TY - JOUR A1 - Kamawal, Yama A1 - Steinert, Andre F A1 - Holzapfel, Boris M A1 - Rudert, Maximilian A1 - Barthel, Thomas T1 - Case report - calcification of the medial collateral ligament of the knee with simultaneous calcifying tendinitis of the rotator cuff JF - BMC Muscoskeletal Disorders N2 - Calcification of the medial collateral ligament (MCL) of the knee is a very rare disease. We report on a case of a patient with a calcifying lesion within the MCL and simultaneous calcifying tendinitis of the rotator cuff in both shoulders. Case presentation: Calcification of the MCL was diagnosed both via x-ray and magnetic resonance imaging (MRI) and was successfully treated surgically. Calcifying tendinitis of the rotator cuff was successfully treated applying conservative methods. Conclusion: This is the first case report of a patient suffering from both a calcifying lesion within the medial collateral ligament and calcifying tendinitis of the rotator cuff in both shoulders. Clinical symptoms, radio-morphological characteristics and macroscopic features were very similar and therefore it can be postulated that the underlying pathophysiology is the same in both diseases. Our experience suggests that magnetic resonance imaging and x-ray are invaluable tools for the diagnosis of this inflammatory calcifying disease of the ligament, and that surgical repair provides a good outcome if conservative treatment fails. It seems that calcification of the MCL is more likely to require surgery than calcifying tendinitis of the rotator cuff. However, the exact reason for this remains unclear to date. KW - case report KW - calcification KW - medical collateral ligament KW - knee rotator cuff KW - open surgical repair Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-147669 VL - 17 IS - 283 ER - TY - JOUR A1 - Dotterweich, Julia A1 - Schlegelmilch, Katrin A1 - Keller, Alexander A1 - Geyer, Beate A1 - Schneider, Doris A1 - Zeck, Sabine A1 - Tower, Robert J. J. A1 - Ebert, Regina A1 - Jakob, Franz A1 - Schütze, Norbert T1 - Contact of myeloma cells induces a characteristic transcriptome signature in skeletal precursor cells-implications for myeloma bone disease JF - Bone N2 - Physical interaction of skeletal precursors with multiple myeloma cells has been shown to suppress their osteogenic potential while favoring their tumor-promoting features. Although several transcriptome analyses of myeloma patient-derived mesenchymal stem cells have displayed differences compared to their healthy counterparts, these analyses insufficiently reflect the signatures mediated by tumor cell contact, vary due to different methodologies, and lack results in lineage-committed precursors. To determine tumor cell contact-mediated changes on skeletal precursors, we performed transcriptome analyses of mesenchymal stem cells and osteogenic precursor cells cultured in contact with the myeloma cell line INA-6. Comparative analyses confirmed dysregulation of genes which code for known disease-relevant factors and additionally revealed upregulation of genes that are associated with plasma cell homing, adhesion, osteoclastogenesis, and angiogenesis. Osteoclast-derived coupling factors, a dysregulated adipogenic potential, and an imbalance in favor of anti-anabolic factors may play a role in the hampered osteoblast differentiation potential of mesenchymal stem cells. Angiopoietin-Like 4 (ANGPTL4) was selected from a list of differentially expressed genes as a myeloma cell contact-dependent target in skeletal precursor cells which warranted further functional analyses. Adhesion assays with full-length ANGPTL4-coated plates revealed a potential role of this protein in INA6 cell attachment. This study expands knowledge of the myeloma cell contact-induced signature in the stromal compartment of myelomatous bones and thus offers potential targets that may allow detection and treatment of myeloma bone disease at an