Finally, legumain deficiency resulted in increased plasma levels of 25(OH)D3 and total VD3 and altered expression of key renal enzymes involved in VD3 metabolism (CYP24A1 and CYP27B1). In conclusion, a regulatory interplay between VD3 and legumain is suggested. [ABSTRACT FROM AUTHOR]

Published

2024

2. Interplay between Cultured Human Osteoblastic and Skeletal Muscle Cells: Effects of Conditioned Media on Glucose and Fatty Acid Metabolism.

Author

Lunde, Ngoc Nguyen, Osoble, Nimo Mukhtar Mohamud, Fernandez, Andrea Dalmao, Antobreh, Alfreda S., Jafari, Abbas, Singh, Sachin, Nyman, Tuula A., Rustan, Arild C., Solberg, Rigmor, and Thoresen, G. Hege

Subjects

GLUCOSE transporters, SKELETAL muscle, MUSCLE cells, FATTY acids, MESENCHYMAL stem cells, FATTY acid oxidation

Abstract

The interplay between skeletal muscle and bone is primarily mechanical; however, biochemical crosstalk by secreted mediators has recently gained increased attention. The aim of this study was to investigate metabolic effects of conditioned medium from osteoblasts (OB-CM) on myotubes and vice versa. Human skeletal muscle cells incubated with OB-CM showed increased glucose uptake and oxidation, and mRNA expression of the glucose transporter (GLUT) 1, while fatty acid uptake and oxidation, and mRNA expression of the fatty acid transporter CD36 were decreased. This was supported by proteomic analysis, where expression of proteins involved in glucose uptake, glycolytic pathways, and the TCA cycle were enhanced, and expression of several proteins involved in fatty acid metabolism were reduced. Similar effects on energy metabolism were observed in human bone marrow stromal cells differentiated to osteoblastic cells incubated with conditioned medium from myotubes (SKM-CM), with increased glucose uptake and reduced oleic acid uptake. Proteomic analyses of the two conditioned media revealed many common proteins. Thus, our data may indicate a shift in fuel preference from fatty acid to glucose metabolism in both cell types, induced by conditioned media from the opposite cell type, possibly indicating a more general pattern in communication between these tissues. [ABSTRACT FROM AUTHOR]

Published

2023

3. The Mammalian Cysteine Protease Legumain in Health and Disease.

Author

Solberg, Rigmor, Lunde, Ngoc Nguyen, Forbord, Karl Martin, Okla, Meshail, Kassem, Moustapha, and Jafari, Abbas

Subjects

*CYSTEINE, *BONE remodeling, *CEREBROVASCULAR disease, *TISSUES, *NEURODEGENERATION, *UBIQUITIN ligases

Abstract

The cysteine protease legumain (also known as asparaginyl endopeptidase or δ-secretase) is the only known mammalian asparaginyl endopeptidase and is primarily localized to the endolysosomal system, although it is also found extracellularly as a secreted protein. Legumain is involved in the regulation of diverse biological processes and tissue homeostasis, and in the pathogenesis of various malignant and nonmalignant diseases. In addition to its proteolytic activity that leads to the degradation or activation of different substrates, legumain has also been shown to have a nonproteolytic ligase function. This review summarizes the current knowledge about legumain functions in health and disease, including kidney homeostasis, hematopoietic homeostasis, bone remodeling, cardiovascular and cerebrovascular diseases, fibrosis, aging and senescence, neurodegenerative diseases and cancer. In addition, this review addresses the effects of some marketed drugs on legumain. Expanding our knowledge on legumain will delineate the importance of this enzyme in regulating physiological processes and disease conditions. [ABSTRACT FROM AUTHOR]

Published

2022

4. The Cysteine Protease Legumain Is Upregulated by Vitamin D and Is a Regulator of Vitamin D Metabolism in Mice.

Author

Forbord KM, Okla M, Lunde NN, Bosnjak-Olsen T, Arnekleiv G, Hesselson D, Johansen HT, Tang JCY, Kassem M, Solberg R, and Jafari A

Subjects

Humans, Animals, Mice, Vitamins, Cysteine Endopeptidases, Vitamin D pharmacology, Cysteine Proteases

Abstract

Legumain is a lysosomal cysteine protease that has been implicated in an increasing amount of physiological and pathophysiological processes. However, the upstream mechanisms regulating the expression and function of legumain are not well understood. Here, we provide in vitro and in vivo data showing that vitamin D 3 (VD 3 ) enhances legumain expression and function. In turn, legumain alters VD 3 bioavailability, possibly through proteolytic cleavage of vitamin D binding protein (VDBP). Active VD 3 (1,25(OH) 2 D 3 ) increased legumain expression, activity, and secretion in osteogenic cultures of human bone marrow stromal cells. Upregulation of legumain was also observed in vivo, evidenced by increased legumain mRNA in the liver and spleen, as well as increased legumain activity in kidneys from wild-type mice treated with 25(OH)D 3 (50 µg/kg, subcutaneously) for 8 days compared to a control. In addition, the serum level of legumain was also increased. We further showed that active legumain cleaved purified VDBP (55 kDa) in vitro, forming a 45 kDa fragment. In vivo, no VDBP cleavage was found in kidneys or liver from legumain-deficient mice ( Lgmn -/- ), whereas VDBP was cleaved in wild-type control mice ( Lgmn +/+ ). Finally, legumain deficiency resulted in increased plasma levels of 25(OH)D 3 and total VD 3 and altered expression of key renal enzymes involved in VD 3 metabolism (CYP24A1 and CYP27B1). In conclusion, a regulatory interplay between VD 3 and legumain is suggested., Competing Interests: The authors declare no conflicts of interest.

Published

2023