CONSTRUCTION OF LENTIVIRAL VECTOR CONTAINING HOMO SAPIENS FORKHEAD BOX C2 GENE AND ITS EXPRESSION IN BONE MARROW MESENCHYMAL STEM CELLS OF RABBITS_Chinese Journal of Reparative and Reconstructive Surgery

Authors：

YOU Wulin , WANG Kunzheng , DUAN Dapeng , WANG Chunsheng , FAN Lihong , LIU Ruiyu.

Department of Orthopedics I, the Second Hospital Affiliated to the Medical College of Xi’an Jiaotong University, Xi’an Shaanxi, 710004, P.R.China. Corresponding author: WANG Kunzheng, E-mail: osteokzw1955@163.com;

Corresponding author：

Keywords：

Bone marrow mesenchymal stem cells; Homo sapiens forkhead box C2 gene; Lentivirus; Gene therapy; Rabbit

DOI：

10.7507/1002-1892.20130120

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Objective To construct the lentiviral vector containing homo sapiens forkhead box C2 (Foxc2) gene and to detect its expression in bone marrow mesenchymal stem cells (BMSCs) of rabbits. Methods Human Foxc2 gene coding region fragment was obtained by RT-PCR and then cloned into the plasmid of LV-green fluorescent protein (GFP) to prepare Foxc2 lentiviral plasmid. Foxc2 lentiviral plasmid, pGC-LV, pHelper1.0, and pHelper2.0 were co-transfected into 293T cells to obtain recombinant virus containing Foxc2 gene. The lentiviral titer was detected. BMSCs were isolated from bone marrow of rabbit and infected with Foxc2 recombined lentiviral, then the optimum multiplicity of infection (MOI) was determined by detecting the intensity of fluorescence expression. The expression of Foxc2 in the infected BMSCs was determined at 1, 3, and 7 days after transfection by inverted fluorescence microscope and Western blot. After osteogenic induction, Alizarin red staining was done to observe the formation of mineralized nodule. Results The Foxc2 recombinant lentiviral vector was constructed and was confirmed by restriction enzyme digestion and sequencing analysis. It could efficiently transfect 293T cells and express in 293T cells. The lentiviral titer was 2 × 108 TU/mL. The optimum MOI was 200. The inverted fluorescence microscope observation showed that the Foxc2 gene expressed in 84.5% ± 4.8% of infected BMSCs at 3 days after transfection. The expression of Foxc2 in infected BMSCs was stable and high, and increased gradually within 7 days after transfection by Western blot. At 2 weeks after osteogenic induction, Alizarin red staining showed that there were a large number of red calcified matrix deposition in the cytoplasm. Conclusion Foxc2 recombined lentivirus with high viral titer is successfully constructed and packaged, and the Foxc2 gene can be transfected into BMSCs with stable and high expression of Foxc2 in infected cells, and these cells may be applied for gene therapy of avascular necrosis of the femoral head.

Citation： YOU Wulin,WANG Kunzheng,DUAN Dapeng,WANG Chunsheng,FAN Lihong,LIU Ruiyu.. CONSTRUCTION OF LENTIVIRAL VECTOR CONTAINING HOMO SAPIENS FORKHEAD BOX C2 GENE AND ITS EXPRESSION IN BONE MARROW MESENCHYMAL STEM CELLS OF RABBITS. Chinese Journal of Reparative and Reconstructive Surgery, 2013, 27(5): 535-540. doi: 10.7507/1002-1892.20130120 Copy

