| Literature DB >> 25982065 |
Anna Malashicheva1, Maria Bogdanova2, Arsenii Zabirnyk3, Natalia Smolina4, Elena Ignatieva3, Olga Freilikhman3, Anton Fedorov3, Renata Dmitrieva3, Gunnar Sjöberg5, Thomas Sejersen5, Anna Kostareva6.
Abstract
Various mutations in LMNA gene, encoding for nuclear lamin A/C protein, lead to laminopathies and contribute to over ten human disorders, mostly affecting tissues of mesenchymal origin such as fat tissue, muscle tissue, and bones. Recently it was demonstrated that lamins not only play a structural role providing communication between extra-nuclear structures and components of cell nucleus but also control cell fate and differentiation. In our study we assessed the effect of various LMNA mutations on the expression profile of mesenchymal multipotent stem cells (MMSC) during adipogenic and osteogenic differentiation. We used lentiviral approach to modify human MMSC with LMNA-constructs bearing mutations associated with different laminopathies--G465D, R482L, G232E, R527C, and R471C. The impact of various mutations on MMSC differentiation properties and expression profile was assessed by colony-forming unit analysis, histological staining, expression of the key differentiation markers promoting adipogenesis and osteogenesis followed by the analysis of the whole set of genes involved in lineage-specific differentiation using PCR expression arrays. We demonstrate that various LMNA mutations influence the differentiation efficacy of MMSC in mutation-specific manner. Each LMNA mutation promotes a unique expression pattern of genes involved in a lineage-specific differentiation and this pattern is shared by the phenotype-specific mutations.Entities:
Keywords: Differentiation; Expression profile; Lamin A/C; Multipotent mesenchymal stem cells; Mutation
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Year: 2015 PMID: 25982065 DOI: 10.1016/j.ymgme.2015.04.006
Source DB: PubMed Journal: Mol Genet Metab ISSN: 1096-7192 Impact factor: 4.797