Browse > Article

Highly Efficient Gene Expression in Rabbit Synoviocytes Using EBV-Based Plasmid  

Kim, Jin Young (Research Institute of Immunobiology, Catholic Research Institutes of Medical Science, Catholic University of Korea)
Oh, Sang Taek (Research Institute of Immunobiology, Catholic Research Institutes of Medical Science, Catholic University of Korea)
Youn, JeeHee (Department of Anatomy and Cell Biology, Hanyang University School of Medicine)
Lee, Suk Kyeong (Research Institute of Immunobiology, Catholic Research Institutes of Medical Science, Catholic University of Korea)
Publication Information
IMMUNE NETWORK / v.4, no.3, 2004 , pp. 190-197 More about this Journal
Abstract
Background: Rheumatoid arthritis (RA) is an autoimmune disorder characterized by chronic synovial inflammation which leads to joint destruction. Gene therapy of RA targets the players of inflammation or articular destruction. However, viral vectors have safety problems and side effects, while non-viral vectors suffer from inefficient gene transfer and fast loss of gene expression. To overcome the limits of non-vial vectors, an EBV-based plasmid which is known to exert prolonged high level gene expression can be used. Methods: pEBVGFP, pEBVIL-10, and pEBVvIL-10 were constructed by cloning GFP, IL-10, and vIL-10 genes into an EBV-based plasmid, respectively. The pGFP was used as a control plasmid. Each constructs were lipofected into HIG-82 rabbit synoviocytes. The expression of GFP was monitored by FACS and confocal microscopy. IL-10 and vIL-10 expressions were measured by ELISA. Results: GFP expression 2 days after transfection was achieved in 33.2% of cells. GFP-expressing cells transfected with pGFP decreased rapidly from 4 days after transfection and disappeared completely by 11 days. Cells transfected with pEBVGFP began to decrease slowly from 4 days. But GFP expression was detected for over 35 days. In addition, HIG-82 cells transfected with pEBVIL-10 ($44.6{\pm}1.5ng/ml$) or pEBVvIL-10 ($51.0{\pm}5.7ng/ml$) secreted these cytokines at high levels. High level cytokine production by hygromycin selection was maintained at least for up to 26 days after transfection. Conclusion: These results suggest that the EBV-based plasmid has a potential to improve non-viral gene transfer system and may be applicable to treat RA without the drawbacks of viral vectors.
Keywords
Rheumatoid arthritis; EBV-based plasmid; IL-10; vIL-10; synoviocyte; rabbit;
Citations & Related Records
Times Cited By KSCI : 1  (Citation Analysis)
연도 인용수 순위
1 Feldmann M, Brennan FM, Maini RN: Rheumatoid Arthritis. Cell 85;307-310, 1996   DOI   ScienceOn
2 Ghivizzani SC, Oligino TJ, Glorioso JC, Robbins PD, Evans CH: Direct gene delivery strategies for the treatment of rheumatoid arthritis. Drug Discov Today 6;259-267, 2001   DOI   ScienceOn
3 Min KA, Oh ST, Yoon KH, Kim CK, Lee SK: Prolonged gene expression in primary porcine pancreatic cells using an Epstein-Barr virus-based episomal vector. BBRC 305;108-115, 2003
4 Vervoordeldonk MJ, Tak PP: Gene therapy in rheumatic diseases. Best Pract Res Clin Rheumatol 15;771-788, 2001   DOI   ScienceOn
5 Zhang J, Wilson A, Alber S, Ma Z, Tang ZL, Satoh E, Mazda O, Watkins S, Huang L, Pitt B, Li S: Prolonged gene expression in mouse lung endothelial cells following transfection with Epstein-Barr virus-based episomal plasmid. Gene Ther 10;822-826, 2003   DOI   ScienceOn
