1. Comparative proteomic analysis of osteogenic differentiated human adipose tissue and bone marrow‐derived stromal cells
- Author
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Marcus Lehnhardt, Manfred Köller, Christina Sengstock, Christoph Wallner, Björn Behr, Johannes Maximilian Wagner, Mustafa Becerikli, Jan Geßmann, Lukas Schilde, Thomas A. Schildhauer, Caroline May, Annika Guntermann, Katrin Marcus, Dominik Seybold, Stephanie Dittfeld, Bettina Serschnitzki, and Mehran Dadras
- Subjects
Adult ,Male ,Proteomics ,0301 basic medicine ,Cell type ,Stromal cell ,Proteome ,Cell ,Integrin ,Subcutaneous Fat ,Adipose tissue ,Biology ,bone ,osteogenesis ,03 medical and health sciences ,0302 clinical medicine ,medicine ,Humans ,mesenchymal stem cells ,Mesenchymal stem cell ,Cell Differentiation ,hemic and immune systems ,Original Articles ,Cell Biology ,Middle Aged ,Fold change ,Cell biology ,030104 developmental biology ,medicine.anatomical_structure ,Adipose Tissue ,030220 oncology & carcinogenesis ,Cancellous Bone ,biology.protein ,Molecular Medicine ,Original Article ,Female ,Bone marrow - Abstract
Mesenchymal stromal cells are promising candidates for regenerative applications upon treatment of bone defects. Bone marrow‐derived stromal cells (BMSCs) are limited by yield and donor morbidity but show superior osteogenic capacity compared to adipose‐derived stromal cells (ASCs), which are highly abundant and easy to harvest. The underlying reasons for this difference on a proteomic level have not been studied yet. Human ASCs and BMSCs were characterized by FACS analysis and tri‐lineage differentiation, followed by an intraindividual comparative proteomic analysis upon osteogenic differentiation. Results of the proteomic analysis were followed by functional pathway analysis. 29 patients were included with a total of 58 specimen analysed. In these, out of 5148 identified proteins 2095 could be quantified in >80% of samples of both cell types, 427 in >80% of ASCs only and 102 in >80% of BMSCs only. 281 proteins were differentially regulated with a fold change of >1.5 of which 204 were higher abundant in BMSCs and 77 in ASCs. Integrin cell surface interactions were the most overrepresented pathway with 5 integrins being among the proteins with highest fold change. Integrin 11a, a known key protein for osteogenesis, could be identified as strongly up‐regulated in BMSC confirmed by Western blotting. The integrin expression profile is one of the key distinctive features of osteogenic differentiated BMSCs and ASCs. Thus, they represent a promising target for modifications of ASCs aiming to improve their osteogenic capacity and approximate them to that of BMSCs.
- Published
- 2020