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[角膜移植术后通过CTLA4-Ig和抗CD154抗体进行的免疫调节]

[Immunomodulation after keratoplasty by CTL4-Ig and anti-CD154 antibodies].

作者信息

Zhang E P, Bulfone-Paus S, Hoffmann F

机构信息

Universitätsklinikum Benjamin Franklin, Augenklinik, Berlin.

出版信息

Ophthalmologe. 2002 Mar;99(3):183-7. doi: 10.1007/s003470100482.

Abstract

BACKGROUND

The immunoreaction after corneal transplantation is caused by the T cell receptor interacting with the major histocompatibility complex (MHC) receptor of the antigen-presenting cell. The signal is amplified by the CD4 receptor and the costimulatory signal interactions of CD28-B7 and CD40-CD154. We investigated the influence of costimulatory signal blocking on corneal transplant survival in mice.

METHODS

Seven groups of 6 BALB/c mice received an orthotopic corneal transplant from C3H mice differing in minor and major MHC and were postoperatively treated as follows: (1) 80 micrograms of CTLA4 fusion protein intraperitoneally (i.p.) for 6 days; (2) 50 microliters of PBS i.p. for 6 days; (3) 1 mg of Solu-Decortin H i.p. for 5 days + dexamethasone AT 0.1% for 35 days; (4) therapy (3) + 50 micrograms of CTLA4 fusion protein i.p. for 6 days; (5) CTLA4-Ig as in (1) + 15 micrograms of anti-CD154 subconjunctivally (s.c.) on days 0, 2, 4, 6, and 8; (6) CTLA4-Ig as in (1) + 25 micrograms of anti-CD154 s.c. for 9 days; and (7) 25 microliters of PBS s.c. for 9 days.

RESULTS

All animals had an immunoreaction on the following days: (1) day 18 +/- 3.1; (2) day 13.6 +/- 1.6; (3) day 48 +/- 6.6; (4) day 65 +/- 41; (5) day 23.5 +/- 8.5; (6) day 16.2 +/- 3.6; (7) day 13.8 +/- 2.7.

CONCLUSION

The significant prolongation of transplant survival achieved by corticosteroids alone (P < 0.001) is again significantly increased by combining them with CTLA4-Ig (P < 0.001). Specific immunotherapy combined with nonspecific steroid therapy may also improve clinical corneal transplantation results. Compared to the two control groups, CTLA4-Ig and anti-CD154 only influenced transplant survival at a low dosage (P < 0.001).

摘要

背景

角膜移植后的免疫反应是由T细胞受体与抗原呈递细胞的主要组织相容性复合体(MHC)受体相互作用引起的。该信号通过CD4受体以及CD28 - B7和CD40 - CD154的共刺激信号相互作用而放大。我们研究了共刺激信号阻断对小鼠角膜移植存活的影响。

方法

将7组每组6只BALB/c小鼠接受来自C3H小鼠的原位角膜移植,C3H小鼠在次要和主要MHC方面存在差异,术后治疗如下:(1)腹腔内注射80微克CTLA4融合蛋白,共6天;(2)腹腔内注射50微升PBS,共6天;(3)腹腔内注射1毫克氢化可的松琥珀酸钠,共5天 + 0.1%地塞米松,共35天;(4)治疗方案(3) + 腹腔内注射50微克CTLA4融合蛋白,共6天;(5)如(1)所述的CTLA4 - Ig + 在第0、2、4、6和8天结膜下注射15微克抗CD154;(6)如(1)所述的CTLA4 - Ig + 结膜下注射25微克抗CD154,共9天;(7)结膜下注射25微升PBS,共9天。

结果

所有动物在以下天数出现免疫反应:(1)第18±3.1天;(2)第13.6±1.6天;(3)第48±6.6天;(4)第65±41天;(5)第23.5±8.5天;(6)第16.2±3.6天;(7)第13.8±2.7天。

结论

单独使用皮质类固醇显著延长移植存活时间(P < 0.001),将其与CTLA4 - Ig联合使用后存活时间再次显著延长(P < 0.001)。特异性免疫疗法与非特异性类固醇疗法联合使用也可能改善临床角膜移植结果。与两个对照组相比,CTLA4 - Ig和抗CD154仅在低剂量时影响移植存活(P < 0.001)。

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