Augmented healing of critical-size calvarial defects by baculovirus-engineered MSCs that persistently express growth factors

  • Chin Yu Lin
  • , Yu Han Chang
  • , Chun Yu Kao
  • , Chia Hsin Lu
  • , Li Yu Sung
  • , Tzu Chen Yen
  • , Kun Ju Lin
  • , Yu Chen Hu*
  • *Corresponding author for this work

Research output: Contribution to journalJournal Article peer-review

79 Scopus citations

Abstract

Repair of large calvarial bony defects remains clinically challenging because successful spontaneous calvarial re-ossification rarely occurs. Although bone marrow-derived mesenchymal stem cells (BMSCs) genetically engineered with baculovirus (BV) for transient expression of osteogenic/angiogenic factors hold promise for bone engineering, we hypothesized that calvarial bone healing necessitates prolonged growth factor expression. Therefore, we employed a hybrid BV vector system whereby one BV expressed FLP while the other harbored the BMP2 (or VEGF) cassette flanked by Frt sequences. Transduction of rabbit BMSCs with the FLP/Frt-based BV vector led to FLP-mediated episome formation, which not only extended the BMP2/VEGF expression beyond 28 days but augmented the BMSCs osteogenesis. After allotransplantation into rabbits, X-ray, PET/CT, μCT and histological analyses demonstrated that the sustained BMP2/VEGF expression remarkably ameliorated the angiogenesis and regeneration of critical-size (8 mm) calvarial defects, when compared with the group implanted with BMSCs transiently expressing BMP2/VEGF. The prolonged expression by BMSCs accelerated the bone remodeling and regenerated the bone through the natural intramembranous pathway, filling ≈83% of the area and ≈63% of the volume in 12 weeks. These data implicated the potential of the hybrid BV vector to engineer BMSCs for sustained BMP2/VEGF expression and the repair of critical-size calvarial defects.

Original languageEnglish
Pages (from-to)3682-3692
Number of pages11
JournalBiomaterials
Volume33
Issue number14
DOIs
StatePublished - 05 2012

Keywords

  • Baculovirus
  • Calvarial bone defect
  • Gene therapy
  • Mesenchymal stem cells
  • Sustained expression
  • Tissue engineering

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