1.	Mont MA, Hangerford DS. Non-traumatic avasclar necrosis of femarol head. J Bone Joint Surg (Am), 1995, 77(1): 459-474.
2.	Jones JP Jr. Concepts of etiology and early pathogensis of osteonecrotisis. Instr Course Lect, 1994, 43: 499-512.
3.	McMahon JM, Conroy S, Lyons M, et al. Gene transfer into rat mesenchymal stem cells: a comparative study of viral and nonviral vectors. Stem Cells Dev, 2006, 15(1): 87-96.
4.	Naldini L, Blomer U, Gage FH, et al. Efficient transfer, integration, and sustained long-term expression of the transgene in adult rat brains injected with a lentiviral vector. Proc Natl Acad Sci U S A, 1996, 93(21): 11382-11388.
5.	Cederberg A, Grønning LM, Ahrén B, et al. FOXC2 is a winged helix gene that counteracts obesity, hypertriglyceridemia, and diet-induced insulin resistance. Cell, 2001, 106(5): 563-573.
6.	Kim SH, Cho K, Choi HS, et al. The forkhead transcription factor Foxc2 stimulates osteoblast differentiation. Biochem Biophys Res Commun, 2009, 386(3): 532-536.
7.	庞永刚, 陈文弦, 崔鹏程. 人骨髓间质干细胞的优化培养. 中国修复重建外科杂志, 2004, 18(3): 220-224.
8.	Tsakano-Murakami R, Tokunaga N, Kondo N, et al. Glucocorticoid inhibits bone regeneration after osteonecrosis of the femoral head in aged female rats. Tohoku J Exp Med, 2009, 217(1): 51-58.
9.	Kuribayashi M, Fujioka M, Takahashi KA, et al. Combination analysis of three polymorphism for predicting the risk for steroid-induced osteonecrosis of the femoral head. J Orthop Sci, 2008, 13(4): 297-303.
10.	Séguin C, Kassis J, Busque L, et al. Non-traumatic necrosis of bone (osteonecrosis) is associated with endothelial cell activation but not thrombophilia. Rheumatology (Oxford), 2008, 47(8): 1151-1155.
11.	Deten A, Volz HC, Clamors S, et al. Hematopoietic stem cells do not repair the infracted mouse heart. Cardiovasc Res, 2005, 65(1): 52-63.
12.	Priller J. Grenzgänger: adult bone marrow cells populate the brain. Histoehem Cell Biol, 2003, 120(2): 85-91.
13.	Davis KE, Moldes M, Farmer SR. The forkhead transcription factor Foxc2 inhibits white adipocyte differentiation. J Biol Chem, 2004, 279(41): 42453-42461.
14.	Pandya S, Klimatcheva E, Planelles V. Lentivirus and foamy virus vectors: novel gene therapy tools. Expert Opin Biol Ther, 2001, 1(1): 17-40.
15.	Relph K, Harrington K, Pandha H. Recent developments and current status of gene therapy using viral vectors in the United Kingdom. BMJ, 2004, 329 (7470): 839-842.
16.	Hargrove PW, Kepes S, Hanawa H, et al. Globin Lentiviral vector insertion can perturb the expression of endogenous genes in betathalassemic hematopoietic cells. Mol Ther, 2008, 16(3): 525-533.
17.	Migliaccio AR, Quarto R, Piacibello W. Cell therapy: filling the gap between basic science and clinical trials October 15-17, 2001, Rome, Italy. Stem Cells, 2003, 21(3): 348-356.
18.	Lou S, Gu P, Chen F, et al. The effect of bone marrow stromal cells on neuronal differentiation of mesencephalic neural stem cells in Spragu-Dawley rats. Brain Res, 2003, 968(1): 114-121.
19.	Paul R, Haydon RC, Cheng HW, et al. Potential use of Sox9 gene therapy for intervertebral degenerative disc disease. Spine (Phila Pa 1976), 2003, 28(8): 755-763.
20.	Deans RJ, Moseley AB. Mesenchymal stem cells: biology and potential clinical uses. Exp Hematol, 2000, 28(8): 875-884.