early stage. KW - marrow stromal cells KW - Endothelial growth-factor KW - precedes multiple-myeloma KW - monoclonial gammopathy KW - in-vitro KW - mesenchymal stem-cells KW - undetermined significance KW - angiogenic cytokines KW - peripheral-blood KW - gene-expression KW - Multiple myeloma KW - Bone disease KW - Angiopoietin-like 4 KW - Gene expression profiling KW - Mesenchymal stem cells KW - Osteogenic precursor cells Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-186688 VL - 93 ER - TY - THES A1 - Schmalzl, Jonas Georg T1 - Genetische Modifikation humaner mesenchymaler Stammzellen zur Stimulation der Knochenheilung T1 - Synergistic effect of Indian hedgehog and BMP-2 gene transfer to increase the osteogenic potential of human mesenchymal stem cells N2 - Fragestellung: Die Therapie von Knochendefekten kritischer Größe mit kompromittiertem Regenerationspotential, stellt ein schwerwiegendes Problem dar. Die Forschung auf dem Gebiet der Knochenheilung hat sich in jüngster Vergangenheit daher auf die Anwendung mesenchymaler Vorläuferzellen (MSZ) zur Stimulierung des Knochenwachstums konzentriert. In der vorliegenden Studie wurde in humanen MSZ eine Überexpression spezifischer Wachstumsfaktoren induziert mit dem Ziel, deren osteogenes Potential zu steigern. Methodik: MSZ wurden nach etablierten Protokollen expandiert. Durch adenovirale Transfektion wurde eine überexpression von grün fluoreszierendem Protein (GFP, Kontrolle), indian hedgehog (IHH), bone morphogenetic protein 2 (BMP-2) und IHH in Kombination mit BMP-2 induziert. Die MSZ wurden für 28 Tage mit osteogenem Differenzierungs- und Kontrollmedium kultiviert. Als weitere Kontrolle dienten native MSZ. Es wurden die Auswirkungen der jeweiligen genetischen Veränderungen auf die metabolische Aktivität (Alamar Blau), die Proliferation (Qubit dsDNA BR), die Aktivität des Enzyms alkalische Phosphatase (ALP)(p-Nitrophenylphosphat), die Mineralisierung (Alizarinrot S, Calcium O-Cresolphthalein) sowie auf die Expression charakteristischer Markergene untersucht (qRT-PCR). Ergebnis: In den ersten 72h nach Transfektion konnte eine leichte, im Vergleich zu nativen Zellen nicht signifikante Abnahme der metabolischen Aktivität in allen Gruppen beobachtet werden. Das Proliferationsverhalten transfizierter und nativer MSZ unterschied sich während des Untersuchungszeitraums nicht signifikant. Bei der Analyse der ALP-Aktivität zeigte sich ein typisches Rise-and-Fall Muster. Alle ost Gruppen wiesen sowohl im Assay als auch in der PCR eine signifikant höhere ALP-Aktivität auf. Die Überexpression von BMP-2 und IHH+BMP-2 bewirkte eine signifikant stärkere Mineralisierung an Tag 28. In der PCR zeigte sich für BMP-2 ost und IHH+BMP2 ost ein signifikanter Anstieg der Osteopontin und BMP-2 Expression über die Zeit. Zudem stieg bei allen ost Gruppen die Runx2 Expression bis Tag 21 an. Schlussfolgerung: Die virale Transfektion hatte keinen negativen Einfluss auf die metabolische Aktivität der Zellen oder deren Proliferationsverhalten. Die Überexpression von BMP-2 ohne oder in Kombination mit IHH führte zu einer vermehrten Produktion extrazellulärer Matrix und zu einer gesteigerten Genexpression osteogener Marker. Die virale Transfektion stellt daher eine vielversprechende Möglichkeit dar, das osteogene Potential von MSZ zu steigern. N2 - Introduction: To stimulate healing of large bone defects research has concentrated on the application of mesenchymal stem cells (MSCs). Methods: In the present study, we induced the overexpression of the growth factors bone morphogenetic protein 2 (BMP-2) and/or indian hedgehog (IHH) in human MSCs by adenoviral transduction to increase their osteogenic potential. GFP and non-transduced MSCc served as controls. The influence of the respective genetic modification on cell metabolic activity, proliferation, alkaline phosphatase activity (ALP), mineralization in cell culture, and osteogenic marker