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Long-term Graft Acceptance in Rat Heart Transplantation by CTLA4Ig Gene Transfection Combined with FTY720 Treatment
被引:0
|作者:
Masanao Ohba
Xiao-Kang Li
Yusuke Kita
Shin Enosawa
Naoko Funeshima
Haruko Nagai
Hui-qi Zhang
Torayuki Okuyama
Shohei Ogoshi
Shiro Sasaguri
Hiroshi Amemiya
Seiichi Suzuki
机构:
[1] Department of Experimental Surgery and Bioengineering,
[2] National Children's Medical Research Center,undefined
[3] 3-35-31 Taishido,undefined
[4] Setagaya-ku,undefined
[5] Tokyo 154-8509,undefined
[6] Japan,undefined
[7] Department of Surgery II,undefined
[8] Kochi Medical School,undefined
[9] 185-1 Kohasu,undefined
[10] Oko-cho,undefined
[11] Nankoku,undefined
[12] Kochi 783-8505,undefined
[13] Japan,undefined
[14] Department of Genetics,undefined
[15] National Children's Medical Research Center,undefined
[16] 3-35-31,undefined
[17] Taishido,undefined
[18] Setagaya-ku,undefined
[19] Tokyo 154-8509,undefined
[20] Japan,undefined
来源:
World Journal of Surgery
|
2001年
/
25卷
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摘要:
CTLA4Ig strongly adheres to B7 molecules on antigen-presenting cells to block intracellular signal transduction via CD28 on helper T cells, which eventually inhibits immune responses. We have demonstrated that the administration to recipient animals of adenoviral vectors containing CTLA4Ig gene (adCTLA4Ig) prolonged graft survival, although the gene expression diminished in a time-dependent manner and the grafts were finally rejected. In addition, recipient animals treated with FTY720, a new immunosuppressant, exhibited a decrease in the number of peripheral lymphocytes due to apoptosis. In this study, we performed adCTLA4Ig transfection combined with FTY720 treatment in heart-grafted rats to determine if the combination could induce a mutual effect on graft survival. The recipient animals were given injections of 1 × 109 plaque-forming units of adCTLA4Ig via the tail vein immediately after grafting. On the day before transplantation we administered FTY720 orally to some of these animals at a dosage of 5 mg/kg and again on the day of transplantation. The median graft survival period in the adCTLA4Ig-only group was 27 days, whereas that in the combination group was markedly prolonged to 56 days. Of 15 grafts, 5 survived indefinitely. In these groups we observed detectable levels of CTLA4Ig in the sera 49 days after grafting; the levels were always higher in the combination group than in the adCTLA4Ig-only group. As a result, this study revealed that FTY720 and adCTLA4Ig have a potent mutual effect on graft survival during rat heart transplantation. Furthermore, it is highly possible that FTY720 enhances gene expression of adCTLA4Ig, which may be related to the long-term acceptance of grafts.
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页码:391 / 398
页数:7
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