4.5 Article

FIBRIN-GENIPIN ADHESIVE HYDROGEL FOR ANNULUS FIBROSUS REPAIR: PERFORMANCE EVALUATION WITH LARGE ANIMAL ORGAN CULTURE, IN SITU BIOMECHANICS, AND IN VIVO DEGRADATION TESTS

Journal

EUROPEAN CELLS & MATERIALS
Volume 28, Issue -, Pages 25-38

Publisher

AO RESEARCH INSTITUTE DAVOS-ARI
DOI: 10.22203/eCM.v028a03

Keywords

Intervertebral disc; annulus fibrosus repair; injectable hydrogel; fibrin-genipin; adhesive biomaterial; organ culture; motion segment testing; in vivo degradation; herniation; discectomy

Funding

  1. NIAMS/NIH grant [R01 AR057397]
  2. AO Exploratory Research Board
  3. Studienstiftung des deutschen Volkes award

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Annulus fibrosus (AF) defects from annular tears, herniation, and discectomy procedures are associated with painful conditions and accelerated intervertebral disc (IVD) degeneration. Currently, no effective treatments exist to repair AF damage, restore IVD biomechanics and promote tissue regeneration. An injectable fibrin-genipin adhesive hydrogel (Fib-Gen) was evaluated for its performance repairing large AF defects in a bovine caudal IVD model using ex vivo organ culture and biomechanical testing of motion segments, and for its in vivo longevity and biocompatibility in a rat model by subcutaneous implantation. Fib-Gen sealed AF defects, prevented IVD height loss, and remained well-integrated with native AF tissue following approximately 14,000 cycles of compression in 6-day organ culture experiments. Fib-Gen repair also retained high viability of native AF cells near the repair site, reduced nitric oxide released to the media, and showed evidence of AF cell migration into the gel. Biomechanically, Fib-Gen fully restored compressive stiffness to intact levels validating organ culture findings. However, only partial restoration of tensile and torsional stiffness was obtained, suggesting opportunities to enhance this formulation. Subcutaneous implantation results, when compared with the literature, suggested Fib-Gen exhibited similar biocompatibility behaviour to fibrin alone but degraded much more slowly. We conclude that injectable Fib-Gen successfully sealed large AF defects, promoted functional restoration with improved motion segment biomechanics, and served as a biocompatible adhesive biomaterial that had greatly enhanced in vivo longevity compared to fibrin. Fib-Gen offers promise for AF repairs that may prevent painful conditions and accelerated degeneration of the IVD, and warrants further material development and evaluation.

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