Your search keyword '"Cottin, Patrick"' showing total 4 results

1. Calpains: Markers of tumor aggressiveness?

Author

Roumes, Hélène, Leloup, Ludovic, Dargelos, Elise, Brustis, Jean-Jacques, Daury, Laetitia, and Cottin, Patrick

Subjects

*CALPAIN, *TUMOR markers, *RHABDOMYOSARCOMA, *CYTOSKELETON, *CANCER invasiveness, *CELL migration, *METASTASIS

Abstract

Abstract: Rhabdomyosarcoma (RMS) are soft-tissue sarcoma commonly encountered in childhood. RMS cells can acquire invasive behavior and form metastases. The metastatic dissemination implicates many proteases among which are μ-calpain and m-calpain. Study of calpain expression and activity underline the deregulation of calpain activity in RMS. Analysis of kinetic characteristics of RMS cells, compared to human myoblasts LHCN-M2 cells, shows an important migration velocity in RMS cells. One of the major results of this study is the positive linear correlation between calpain activity and migration velocity presenting calpains as a marker of tumor aggressiveness. The RMS cytoskeleton is disorganized. Specifying the role of μ- and m-calpain using antisense oligonucleotides led to show that both calpains up-regulate α- and β-actin in ARMS cells. Moreover, the invasive behavior of these cells is higher than that of LHCN-M2 cells. However, it is similar to that of non-treated LHCN-M2 cells, when calpains are inhibited. In summary, calpains may be involved in the anarchic adhesion, migration and invasion of RMS. The direct relationship between calpain activity and migration velocities or invasive behavior indicates that calpains could be considered as markers of tumor aggressiveness and as potential targets for limiting development of RMS tumor as well as their metastatic behavior. [Copyright &y& Elsevier]

Published

2010

2. Up-regulation of calcium-dependent proteolysis in human myoblasts under acute oxidative stress

Author

Dargelos, Elise, Brulé, Cédric, Stuelsatz, Pascal, Mouly, Vincent, Veschambre, Philippe, Cottin, Patrick, and Poussard, Sylvie

Subjects

*PROTEOLYSIS, *CELLULAR control mechanisms, *PHYSIOLOGICAL effects of calcium, *OXIDATIVE stress, *MYOBLASTS, *HYDROGEN peroxide, *SATELLITE cells, *MUSCLE physiology

Abstract

Abstract: The reduced regenerative potential of muscle fibres, most likely due to a decreased number and/or function of satellite cells, could play a significant role in the progression of muscle ageing. Accumulation of reactive oxygen species has been clearly correlated to sarcopenia and could contribute to the impairment of satellite cell function. In this work we have investigated the effect of oxidative stress generated by hydrogen peroxide in cultured human skeletal muscle satellite cells. We specifically focused on the activity and regulation of calpains. These calcium-dependent proteases are known to regulate many transduction pathways including apoptosis and play a critical role in satellite cell function. In our experimental conditions, which induce an increase in calcium concentration, protein oxidation and apoptotic cell death, a significant up-regulation of calpain expression and activity were observed and ATP synthase, a major component of the respiratory chain, was identified as a calpain target. Interestingly we were able to protect the cells from these H2O2-induced effects and prevent calpain up-regulation with a natural antioxidant extracted from pine bark (Oligopin®). These data strongly suggest that oxidative stress could impair satellite cell functionality via calpain-dependent pathways and that an antioxidant such as Oligopin® could prevent apoptosis and calpain activation. [Copyright &y& Elsevier]

Published

2010

3. Myoblast migration is regulated by calpain through its involvement in cell attachment and cytoskeletal organization

Author

Dedieu, Stéphane, Poussard, Sylvie, Mazères, Germain, Grise, Florence, Dargelos, Elise, Cottin, Patrick, and Brustis, Jean-Jacques

Subjects

*CELL migration, *CALPAIN, *MYOBLASTS, *CELL lines

Abstract

Cell migration is a fundamental cellular function particularly during skeletal muscle development. Ubiquitous calpains are well known to play a pivotal role during muscle differentiation, especially at the onset of fusion. In this study, the possible positive regulation of myoblast migration by calpains, a crucial step required to align myoblasts to permit them to fuse, was investigated. Inhibition of calpain activity by different pharmacological inhibitors argues for the involvement of these proteinases during the migration of myoblasts. Moreover, a clonal cell line that fourfold overexpresses calpastatin, the endogenous inhibitor of calpains, and that exhibits deficient calpain activities was obtained. The results showed that the migratory capacity of C2C12 and fusion into multinucleated myotubes were completely prevented in these clonal cells. Calpastatin-overexpressing myoblasts unable to migrate were characterized by rounded morphology, the loss of membrane extensions, the disorganization of stress fibers and exhibited a major defect in new adhesion formation. Surprisingly, the proteolytic patterns of desmin, talin, vinculin, focal adhesion kinase (FAK) and ezrin, radixin, moesin (ERM) proteins are the same in calpastatin-overexpressing myoblasts as compared to control cells. However, an important accumulation of myristoylated alanine-rich C kinase substrate (MARCKS) was observed in cells showing a reduced calpain activity, suggesting that the proteolysis of this actin-binding protein is calpain-dependent and could be involved in both myoblast adhesion and migration. [Copyright &y& Elsevier]

Published

2004

4. Transactivation of capn2 by Myogenic Regulatory Factors During Myogenesis

Author

Dedieu, Stéphane, Mazères, Germain, Dourdin, Nathalie, Cottin, Patrick, and Brustis, Jean-Jacques

Subjects

*PROTEOLYTIC enzymes, *SERUM

Abstract

The calcium-activated cysteine protease m-calpain plays a pivotal role during the earlier stages of myogenesis, particularly during fusion. The enzyme is a heterodimer, encoded by the genes capn2, for the large subunit, and capn4, for the small subunit. To study the regulation of m-calpain, the DNA sequence upstream of capn2 was analyzed for promoter elements, revealing the existence of five consensus-binding sites (E-box) for several myogenic regulatory factors and one binding site for myocyte enhancer factor-2 (MEF-2). Transient transfections with reporter gene constructs containing the E-box revealed that MyoD presents a high level of transactivation of reporter constructs containing this region, in particular the sequences including the MEF-2/E4-box. In addition, over-expression of various myogenic factors demonstrated that MyoD and myogenin with much less efficiency, can up-regulate capn2, both singly and synergistically, while Myf5 has no effect on synthesis of the protease. Experiments with antisense oligonucleotides directed against each myogenic factor revealed that MyoD plays a specific and pivotal role during capn2 regulation, and cannot be replaced wholly by myogenin and Myf5. [Copyright &y& Elsevier]

Published

2003