Shi Weiyun, Chen Min, Xie Lixin
State Key Laboratory Cultivation Base, Shandong Provincial Key Laboratory of Ophthalmology, Shandong Eye Institute, Qingdao, China.
Graefes Arch Clin Exp Ophthalmol. 2007 Nov;245(11):1691-7. doi: 10.1007/s00417-007-0606-5. Epub 2007 May 31.
To investigate the therapeutic effect of CTLA4-FasL-B7 costimulatory pathway blockage-on graft survival in a murine model of corneal transplantation.
Orthotopic penetrating keratoplasty was performed on BALB/c mice. The mice were randomized into four groups: the isograft group, untreated allograft group, cyclosporine A drug delivery system (CsA DDS)-anterior chamber implanted group, and 10 microg/mL CTLA4-FasL-treated group. Allografts were from C57BL/6 mice. Survival time of corneal grafts was evaluated. Immunohistological method and TdT-mediated dUTP Nick End Labeling (TUNEL) were applied for the detection of CD4+ T cells and apoptotic cells in corneal transplants. To assess whether peripheral immune tolerance appeared after the treatment of CTLA4-FasL, CsA DDS-implanted- and CTLA4-FasL-treated BALB/c mice with clear grafts received skin allografts at 4 weeks after keratoplasty, and the status of corneal transplants were observed when skin grafts were rejected.
Allografts in the CTLA4-FasL group (median survival time [MST] = 106 days, p = 0.0042) and the CsA DDS group (MST = 60 days, p = 0.0037) revealed extending survival time, compared with that in the untreated allograft group (MST = 14 days). There were significantly fewer CD4-positive T cells in both the isograft group and the CsA DDS group. In the untreated allograft group, the number of CD4+ T cells gradually increased from day 1 until the final day of observation (day 21). By contrast, it reached a peak on day 7 and then absolutely reduced in the CTLA4-FasL group. Many apoptotic cells were detected on day 7 in the CTLA4-FasL group, but very few were seen in the other groups. Within 30 days of skin-graft rejection, previously healthy and long-standing corneal grafts became rejected in the CsA DDS group but remained clear in the CTLA4-FasL group.
CTLA4-FasL can prolong the survival time of corneal allografts in mice, exerting a negative regulation on T-cell activation simultaneously by blocking B7 costimulatory signals and inducing Fas-FasL apoptotic pathway. Due to the adjunctive role of FasL, it also appears to be a potential activity of tolerance induction through T-cell apoptotic pathways.
探讨CTLA4 - FasL - B7共刺激通路阻断对小鼠角膜移植模型中移植物存活的治疗效果。
对BALB/c小鼠进行原位穿透性角膜移植。将小鼠随机分为四组:同基因移植组、未治疗的同种异体移植组、环孢素A药物递送系统(CsA DDS)前房植入组和10μg/mL CTLA4 - FasL治疗组。同种异体移植物来自C57BL/6小鼠。评估角膜移植物的存活时间。采用免疫组织学方法和TdT介导的dUTP缺口末端标记法(TUNEL)检测角膜移植片中的CD4 + T细胞和凋亡细胞。为了评估CTLA4 - FasL治疗后是否出现外周免疫耐受,角膜移植术后4周,对角膜移植片清晰的CsA DDS植入组和CTLA4 - FasL治疗组的BALB/c小鼠进行皮肤同种异体移植,并在皮肤移植物排斥时观察角膜移植片的状态。
与未治疗的同种异体移植组(中位存活时间[MST] = 14天)相比,CTLA4 - FasL组(MST = 1〇6天,P = 0.0042)和CsA DDS组(MST = 60天,P = 0.0037)的同种异体移植物存活时间延长。同基因移植组和CsA DDS组中CD4阳性T细胞明显较少。在未治疗的同种异体移植组中,从第1天到观察的最后一天(第21天),CD4 + T细胞数量逐渐增加。相比之下,在CTLA4 - FasL组中,其在第7天达到峰值,然后绝对减少。CTLA4 - FasL组在第7天检测到许多凋亡细胞,而其他组中很少见到。在皮肤移植物排斥的30天内,CsA DDS组中先前健康且长期存在的角膜移植物被排斥,但CTLA4 - FasL组中的角膜移植物仍保持清晰。
CTLA4 - FasL可延长小鼠角膜同种异体移植物的存活时间,通过阻断B7共刺激信号并诱导Fas - FasL凋亡途径同时对T细胞活化发挥负调控作用。由于FasL的辅助作用,它似乎还具有通过T细胞凋亡途径诱导耐受的潜在活性。