Neotendon formation induced by manipulation of the Smad8 signalling pathway in mesenchymal stem cells
Andrea Hoffmann, … , Gerhard Gross, Dan Gazit
Andrea Hoffmann, … , Gerhard Gross, Dan Gazit
Published April 3, 2006
Citation Information: J Clin Invest. 2006;116(4):940-952. https://doi.org/10.1172/JCI22689.
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Research Article

Neotendon formation induced by manipulation of the Smad8 signalling pathway in mesenchymal stem cells

Abstract

Tissue regeneration requires the recruitment of adult stem cells and their differentiation into mature committed cells. In this study we describe what we believe to be a novel approach for tendon regeneration based on a specific signalling molecule, Smad8, which mediates the differentiation of mesenchymal stem cells (MSCs) into tendon-like cells. A biologically active Smad8 variant was transfected into an MSC line that coexpressed the osteogenic gene bone morphogenetic protein 2 (BMP2). The engineered cells demonstrated the morphological characteristics and gene expression profile of tendon cells both in vitro and in vivo. In addition, following implantation in an Achilles tendon partial defect, the engineered cells were capable of inducing tendon regeneration demonstrated by double quantum filtered MRI. The results indicate what we believe to be a novel mechanism in which Smad8 inhibits the osteogenic pathway in MSCs known to be induced by BMP2 while promoting tendon differentiation. These findings may have considerable importance for the therapeutic replacement of tendons or ligaments and for engineering other tissues in which BMP plays a pivotal developmental role.

Authors

Andrea Hoffmann, Gadi Pelled, Gadi Turgeman, Peter Eberle, Yoram Zilberman, Hadassah Shinar, Keren Keinan-Adamsky, Andreas Winkel, Sandra Shahab, Gil Navon, Gerhard Gross, Dan Gazit

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Figure 8

Neotendon tissue formation in a partial-defect model in the Achilles tendon of a rat.

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Neotendon tissue formation in a partial-defect model in the Achilles ten...
C3H10T1/2-BMP2 (AC), C3H10T1/2-Smad8 L+MH2 (DF), and C3H10T1/2-BMP2/Smad8 L+MH2 cells infected with adeno-LacZ (GI) were implanted in an Achilles tendon defect in nude rats (3 × 106 cells per implant). (AF) Histological (H&E) and (GI) immunohistochemical (anti-LacZ) staining was performed 4 weeks after implantation. (AC) Tendon implanted with C3H10T1/2-BMP2 cells demonstrated cartilage and bone foci formation within the tendon tissue (arrows). (DF) Tendon implanted with C3H10T1/2-Smad8 L+MH2 cells showed mesenchyme-like tissue formation at the site of implantation (dashed arrow shows suture used to hold collagen scaffold in the defect site). (GI) Tendon implanted with C3H10T1/2-BMP2/Smad8 L+MH2 cells infected with adeno-LacZ prior to implantation showed LacZ-positive cells in the tenogenic implant (arrowheads). Cells seemed to be arranged parallel to the tendon long axis. Magnification, ×10 (top panels), ×40 (middle panels), ×100 (bottom panels).