Your search keyword '"Elisabeth Schwob"' showing total 4 results

1. MicroRNA miR-29b regulates diabetic aortic remodeling and stiffening

Author

Isabel N. Schellinger, Markus Wagenhäuser, Giriprakash Chodisetti, Karin Mattern, Angelika Dannert, Anne Petzold, Joanna Jakubizka-Smorag, Fabian Emrich, Josephina Haunschild, Andreas Schuster, Elisabeth Schwob, Kei Schulz, Lars Maegdefessel, Joshua M. Spin, Michael Stumvoll, Gerd Hasenfuß, Philip S. Tsao, and Uwe Raaz

Subjects

diabetes mellitus, arterial stiffness, microRNA, non-coding RNA, extracellular matrix, collagen, Therapeutics. Pharmacology, RM1-950

Abstract

Patients with type 2 diabetes (T2D) are threatened by excessive cardiovascular morbidity and mortality. While accelerated arterial stiffening may represent a critical mechanistic factor driving cardiovascular risk in T2D, specific therapies to contain the underlying diabetic arterial remodeling have been elusive. The present translational study investigates the role of microRNA-29b (miR-29b) as a driver and therapeutic target of diabetic aortic remodeling and stiffening. Using a murine model (db/db mice), as well as human aortic tissue samples, we find that diabetic aortic remodeling and stiffening is associated with medial fibrosis, as well as fragmentation of aortic elastic layers. miR-29b is significantly downregulated in T2D and miR-29b repression is sufficient to induce both aortic medial fibrosis and elastin breakdown through upregulation of its direct target genes COL1A1 and MMP2 thereby increasing aortic stiffness. Moreover, antioxidant treatment restores aortic miR-29b levels and counteracts diabetic aortic remodeling. Concluding, we identify miR-29b as a comprehensive—and therefore powerful—regulator of aortic remodeling and stiffening in T2D that moreover qualifies as a (redox-sensitive) target for therapeutic intervention.

Published

2021

2. MicroRNA miR-29b regulates diabetic aortic remodeling and stiffening

Author

Andreas Schuster, Josephina Haunschild, Karin Mattern, Lars Maegdefessel, Philip S. Tsao, Anne Petzold, Isabel N. Schellinger, Uwe Raaz, Fabian Emrich, Elisabeth Schwob, Angelika Dannert, Giriprakash Chodisetti, Joshua M. Spin, Markus U. Wagenhäuser, Kei Schulz, Michael Stumvoll, Gerd Hasenfuß, and Joanna Jakubizka-Smorag

Subjects

0301 basic medicine, collagen, medicine.medical_specialty, MMP2, extracellular matrix, non-coding RNA, elastin, RM1-950, Type 2 diabetes, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Fibrosis, Internal medicine, Diabetes mellitus, Drug Discovery, medicine, biology, microRNA, business.industry, medicine.disease, 3. Good health, 030104 developmental biology, arterial stiffness, 030220 oncology & carcinogenesis, diabetes mellitus, biology.protein, Arterial stiffness, Cardiology, cardiovascular system, Molecular Medicine, Aortic stiffness, Original Article, Therapeutics. Pharmacology, business, Elastin

Abstract

Patients with type 2 diabetes (T2D) are threatened by excessive cardiovascular morbidity and mortality. While accelerated arterial stiffening may represent a critical mechanistic factor driving cardiovascular risk in T2D, specific therapies to contain the underlying diabetic arterial remodeling have been elusive. The present translational study investigates the role of microRNA-29b (miR-29b) as a driver and therapeutic target of diabetic aortic remodeling and stiffening. Using a murine model (db/db mice), as well as human aortic tissue samples, we find that diabetic aortic remodeling and stiffening is associated with medial fibrosis, as well as fragmentation of aortic elastic layers. miR-29b is significantly downregulated in T2D and miR-29b repression is sufficient to induce both aortic medial fibrosis and elastin breakdown through upregulation of its direct target genes COL1A1 and MMP2 thereby increasing aortic stiffness. Moreover, antioxidant treatment restores aortic miR-29b levels and counteracts diabetic aortic remodeling. Concluding, we identify miR-29b as a comprehensive—and therefore powerful—regulator of aortic remodeling and stiffening in T2D that moreover qualifies as a (redox-sensitive) target for therapeutic intervention., Graphical Abstract, Stiffening of large arteries represents a significant complication in patients with diabetes mellitus resulting in high blood pressure levels and widespread organ damage (in particular in heart, brain, and kidneys). In this study we identify microRNA-29b as a comprehensive regulator and potential therapeutical target of diabetic arterial remodeling and stiffening.