6 Langle-Rouault F, Patzel V, Benavente A, Taillez M, Silvestre N, Bompard A, Sczakiel G, Jacobs E, Rittner K: Up to 100-Fold Increase of Apparent Gene Expression in the Presence of Epstein-Barr Virus oriP Sequences and EBNA1: Implications of the Nuclear Import of Plasmids. J Virol 72;6181-6185, 1998
7 Lubberts E, Joosten LA, Van Den Bersselaar L, Helsen MM, Bakker AC, Xing Z, Richards CD, Van Den Berg WB: Intraarticular IL-10 gene transfer regulates the expression of collagen-induced arthritis (CIA) in the knee and ipsilateral paw. Clin Exp Immunol 120;375-383, 2000   DOI
8 Ma Y, Thornton S, Duwel LE, Boivin GP, Giannini EH, Leiden JM, Bluestone JA, Hirsch R: Inhibition of Collagen- Induced Arthritis in Mice by Viral IL-10 Gene Transfer. J Immunol 161;1516-1524, 1998
9 Enzmann V, Hollborn M, Poschinger K, Wiedemann P, Kohen L: Immunosupperss-ion by IL-10-transfected human retinal pigment epithelialcells in vitro. Curr Eye Res 23;98-105, 2001   DOI   ScienceOn
10 Taga K, Tosato G: IL-10 inhibits human T cell proliferation and IL-2 production. J Immunol 148;1143-1148, 1992
11 Afeltra A: Treatment of Rheumatoid arthritis: New Therapeutic Approaches with Biological Agents. Curr Drug Targets Immune Endocr Metabol Disord 1;45-65, 2001   DOI   ScienceOn
12 Katsikis PD, Chu CQ, Brennan FM, Maini RN, Feldmann M: Immunoregulatory role of interleukin 10 in rheumatoid arthritis. J Exp Med 179;1517-1527, 1994   DOI   ScienceOn
13 Evans CH, Ghivizzani SC, Kang R, Muzzonigro T, Wasko MC, Herndon JH, Robbins PD: Gene therapy for rheumatic diseases. Arthritis Rheum 42;1-16, 1999   DOI   ScienceOn
14 Robbins PD, Evans CH, Chernajovsky Y: Gene therapy for arthritis. Gene Ther 10;902-911, 2003   DOI   ScienceOn
15 Mazda O: Improvement of Nonviral Gene Therapy by Epstein-Barr Virus (EBV)-based Plasmid Vectors. Curr Gene Ther 2;379-392, 2002   DOI   PUBMED   ScienceOn
16 Boissier MC, Bessis N: Therapeutic gene transfer for rheumatoid arthritis. Reumatismo 56;51-61, 2004
17 Feldmann M, Brennan FM, Maini, RN: Role of cytokines in rheumatoid arthritis. Annu Rev Immunol 14;397-440, 1996   DOI   ScienceOn
18 Sasaki M, Jordan P, Houghton J, Meng X, Itoh M, Joh T, Alexander JS: Transfection of IL-10 expression vectors into endothelial cultures attenuates alpha4beta7-dependent lymphocyte adhesion mediated by MAdCAM-1. BMC Gastroenterol 3;3-10, 2003   DOI   ScienceOn
19 Middleton T, Sugden B: Retention of plasmid DNA in mammalian cells is enhanced by binding of the Epstein-Barr virus replication protein EBNA1. J Virol 68;4067-4071, 1994
20 Schulze-Koops H, Kalden JR: The balance of Th1/Th2 cytokines in rheumatoid arthritis. Best Pract Res Clin Rheumatol 15;677-691, 2001   DOI   ScienceOn
21 Bessis N, Doucet C, Cottard V, Douar AM, Firat H, Jorgensen C, Mezzina M, Boissier MC: Gene therapy for rheumatoid arthritis. J Gene Med 4;581-591, 2002   DOI   ScienceOn
22 Henderson B, Glynn LE: Metabolic alterations in the synoviocytes in chronically inflamed knee joints in immune arthritis in the rabbits: comparison with rheumatoid arthritis. Br J Exp Pathol. 62;27-33, 1981
23 Otani K, Nita I, Macaulay W, Georgescu HI, Robbins PD, Evans CH: Suppression of antigen-induced arthritis in rabbits by ex vivo gene therapy. J Immunol 156;3558-3562, 1996
24 오상택, 민경아, 김종국, 이숙경: HSV-TK 유전자를 암호화하는 EBV 유래 플라스미드를 이용한 유전자 치료. 약제학회지 33;267-272, 2003   과학기술학회마을
25 Mucke S, Polack A, Pawlita M, Zehnpfennig D, Massoudi N, Bohlen H, Doerfler W, Bornkamm G, Diehl V, Wolf J: Suitability of Epstein-Barr virus-based episomal vectors for expression of cytokine genes in human lymphoma cells. Gene Ther 4;82-92, 1997   DOI   ScienceOn