Your search keyword '"Susanne V. Fleig"' showing total 8 results

1. Long‐term B cell depletion associates with regeneration of kidney function

Author

Susanne V. Fleig, Franz F. Konen, Christoph Schröder, Jessica Schmitz, Stefan Gingele, Jan H. Bräsen, Svjetlana Lovric, Bernhard M. W. Schmidt, Hermann Haller, Thomas Skripuletz, and Sibylle vonVietinghoff

Subjects

cancer, cell migration, liver/hepatocytes, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract Background Chronic kidney disease (CKD) is a common condition that increases mortality and the risk of cardiovascular and other morbidities regardless of underlying renal condition. Chronic inflammation promotes renal fibrosis. Recently, renal B cell infiltrates were described in chronic kidney disease of various etiologies beyond autoimmunity. Methods We here investigated B cells and indicators of tertiary lymphoid structure formation in human renal biopsies. Renal function was studied during long‐term B cell depletion in human patients with membranous nephropathy and with CKD of unknown origin. Results Cytokine profiles of tertiary lymphoid structure formation were detected in human renal interstitium in a range of kidney diseases. Complex B cell structures consistent with tertiary lymphoid organ formation were evident in human membranous nephropathy. Here, B cell density did not significantly associate with proteinuria severity, but with worse excretory renal function. Proteinuria responses mostly occurred within the first 6 months of B cell depletion. In contrast, recovery of excretory kidney function was observed only after 18 months of continuous therapy, consistent with a structural process. Renal tertiary lymphatic structures were also detected in the absence of autoimmune kidney disease. To start to address whether B cell depletion may affect CKD in a broader population, we assessed kidney function in neurologic patients with CKD of unknown origin. In this cohort, eGFR significantly increased within 24 months of B cell depletion. Conclusion Long‐term B cell depletion associated with significant improvement of excretory kidney function in human CKD. Kinetics and mechanisms of renal B cell aggregation should be investigated further to stratify the impact of B cells and their aggregates as therapeutic targets.

Published

2021

2. Myeloid CCR2 Promotes Atherosclerosis after AKI

Author

Anne M. Hüsing, Vera C. Wulfmeyer, Svenja Gaedcke, Susanne V. Fleig, Song Rong, David DeLuca, Hermann Haller, Roland Schmitt, and Sibylle von Vietinghoff

Subjects

Nephrology, General Medicine

Abstract

The risk of cardiovascular events rises after AKI. Leukocytes promote atherosclerotic plaque growth and instability. We established a model of enhanced remote atherosclerosis after renal ischemia-reperfusion (IR) injury and investigated the underlying inflammatory mechanisms.Atherosclerotic lesions and inflammation were investigated in native and bone marrow-transplanted LDL receptor-deficient (Aortic root atherosclerotic lesions were significantly larger after renal IR injury than in controls. A gene expression screen revealed enrichment for chemokines and their cognate receptors in aortas of IR-injured mice in early atherosclerosis, and of T cell-associated genes in advanced disease. Confocal microscopy revealed increased aortic macrophage proximity to T cells. Differential aortic inflammatory gene regulation in IR-injured mice largely paralleled the pattern in the injured kidney. Single-cell analysis identified renal cell types that produced soluble mediators upregulated in the atherosclerotic aorta. The analysis revealed a marked early increase inOur data introduce an experimental model of remote proatherogenic effects of renal IR and delineate myeloid CCR2 signaling as a mechanistic requirement. Monocytes should be considered as mobile mediators when addressing systemic vascular sequelae of kidney injury.

Published

2022

3. Perivascular Gli1+ Progenitors Are Key Contributors to Injury-Induced Organ Fibrosis

Author

Benjamin D. Humphreys, Flavia Gomes Machado, Benjamin L. Ebert, Susanne V. Fleig, Rebekka K. Schneider, Joel M. Henderson, Rafael Kramann, Derek P. DiRocco, and Philip A. Bondzie

Subjects

Pathology, Cellular differentiation, Mice, 0302 clinical medicine, Fibrosis, Homeostasis, Diphtheria Toxin, Stem Cell Niche, Myofibroblasts, Aorta, Cells, Cultured, 0303 health sciences, education.field_of_study, Cell Differentiation, Organ Specificity, 030220 oncology & carcinogenesis, Molecular Medicine, Proteoglycans, medicine.medical_specialty, Heart Injury, Heart Ventricles, Population, Kruppel-Like Transcription Factors, Neovascularization, Physiologic, Bone Marrow Cells, Biology, Zinc Finger Protein GLI1, Colony-Forming Units Assay, Receptor, Platelet-Derived Growth Factor beta, 03 medical and health sciences, medicine, Genetics, Animals, Humans, Cell Lineage, Antigens, Progenitor cell, education, 030304 developmental biology, Mesenchymal stem cell, Endothelial Cells, Mesenchymal Stem Cells, Cell Biology, medicine.disease, Immunology, Blood Vessels, Solid organ, Pericytes