Published

2021

3. Transporters involved in renal excretion of N-carbamoylglutamate, an orphan drug to treat inborn n-acetylglutamate synthase deficiency

Author

Birgitta C. Burckhardt, Gerhard Burckhardt, Yohannes Hagos, and Elisabeth Schwob

Subjects

medicine.medical_specialty, Physiology, Amino-Acid N-Acetyltransferase, Organic Anion Transporters, Sodium-Dependent, Transfection, Cofactor, Membrane Potentials, Kidney Tubules, Proximal, Xenopus laevis, 03 medical and health sciences, Organic Anion Transport Protein 1, 0302 clinical medicine, Glutamates, Internal medicine, medicine, Animals, Humans, N-Acetylglutamate synthase deficiency, Urea Cycle Disorders, Inborn, 030304 developmental biology, Dicarboxylic Acid Transporters, 0303 health sciences, Symporters, biology, ATP synthase, urogenital system, Hyperammonemia, Transporter, medicine.disease, 3. Good health, Renal Elimination, HEK293 Cells, Endocrinology, Urea cycle, Renal physiology, Organic anion transport, biology.protein, 030217 neurology & neurosurgery

Abstract

Inborn defects in N-acetylglutamate (NAG) synthase (NAGS) cause a reduction of NAG, an essential cofactor for the initiation of the urea cycle. As a consequence, blood ammonium concentrations are elevated, leading to severe neurological disorders. The orphan drug N-carbamoylglutamate (NCG; Carbaglu), efficiently overcomes NAGS deficiency. However, not much is known about the transporters involved in the uptake, distribution, and elimination of the divalent organic anion NCG. Organic anion-transporting polypeptides (OATPs) as well as organic anion transporters (OATs) working in cooperation with sodium dicarboxylate cotransporter 3 (NaDC3) accept a wide variety of structurally unrelated drugs. To test for possible interactions with OATPs and OATs, the impact of NCG on these transporters in stably transfected human embryonic kidney-293 cells was measured. The two-electrode voltage-clamp technique was used to monitor NCG-mediated currents in Xenopus laevis oocytes that expressed NaDC3. Neither OATPs nor OAT2 and OAT3 interacted with NCG, but OAT1 transported NCG. In addition, NCG was identified as a high-affinity substrate of NaDC3. Preincubation of OAT4-transfected human embryonic kidney-293 cells with NCG showed an increased uptake of estrone sulfate, the reference substrate of OAT4, indicating efflux of NCG by OAT4. In summary, NaDC3 and, to a lesser extent, OAT1 are likely to be responsible for the uptake of NCG from the blood. Efflux of NCG across the luminal membrane into the tubular lumen probably occurs by OAT4 completing renal secretion of this drug.

Published

2014

4. The orphan drug carbaglu is a substrate of the sodium dicarboxylate transporter 3 (896.8)

Author

Birgitta C. Burckhardt, Yohannes Hagos, Elisabeth Schwob, and Gerhard Burckhardt

Subjects

chemistry, Sodium, Genetics, chemistry.chemical_element, Substrate (chemistry), Molecular Biology, Biochemistry, Combinatorial chemistry, Dicarboxylate Transporter, Biotechnology

Published

2014