gene expression was investigated. Results: Transduction had no negative influence on cell metabolic activity or proliferation. ALP activity showed a typical rise-and-fall pattern with a maximal activity at day 14 and 21 after osteogenic induction. Enzyme activity was significantly higher in groups cultured with osteogenic media. The overexpression of BMP-2 and especially IHH+BMP-2 resulted in a significantly higher mineralization after 28 days. This was in line with obtained qRT-PCR analyses, which showed a significant increase in osteopontin and osteocalcin expression for osteogenicly induced BMP-2 and IHH+BMP-2 transduced cells when compared to the other groups. Moreover, an increase in runx2 expression was observed in all osteogenic groups toward day 21. It was again more pronounced for BMP-2 and IHH+BMP-2 transduced cells cultured in osteogenic media. Conclusion: In summary, viral transduction did not negatively influence cell metabolic activity and proliferation. The overexpression of BMP-2 in combination with or without IHH resulted in an increased deposition of mineralized extracellular matrix, and expression of osteogenic marker genes. Viral transduction therefore represents a promising means to increase the osteogenic potential of MSCs and the combination of different transgenes may result in synergistic effects. KW - Stammzellen KW - Osteogenese KW - Adenoviren KW - Wachstumsfaktoren KW - Knochenheilung KW - mesenchymale Stammzellen KW - bone morphogenic protein 2 KW - indian hedgehoc KW - gene transfer KW - osteogenic potential KW - mesenchymal stem cells KW - osteogenes Potential KW - growth factors KW - adenovirale Transduktion KW - Gen Transfer Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-142391 ER - TY - JOUR A1 - Wittmann, Katharina A1 - Sieber, Cornel A1 - von Stengel, Simon A1 - Kohl, Matthias A1 - Freiberger, Ellen A1 - Jakob, Franz A1 - Lell, Michael A1 - Engelke, Klaus A1 - Kemmler, Wolfgang T1 - Impact of whole body electromyostimulation on cardiometabolic risk factors in older women with sarcopenic obesity: the randomized controlled FORMOsA-sarcopenic obesity study JF - Clinical Interventions in Aging N2 - Background: Sarcopenic obesity (SO) is characterized by a combination of low muscle and high fat mass with an additive negative effect of both conditions on cardiometabolic risk. The aim of the study was to determine the effect of whole-body electromyostimulation (WB-EMS) on the metabolic syndrome (MetS) in community-dwelling women aged ≥70 years with SO. Methods: The study was conducted in an ambulatory university setting. Seventy-five community-dwelling women aged ≥70 years with SO living in Northern Bavaria, Germany, were randomly allocated to either 6 months of WB-EMS application with (WB-EMS&P) or without (WB-EMS) dietary supplementation (150 kcal/day, 56% protein) or a non-training control group (CG). WB-EMS included one session of 20 min (85 Hz, 350 µs, 4 s of strain–4 s of rest) per week with moderate-to-high intensity. The primary study endpoint was the MetS Z-score with the components waist circumference (WC), mean arterial pressure (MAP), triglycerides, fasting plasma glucose, and high-density lipoprotein cholesterol (HDL-C); secondary study endpoints were changes in these determining variables. Results: MetS Z-score decreased in both groups; however, changes compared with the CG were significant (P=0.001) in the WB-EMS&P group only. On analyzing the components of the MetS, significant positive effects for both WB-EMS groups (P≤0.038) were identified for MAP, while the WB-EMS group significantly differed for WC (P=0.036), and the WB-EMS&P group significantly differed for HDL-C (P=0.006) from the CG. No significant differences were observed between the WB-EMS groups. Conclusion: The study clearly confirms the favorable effect of WB-EMS application on the MetS in community-dwelling women aged ≥70 years with