Abstract

Mesenchymal stem cells (MSCs) reside in the perivascular niche of many organs, including kidney, lung, liver, and heart, although their roles in these tissues are poorly understood. Here, we demonstrate that Gli1 marks perivascular MSC-like cells that substantially contribute to organ fibrosis. In vitro, Gli1(+) cells express typical MSC markers, exhibit trilineage differentiation capacity, and possess colony-forming activity, despite constituting a small fraction of the platelet-derived growth factor-β (PDGFRβ)(+) cell population. Genetic lineage tracing analysis demonstrates that tissue-resident, but not circulating, Gli1(+) cells proliferate after kidney, lung, liver, or heart injury to generate myofibroblasts. Genetic ablation of these cells substantially ameliorates kidney and heart fibrosis and preserves ejection fraction in a model of induced heart failure. These findings implicate perivascular Gli1(+) MSC-like cells as a major cellular origin of organ fibrosis and demonstrate that these cells may be a relevant therapeutic target to prevent solid organ dysfunction after injury.

Published

2015

4. Contents Vol. 127, 2014

Author

Dianne B. McKay, Benjamin D. Humphreys, Sanjeev Noel, Michael Heung, Paul W. Sanders, Joseph C. Gigliotti, Maria N. Martina-Lingua, Sashi G. Kasimsetty, Lakhmir S. Chawla, Kathleen D. Liu, S. Noel, Antoine G. Schneider, Can Ince, Zheng Dong, Peter A. McCullough, Timothy Ball, Raghavan Murugan, Hamid Rabb, Zoltan H. Endre, Etienne Macedo, Isaah S. Vincent, Liyu He, Stuart L. Goldstein, Didier Portilla, Rosalinde Masereeuw, Emaad M. Abdel-Rahman, Peter Pickkers, Daniel A. Peterson, A.R.A. Hamad, Nattachai Srisawat, Monica Zanella, Andrew D. Shaw, Hyun-Joon Shin, Kelly K. Andringa, Satz Mengensatzproduktion, Francesco Garzotto, Susanne V. Fleig, Samatha Bandapalle, Anupam Agarwal, Prasad Devarajan, Aashish Sharma, Esther Peters, Jennifer L. Pluznick, Sean M. Bagshaw, Volker Vallon, Mark D. Okusa, Claudio Ronco, Druckerei Stückle, Richard A. Zager, Man J. Livingston, Sean E. DeWolf, Ravindra L. Mehta, H. Rabb, John A. Kellum, Abdel Rahim A. Hamad, Mélanie Godin, Alana A. Shigeoka, Joseph V. Bonventre, Aneley Hundae, Marìa Jimena Mucino, Patrick T. Murray, Samir M. Parikh, Prabhleen Singh, Noureddin Nourbakhsh, S. Bandapalle, Mei Tran, Frederic T. Billings, M.N. Martina, and Ali C.M. Johnson

Subjects

Nephrology, business.industry, Physiology, Medicine, General Medicine, business

Published

2014

5. Translational Profiles of Medullary Myofibroblasts during Kidney Fibrosis

Author

Andreas Hofmeister, Jing Liu, Andrew P. McMahon, Ivica Grgic, Benjamin D. Humphreys, Jeremy S. Duffield, A. Michaela Krautzberger, Derek P. DiRocco, Susanne V. Fleig, Matthew A. Lalli, and Bruce J. Aronow

Subjects

Ribosomal Proteins, Ribosomal Protein L10, Recombinant Fusion Proteins, Transgene, Green Fluorescent Proteins, Mice, Transgenic, Biology, Kidney, Collagen Type I, Mice, Western blot, Fibrosis, Gene expression, medicine, Animals, RNA, Messenger, Myofibroblasts, Oligonucleotide Array Sequence Analysis, Messenger RNA, medicine.diagnostic_test, Gene Expression Profiling, Kidney metabolism, General Medicine, medicine.disease, Molecular biology, Up-Regulation, Cell biology, Collagen Type I, alpha 1 Chain, Mice, Inbred C57BL, Disease Models, Animal, Basic Research, Real-time polymerase chain reaction, Mice, Inbred DBA, Nephrology, Myofibroblast, Ureteral Obstruction