1. Mont MA, Hangerford DS. Non-traumatic avasclar necrosis of femarol head. J Bone Joint Surg (Am), 1995, 77(1): 459-474.
2. Jones JP Jr. Concepts of etiology and early pathogensis of osteonecrotisis. Instr Course Lect, 1994, 43: 499-512.
3. McMahon JM, Conroy S, Lyons M, et al. Gene transfer into rat mesenchymal stem cells: a comparative study of viral and nonviral vectors. Stem Cells Dev, 2006, 15(1): 87-96.
4. Naldini L, Blomer U, Gage FH, et al. Efficient transfer, integration, and sustained long-term expression of the transgene in adult rat brains injected with a lentiviral vector. Proc Natl Acad Sci U S A, 1996, 93(21): 11382-11388.
5. Cederberg A, Grønning LM, Ahrén B, et al. FOXC2 is a winged helix gene that counteracts obesity, hypertriglyceridemia, and diet-induced insulin resistance. Cell, 2001, 106(5): 563-573.
6. Kim SH, Cho K, Choi HS, et al. The forkhead transcription factor Foxc2 stimulates osteoblast differentiation. Biochem Biophys Res Commun, 2009, 386(3): 532-536.
7. 庞永刚, 陈文弦, 崔鹏程. 人骨髓间质干细胞的优化培养. 中国修复重建外科杂志, 2004, 18(3): 220-224.
8. Tsakano-Murakami R, Tokunaga N, Kondo N, et al. Glucocorticoid inhibits bone regeneration after osteonecrosis of the femoral head in aged female rats. Tohoku J Exp Med, 2009, 217(1): 51-58.
9. Kuribayashi M, Fujioka M, Takahashi KA, et al. Combination analysis of three polymorphism for predicting the risk for steroid-induced osteonecrosis of the femoral head. J Orthop Sci, 2008, 13(4): 297-303.
10. Séguin C, Kassis J, Busque L, et al. Non-traumatic necrosis of bone (osteonecrosis) is associated with endothelial cell activation but not thrombophilia. Rheumatology (Oxford), 2008, 47(8): 1151-1155.
11. Deten A, Volz HC, Clamors S, et al. Hematopoietic stem cells do not repair the infracted mouse heart. Cardiovasc Res, 2005, 65(1): 52-63.
12. Priller J. Grenzgänger: adult bone marrow cells populate the brain. Histoehem Cell Biol, 2003, 120(2): 85-91.
13. Davis KE, Moldes M, Farmer SR. The forkhead transcription factor Foxc2 inhibits white adipocyte differentiation. J Biol Chem, 2004, 279(41): 42453-42461.
14. Pandya S, Klimatcheva E, Planelles V. Lentivirus and foamy virus vectors: novel gene therapy tools. Expert Opin Biol Ther, 2001, 1(1): 17-40.
15. Relph K, Harrington K, Pandha H. Recent developments and current status of gene therapy using viral vectors in the United Kingdom. BMJ, 2004, 329 (7470): 839-842.
16. Hargrove PW, Kepes S, Hanawa H, et al. Globin Lentiviral vector insertion can perturb the expression of endogenous genes in betathalassemic hematopoietic cells. Mol Ther, 2008, 16(3): 525-533.
17. Migliaccio AR, Quarto R, Piacibello W. Cell therapy: filling the gap between basic science and clinical trials October 15-17, 2001, Rome, Italy. Stem Cells, 2003, 21(3): 348-356.
18. Lou S, Gu P, Chen F, et al. The effect of bone marrow stromal cells on neuronal differentiation of mesencephalic neural stem cells in Spragu-Dawley rats. Brain Res, 2003, 968(1): 114-121.
19. Paul R, Haydon RC, Cheng HW, et al. Potential use of Sox9 gene therapy for intervertebral degenerative disc disease. Spine (Phila Pa 1976), 2003, 28(8): 755-763.
20. Deans RJ, Moseley AB. Mesenchymal stem cells: biology and potential clinical uses. Exp Hematol, 2000, 28(8): 875-884.

Chinese Journal of Reparative and Reconstructive Surgery

CONSTRUCTION OF LENTIVIRAL VECTOR CONTAINING HOMO SAPIENS FORKHEAD BOX C2 GENE AND ITS EXPRESSION IN BONE MARROW MESENCHYMAL STEM CELLS OF RABBITS

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