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Global remodelling of cellular microenvironment due to loss of collagen VII
Authors:Victoria Küttner  Claudia Mack  Kristoffer TG Rigbolt  Johannes S Kern  Oliver Schilling  Hauke Busch  Leena Bruckner‐Tuderman  Jörn Dengjel
Institution:1. School of Life Science‐LifeNet, Freiburg Institute for Advanced Studies (FRIAS), University of Freiburg, , Freiburg, Germany;2. ZBSA Center for Biological Systems Analysis, University of Freiburg, , Freiburg, Germany;3. Department of Dermatology, University Freiburg Medical Center, , Freiburg, Germany;4. Faculty of Biology, University of Freiburg, , Freiburg, Germany;5. Institute for Molecular Medicine and Cell Research, University of Freiburg, , Freiburg, Germany;6. BIOSS Centre for Biological Signalling Studies, University of Freiburg, , Freiburg, Germany
Abstract:The mammalian cellular microenvironment is shaped by soluble factors and structural components, the extracellular matrix, providing physical support, regulating adhesion and signalling. A global, quantitative mass spectrometry strategy, combined with bioinformatics data processing, was developed to assess proteome differences in the microenvironment of primary human fibroblasts. We studied secreted proteins of fibroblasts from normal and pathologically altered skin and their post‐translational modifications. The influence of collagen VII, an important structural component, which is lost in genetic skin fragility, was used as model. Loss of collagen VII had a global impact on the cellular microenvironment and was associated with proteome alterations highly relevant for disease pathogenesis including decrease in basement membrane components, increase in dermal matrix proteins, TGF‐β and metalloproteases, but not higher protease activity. The definition of the proteome of fibroblast microenvironment and its plasticity in health and disease identified novel disease mechanisms and potential targets of intervention.
Keywords:disease proteomics  extracellular matrix (ECM)  mass spectrometry  MMP14  primary human fibroblasts
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