Abstract

Myofibroblasts secrete matrix during chronic injury, and their ablation ameliorates fibrosis. Development of new biomarkers and therapies for CKD will be aided by a detailed analysis of myofibroblast gene expression during the early stages of fibrosis. However, dissociating myofibroblasts from fibrotic kidney is challenging. We therefore adapted translational ribosome affinity purification (TRAP) to isolate and profile mRNA from myofibroblasts and their precursors during kidney fibrosis. We generated and characterized a transgenic mouse expressing an enhanced green fluorescent protein (eGFP)–tagged L10a ribosomal subunit protein under control of the collagen1α1 promoter. We developed a one-step procedure for isolation of polysomal RNA from collagen1α1-eGFPL10a mice subject to unilateral ureteral obstruction and analyzed and validated the resulting transcriptional profiles. Pathway analysis revealed strong gene signatures for cell proliferation, migration, and shape change. Numerous novel genes and candidate biomarkers were upregulated during fibrosis, specifically in myofibroblasts, and we validated these results by quantitative PCR, in situ, and Western blot analysis. This study provides a comprehensive analysis of early myofibroblast gene expression during kidney fibrosis and introduces a new technique for cell-specific polysomal mRNA isolation in kidney injury models that is suited for RNA-sequencing technologies.

Published

2014

6. Sonic hedgehog is an autocrine viability factor for myofibroblastic hepatic stellate cells

Author

Susanne V Fleig, Kevin Brown, Hua Mao, Jason K. Sicklick, Ying Wang, Liu Yang, Anna Mae Diehl, Alessia Omenetti, and Yin-Xiong Li

Subjects

medicine.medical_specialty, animal structures, Platelet-derived growth factor, Antimetabolites, medicine.medical_treatment, Blotting, Western, Fluorescent Antibody Technique, Cell Separation, Ligands, Transfection, Article, Adenoviridae, chemistry.chemical_compound, Genes, Reporter, Transduction, Genetic, Internal medicine, medicine, Animals, Hedgehog Proteins, RNA, Messenger, Sonic hedgehog, Autocrine signalling, Hedgehog, Protein kinase B, Cell Proliferation, Caspase 7, Platelet-Derived Growth Factor, Hepatology, biology, Caspase 3, Reverse Transcriptase Polymerase Chain Reaction, Growth factor, Fibroblasts, Rats, Oncogene Protein v-akt, Autocrine Communication, Endocrinology, Bromodeoxyuridine, Liver, chemistry, embryonic structures, Hepatocytes, Cancer research, biology.protein, Hepatic stellate cell, Pericytes, Platelet-derived growth factor receptor

Abstract

Background/Aims Factors released during liver injury, such as platelet derived growth factor-BB (PDGF), promote accumulation of myofibroblastic hepatic stellate cells (MFB) that drive the pathogenesis of cirrhosis. The hedgehog (Hh) pathway regulates remodeling of other injured tissues. This study evaluates the hypothesis that autocrine production of Sonic hedgehog (Shh) promotes MFB growth. Methods Primary rat hepatic stellate cells (HSC) were treated without or with PDGF, a pharmacologic inhibitor of PDGF-regulated kinases, adenovirus expressing activated or dominant negative AKT, or Hh signaling inhibitors. Shh production, expression of Hh inhibitors and target genes, and HSC growth were assessed. Results HSC expressed Shh, Hh pathway components, and the Hh inhibitor, Hip. During culture Hip expression fell, Shh production increased, and Hh target gene expression was induced. Neutralizing Shh antibodies promoted apoptosis. Adding PDGF increased Shh expression and MFB growth. Both processes followed activation of AKT and were abrogated by AKT inhibitors. Adenoviral delivery of activated AKT up-regulated Shh expression, demonstrating a direct role for AKT in regulating Shh expression. Shh-neutralizing antibodies and other Hh pathway inhibitors blocked the mitogenic effects of PDGF. Conclusions These results identify Shh as an autocrine growth factor for MFB and suggest a role for Hh signaling in the pathogenesis of cirrhosis.

Published

2008

7. Hepatic accumulation of Hedgehog-reactive progenitors increases with severity of fatty liver damage in mice

Author

Hendrika M.A. VanDongen, Susanne V Fleig, Liu Yang, Anna Mae Diehl, Steve S. Choi, Jiawen Huang, Jason K. Sicklick, Alessia Omenetti, and Youngmi Jung

