More than 200 million persons worldwide suffer from chronic kidney diseases (CKD). Glomerular disorders account for the majority of cases of CKD. Podocyte injury is central to the development of many different glomerular diseases. Even in normal ageing podocyte loss contributes to age-related decline in renal function. Landmark genetic studies identified hereditary mutations in genes expressed by glomerular podocytes as cause of proteinuria, progressive glomerulosclerosis and end-stage renal disease. These studies initiated a spurt of research that profoundly changed our view of the glomerular filtration barrier and the role of podocyte injury in the development of glomerular disease. Alterations of various independent signaling pathways cause podocyte dysfunction and loss leading to the development of focal and segmental glomerulosclerosis (FSGS) in experimental animals. Unfortunately, the remarkable advance in the understanding of glomerular biology has not yet resulted in better treatment options for patients with podocyte disease such as FSGS and treatment alternatives in patients with steroid-resistant forms of FSGS are still scarce. This CRU is based on the understanding that (primary) FSGS is not a uniform disease entity, but represents a histopathological pattern of injury resulting from many different causative disease mechanisms. However, distinguishing different pathophysiological entities and their specific molecular and cell biological disease-causing mechanisms is key to the development of novel targeted therapeutic strategies. Here, we will combine forces to translate pathophysiological principles studied in mice and newly identified genomic alterations in patients into new diagnostic and therapeutic tools. We will study distinct disease pathomechanisms of podocyte injury, ranging from alterations of slit diaphragm signaling, over cytoskeletal rearrangements, the deregulation of transcriptional networks and non-coding RNA molecules to mitochondrial and metabolic dysfunction and defective immune and stress signaling, to (1) provide a better understanding of individual disease pathomechanisms in podocyte disease, (2) identify markers of these alterations for diagnostics, (3) develop potential tailored therapeutic interventions, based on the pathophysiologic understanding of podocyte disorders in individual patients. The ultimate aim is to be able to diagnose and treat distinctly deregulated pathways in podocyte disease with a tailored approach, i.e. a precision medicine strategy. From the very beginning the Center for Clinical Trials at the University Hospital Cologne will be involved to establish a national registry for renal biopsy, blood and urine samples together with clinical data. We are convinced that this approach will ultimately result in practice-changing research that leads to a new mechanism-based classification of FSGS and allows tailored new treatment options and individualized treatment approaches.

DFG Programme Clinical Research Units

• Alterations of slit diaphragm proteins and the pathogenesis of albuminuria and FSGS (Applicants Benzing, Thomas ;  Bozek, Katarzyna )
• Central mouse generation, phenotyping and imaging (Applicants Bozek, Katarzyna ;  Schauss, Astrid )
• Context-dependent transcriptional programs governed by YAP and TAZ and their nuclear control mechanisms in FSGS (Applicants Habbig, Sandra ;  Schermer, Bernhard )
• Coordination Funds (Applicant Benzing, Thomas )
• DNA damage response pathways in podocytes: novel targets to treat focal segmental glomerulosclerosis (Applicants Kurschat, Christine ;  Schumacher, Björn )
• Gene-regulatory networks in podocytes in health and disease (Applicants Beyer, Andreas ;  Kann, Martin )
• MCD/FSGS registry and digital nephropathology (Applicants Grundmann, Franziska ;  Johannis, Wibke ;  Weber, Lutz T. )
• Podocyte lncRNAs – a novel player in focal-segmental glomerulosclerosis (Applicants Dieterich, Christoph ;  Müller, Roman-Ulrich )
• Role of the podocyte adhesome in the development of FSGS (Applicant Schell, Ph.D., Christoph B. )
• Sequencing-based innovative approaches to study FSGS (Applicants Altmüller, Janine ;  Antczak, Ph.D., Philipp ;  Beck, Bodo )
• The role of mononuclear phagocytes in the development of FSGS (Applicants Brähler, Sebastian ;  Kurts, Christian )
• Understanding the dynamic interplay of altered calcium signaling and actin remodeling in podocytes in FSGS using in vivo imaging (Applicant Hackl, Matthias Johannes )
• Unraveling metabolic signaling in podocytes and its contribution to FSGS (Applicants Brinkkötter, Paul-Thomas ;  Völker, Linus )

Spokesperson Professor Dr. Thomas Benzing

Leader Professor Dr. Paul-Thomas Brinkkötter

Project Heads Dr. Janine Altmüller; Dr. Philipp Antczak, Ph.D.; Privatdozent Dr. Bodo Beck; Professor Dr. Andreas Beyer; Professorin Dr. Katarzyna Bozek; Dr. Sebastian Brähler; Professor Dr. Christoph Dieterich; Dr. Franziska Grundmann; Privatdozentin Dr. Sandra Habbig; Dr. Matthias Johannes Hackl; Dr. Martin Höhne; Dr. Wibke Johannis; Dr. Martin Kann; Professor Dr. Christian Kurts; Professor Dr. Roman-Ulrich Müller; Dr. Astrid Schauss; Privatdozent Dr. Christoph B. Schell, Ph.D.; Professor Dr. Bernhard Schermer; Dr. Linus Völker; Professor Dr. Lutz T. Weber