SO. However, protein-enriched supplements did not increase effects of WB-EMS alone. In summary, we considered this novel technology an effective and safe method to prevent cardiometabolic risk factors and diseases in older women unable or unwilling to exercise conventionally. KW - sarcopenia KW - obesity KW - whole-body electromyostimulation KW - cardiovascular KW - metabolic risk KW - metabolic syndrome KW - community-dwelling KW - older people Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-164930 VL - 11 ER - TY - THES A1 - Krätzig, Theresa T1 - Pilotstudie zum Vergleich der Knorpelrekonstruktion durch Autologe Chondrozytentransplantation und Autologe Stammzelltransplantation in Kollagen I Hydrogelen am Göttinger Mini-Pig T1 - Repair of full-thickness cartilage defects with autologous chondrocytes and autologous mesenchymal stem cells in a collagen-I-hydrogel - a pilot study in mini-pigs N2 - Traumatische und/oder degenerative, umschriebene Knorpeldefekte sind aufgrund der schlechten intrinsischen Regenerationseigenschaften des Knorpelgewebes immer noch eine chirurgische Herausforderung. Therapiemöglichkeiten mittels Knorpelrekonstruktion durch autologes Knorpelgewebe hat den Nachteil der „donor-site-morbidity“ und auch die mit guten klinischen und bildmorphologischen Ergebnissen bereits in der Klinik angewandte matrixgekoppelte autologe Chondrozytentransplantation kommt nicht ohne eine zusätzliche Operation und Entnahme von Knorpelgewebe aus. Autologe mesenchymale Stammzellen sind einfach mittels Beckenkammpunktion zu gewinnen und stellen aufgrund ihres Proliferations- und chondrogenen Differenzierungsvermögens eine vielversprechende Alternative dar. Die Tissue Engineering Division des orthopädischen König-Ludwig-Hauses in Würzburg befasst sich nun seit mehreren Jahren in verschiedenen Versuchsreihen unter anderem mit dieser Alternative der Knorpelrekonstruktion. Vor allem die Optimierung der Nutzung von Stammzellen, die Vordifferenzierungsmöglichkeiten in vitro und das Verhalten in verschiedenen Trägermatrizes wird erforscht. Die vorliegende Arbeit stellt eine Pilotstudie zur Anwendung von Stammzellen analog zu der in klinischer Anwendung befindlichen MACT in vivo in Göttinger Minipigs vor. Wir haben zeigen können, wenn auch nur mit einer geringen Fallzahl und fehlenden signifikanten Aussagen, dass Stammzellen eine vielversprechende Alternative zu Chondrozyten in der Versorgung von Gelenkknorpeldefekten darstellen. Eine Verarbeitung in Kollagen I Hydrogelen ist in gleicher Weise wie mit den Chondrozyten möglich und auch die mechanische Stabilität differiert nicht. Die histologischen und immunhistochemischen Auswertungen haben in den Stammzelltransplantaten gleich gute, in einigen Aspekten sogar gering bessere Ergebnisse erzielt als die bewährten Chondrozytentransplantate. In der Nachbehandlung schien die sofortige volle Belastung der frisch operierten Kniegelenke bei den Minipigs möglicherweise problematisch in Bezug auf die Fixierung und den Verbleib der Gel-Transplantate im Defekt. In der Klinik ist eine zeitweise Teilbelastung und anfangs lediglich passive Bewegung des Gelenks natürlich problemlos möglich. In der Zukunft werden durch Vordifferenzierung und Markierung der Stammzellen sowie durch Vorauswahl von Zellen mit einem hohen chondrogenen Differenzierungspotential die Ergebnisse von ähnlichen Versuchsreihen sicher noch optimiert werden können. N2 - Repair of full-thickness cartilage defects with autologous chondrocytes and autologous mesenchymal stem cells in a collagen-I-hydrogel - a pilot study in mini-pigs KW - Mesenchymale Stammzelle KW - Knorpelzelle KW - Tissue Engineering KW - Knorpelrekonstruktion KW - Chondrozytentransplantation KW - Stammzelltransplantation Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-138822 ER - TY - JOUR A1 - Dotterweich, Julia A1 - Tower, Robert J. A1 - Brandl, Andreas A1 - Müller, Marc A1 - Hofbauer, Lorenz C. A1 - Beilhack, Andreas A1 - Ebert, Regina A1 - Glüer, Claus C. A1 - Tiwari, Sanjay A1 - Schütze, Norbert A1 - Jakob, Franz T1 - The KISS1 Receptor as an In Vivo Microenvironment Imaging Biomarker of Multiple Myeloma Bone Disease JF - PLoS One N2 - Multiple myeloma is one of the most common hematological diseases and is characterized by an aberrant proliferation of plasma cells within the bone marrow. As a result of crosstalk between cancer cells and the bone microenvironment, bone homeostasis is disrupted leading to osteolytic lesions and poor prognosis. Current diagnostic strategies for myeloma typically rely on detection of excess monoclonal immunoglobulins or light chains in the urine or serum. However, these strategies fail to localize the sites of malignancies. In this study we sought to identify novel biomarkers of myeloma bone disease which could target the malignant cells and/or the surrounding cells of the tumor microenvironment. From these studies, the KISS1 receptor (KISS1R), a G-protein-coupled receptor known to play a role in the regulation of endocrine functions, was identified as a target gene that was upregulated on mesenchymal stem cells (MSCs) and osteoprogenitor cells (OPCs) when co-cultured with myeloma cells. To determine the potential of this receptor as a biomarker, in vitro and in vivo studies were performed with the KISS1R ligand, kisspeptin, conjugated with a fluorescent dye. In vitro microscopy showed binding of fluorescently-labeled kisspeptin to both myeloma cells as well as MSCs under direct co-culture conditions. Next, conjugated kisspeptin was injected into immune-competent mice containing myeloma bone lesions. Tumor-burdened limbs showed increased peak fluorescence compared to contralateral controls. These data suggest the utility of the KISS1R as a novel biomarker for multiple myeloma, capable of targeting both tumor cells and host cells of the tumor microenvironment. KW - multiple myeloma Lesions KW - fluorescence microscopy KW - biomarkers Myelomas KW - bone imaging KW - myeloma cells KW - fluorescent dyes Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-146960 VL - 11 IS - 5 ER - TY - JOUR A1 - Rudert, Maximilian A1 - Horas, Konstantin A1 - Hoberg, Maik A1 - Steinert, Andre A1 - Holzapfel, Dominik Emanuel A1 - Hübner, Stefan A1 - Holzapfel, Boris Michael T1 - The Wuerzburg procedure: the tensor fasciae latae perforator is a reliable anatomical landmark to clearly identify the Hueter interval when using the minimally-invasive direct anterior approach to the hip joint JF - BMC Musculoskeletal Disorders N2 - Background The key for successful delivery in minimally-invasive hip replacement lies in the exact knowledge about the surgical anatomy. The minimally-invasive direct anterior approach to the hip joint makes it necessary to clearly identify the tensor fasciae latae muscle in order to enter the Hueter interval without damaging the lateral femoral cutaneous nerve. However, due to the inherently restricted overview in minimally-invasive surgery, this can be difficult even for experienced surgeons. Methods and Surgical Technique In this technical note, we demonstrate for the first time how to use the tensor fasciae latae perforator as anatomical landmark to reliably identify the tensor fasciae latae muscle in orthopaedic surgery. Such perforators are used for flaps in plastic surgery as they are constant and can be found at the lateral third of the tensor fasciae latae muscle in a direct line from the anterior superior iliac spine. Conclusion As demonstrated in this article, a simple knowledge transfer between surgical disciplines can minimize the complication rate associated with minimally-invasive hip replacement. KW - anatomical landmark KW - direct anterior approach KW - Hueter interval KW - minimally-invasive KW - hip replacement KW - perforator Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-146031 VL - 17 IS - 57 ER -