Subjects

Leptin, Male, medicine.medical_specialty, animal structures, Kruppel-Like Transcription Factors, Mice, Obese, Nerve Tissue Proteins, Biology, Ligands, Liver Cirrhosis, Experimental, Pathology and Forensic Medicine, Mice, chemistry.chemical_compound, Zinc Finger Protein Gli3, Hepatocyte Nuclear Factor 6, Fibrosis, Internal medicine, medicine, Animals, Hedgehog Proteins, Ethionine, Molecular Biology, Hedgehog, Liver injury, Fatty liver, Hepatotoxin, Mesenchymal Stem Cells, Cell Biology, medicine.disease, Hedgehog signaling pathway, Fatty Liver, Mice, Inbred C57BL, Endocrinology, chemistry, embryonic structures, Hepatocytes, Chemical and Drug Induced Liver Injury, Signal Transduction

Abstract

Progenitors regenerate fatty livers but the mechanisms involved are uncertain. The Hedgehog pathway regulates mesendodermal progenitors and modulates mesenchymal-epithelial interactions during tissue remodeling. To determine if Hedgehog signaling increases in liver progenitors during fatty liver injury, we compared expression of Hedgehog ligands and target genes across a spectrum of injury. Leptin-deficient ob/ob mice with fatty livers and their healthy lean littermates were studied before and after exposure to the hepatotoxin, ethionine. At baseline, ob/ob mice had greater liver damage than controls. Ethionine induced liver injury in both ob/ob and lean mice, with greater injury occurring in ob/ob mice. After ethionine, the ob/ob mice developed liver atrophy and fibrosis. Liver injury increased hepatic accumulation of progenitors, including ductular cells that produced and responded to Hedgehog ligands. A dose-response relationship was demonstrated between liver injury and expansion of Hedgehog-responsive progenitors. In severely damaged, atrophic livers, nuclei in mature-appearing hepatocytes accumulated the Hedgehog-regulated mesenchymal transcription factor, Gli2 and lost expression of the liver epithelial transcription factor, hepatocyte nuclear factor 6 (HNF-6). Hepatic levels of collagen mRNA and pericellular collagen fibrils increased concomitantly. Hence, fatty liver injury increases Hedgehog activity in liver progenitors, and this might promote epithelial-mesenchymal transitions that result in liver fibrosis.

Published

2007

8. Pharmacological GLI2 inhibition prevents myofibroblast cell-cycle progression and reduces kidney fibrosis

Author

Susanne V. Fleig, Dirk Heckl, Yoichiro Ikeda, Rafael Kramann, Helmut G. Rennke, Sushrut S. Waikar, Benjamin D. Humphreys, Steven L. Fabian, Steven L. Chang, Janewit Wongboonsin, Rebekka K. Schneider, Derek P. DiRocco, and Omar H. Maarouf

Subjects

animal structures, Pyridines, Kruppel-Like Transcription Factors, Biology, Zinc Finger Protein Gli2, Kidney, Zinc Finger Protein GLI1, Arsenicals, Cell Line, Mice, Downregulation and upregulation, Fibrosis, GLI2, medicine, Animals, Humans, Progenitor cell, Myofibroblasts, Mice, Knockout, integumentary system, Mesenchymal stem cell, General Medicine, Cell Cycle Checkpoints, medicine.disease, Glutathione, medicine.anatomical_structure, Pyrimidines, Cancer research, Kidney Diseases, Myofibroblast, Kidney disease, Research Article

Abstract

Chronic kidney disease is characterized by interstitial fibrosis and proliferation of scar-secreting myofibroblasts, ultimately leading to end-stage renal disease. The hedgehog (Hh) pathway transcriptional effectors GLI1 and GLI2 are expressed in myofibroblast progenitors; however, the role of these effectors during fibrogenesis is poorly understood. Here, we demonstrated that GLI2, but not GLI1, drives myofibroblast cell-cycle progression in cultured mesenchymal stem cell–like progenitors. In animals exposed to unilateral ureteral obstruction, Hh pathway suppression by expression of the GLI3 repressor in GLI1+ myofibroblast progenitors limited kidney fibrosis. Myofibroblast-specific deletion of Gli2, but not Gli1, also limited kidney fibrosis, and induction of myofibroblast-specific cell-cycle arrest mediated this inhibition. Pharmacologic targeting of this pathway with darinaparsin, an arsenical in clinical trials, reduced fibrosis through reduction of GLI2 protein levels and subsequent cell-cycle arrest in myofibroblasts. GLI2 overexpression rescued the cell-cycle effect of darinaparsin in vitro. While darinaparsin ameliorated fibrosis in WT and Gli1-KO mice, it was not effective in conditional Gli2-KO mice, supporting GLI2 as a direct darinaparsin target. The GLI inhibitor GANT61 also reduced fibrosis in mice. Finally, GLI1 and GLI2 were upregulated in the kidneys of patients with high-grade fibrosis. Together, these data indicate that GLI inhibition has potential as a therapeutic strategy to limit myofibroblast proliferation in kidney fibrosis.

Published

2013