Author
Listed:
- Christine-Maria Horejs
(Imperial College London
Imperial College London
Institute of Biomedical Engineering, Imperial College London
Karolinska Institutet)
- Jean-Philippe St-Pierre
(Imperial College London
Imperial College London
Institute of Biomedical Engineering, Imperial College London
Present address: Department of Chemical and Biological Engineering, University of Ottawa, 161 Louis-Pasteur, Ottawa, Ontario, Canada K1N 6N5)
- Juha R. M. Ojala
(Karolinska Institutet)
- Joseph A. M. Steele
(Imperial College London
Imperial College London
Institute of Biomedical Engineering, Imperial College London
Karolinska Institutet)
- Patricia Barros da Silva
(Karolinska Institutet)
- Angela Rynne-Vidal
(Centro de Biología Molecular Severo Ochoa, CSIC, Universidad Autónoma de Madrid, Campus de Cantoblanco)
- Stephanie A. Maynard
(Imperial College London
Imperial College London
Institute of Biomedical Engineering, Imperial College London)
- Catherine S. Hansel
(Imperial College London
Imperial College London
Institute of Biomedical Engineering, Imperial College London
Imperial College London)
- Clara Rodríguez-Fernández
(Imperial College London
Imperial College London
Institute of Biomedical Engineering, Imperial College London)
- Manuel M. Mazo
(Imperial College London
Imperial College London
Institute of Biomedical Engineering, Imperial College London)
- Amanda Y. F. You
(Imperial College London
Imperial College London
Institute of Biomedical Engineering, Imperial College London)
- Alex J. Wang
(Imperial College London
Imperial College London
Institute of Biomedical Engineering, Imperial College London)
- Thomas von Erlach
(Imperial College London
Imperial College London
Institute of Biomedical Engineering, Imperial College London)
- Karl Tryggvason
(Karolinska Institutet
Cardiovascular and Metabolic Disorders Program, Duke-NUS)
- Manuel López-Cabrera
(Centro de Biología Molecular Severo Ochoa, CSIC, Universidad Autónoma de Madrid, Campus de Cantoblanco)
- Molly M. Stevens
(Imperial College London
Imperial College London
Institute of Biomedical Engineering, Imperial College London
Karolinska Institutet)
Abstract
Matrix metalloproteinases (MMPs) contribute to the breakdown of tissue structures such as the basement membrane, promoting tissue fibrosis. Here we developed an electrospun membrane biofunctionalized with a fragment of the laminin β1-chain to modulate the expression of MMP2 in this context. We demonstrate that interfacing of the β1-fragment with the mesothelium of the peritoneal membrane via a biomaterial abrogates the release of active MMP2 in response to transforming growth factor β1 and rescues tissue integrity ex vivo and in vivo in a mouse model of peritoneal fibrosis. Importantly, our data demonstrate that the membrane inhibits MMP2 expression. Changes in the expression of epithelial-to-mesenchymal transition (EMT)-related molecules further point towards a contribution of the modulation of EMT. Biomaterial-based presentation of regulatory basement membrane signals directly addresses limitations of current therapeutic approaches by enabling a localized and specific method to counteract MMP2 release applicable to a broad range of therapeutic targets.
Suggested Citation
Christine-Maria Horejs & Jean-Philippe St-Pierre & Juha R. M. Ojala & Joseph A. M. Steele & Patricia Barros da Silva & Angela Rynne-Vidal & Stephanie A. Maynard & Catherine S. Hansel & Clara Rodríguez, 2017.
"Preventing tissue fibrosis by local biomaterials interfacing of specific cryptic extracellular matrix information,"
Nature Communications, Nature, vol. 8(1), pages 1-15, August.
Handle:
RePEc:nat:natcom:v:8:y:2017:i:1:d:10.1038_ncomms15509
DOI: 10.1038/ncomms15509
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