Bàrbara Flix scite author profile

Bàrbara Flix

2Publications

79Citation Statements Received

98Citation Statements Given

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Affiliations

Hospital de Sant Pau, Autonomous University of Barcelona, Biomedical Research Networking Center on Neurodegenerative Diseases

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Comparison of Dysferlin Expression in Human Skeletal Muscle with That in Monocytes for the Diagnosis of Dysferlin Myopathy

et al. 2011

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BackgroundDysferlinopathies are caused by mutations in the dysferlin gene (DYSF). Diagnosis is complex due to the high clinical variability of the disease and because dysferlin expression in the muscle biopsy may be secondarily reduced due to a primary defect in some other gene. Dysferlin is also expressed in peripheral blood monocytes (PBM). Studying dysferlin in monocytes is used for the diagnosis of dysferlin myopathies. The aim of the study was to determine whether dysferlin expression in PBM correlates with that in skeletal muscle.Methodology/Principal FindingsUsing western-blot (WB) we quantified dysferlin expression in PBM from 21 pathological controls with other myopathies in whom mutations in DYSF were excluded and from 17 patients who had dysferlinopathy and two mutations in DYSF. Results were compared with protein expression in muscle by WB and immunohistochemistry (IH). We found a good correlation between skeletal muscle and monocytes using WB. However, IH results were misleading because abnormal expression of dysferlin was also observed in 13/21 pathological controls.Conclusions/SignificanceThe analysis of dysferlin protein expression in PBM is helpful when: 1) the skeletal muscle IH pattern is abnormal or 2) when muscle WB can not be performed either because muscle sample is lacking or insufficient or because the muscle biopsy is taken from a muscle at an end-stage and it mainly consists of fat and fibrotic tissue.

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Dysferlin Regulates Cell Adhesion in Human Monocytes

Morrée

Flix

Bagaric

et al. 2013

Journal of Biological Chemistry

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Background: Dysferlin mutations cause progressive muscular dystrophies with strong inflammation, yet its function in immune cells is unclear.Results: Dysferlin forms a protein complex with focal adhesion proteins, and its loss in monocytes results in deregulated adhesion. Conclusion: Dysferlin is involved in regulating cellular interactions in human monocytes. Significance: Dysferlin dysfunction in monocytes may contribute to pathology in dysferlinopathy.

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Bàrbara Flix

Comparison of Dysferlin Expression in Human Skeletal Muscle with That in Monocytes for the Diagnosis of Dysferlin Myopathy

Dysferlin Regulates Cell Adhesion in Human Monocytes

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