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[雷帕霉素持续给药系统预防兔高危角膜移植排斥反应及新生血管形成]

[Sustained rapamycin drug delivery system in prevention of high risk corneal allograft rejection and neovascularization in rabbits].

作者信息

Gao Hua, Shi Wei-yun, Xie Li-xin, Wang Shen-guo

机构信息

Shangdong Eye Institute, Qingdao 266071, China.

出版信息

Zhonghua Yan Ke Za Zhi. 2006 Jan;42(1):6-11.

PMID:16638273
Abstract

OBJECTIVE

To evaluate the immunosuppressive and antiangiogenesis effects of rapamycin drug delivery system (RAPA DDS) in high risk rabbit model of penetrating keratoplasty (PK).

METHODS

(1) RAPA DDS preparation: 50 mg of PGLC and 50 mg of RAPA were mixed as a RAPA drug delivery system. (2) High risk rabbit model: Corneal vascularization was induced in 45 New Zealand white rabbits (45 eyes) by passing 5 - 0 silk sutures in corneal stroma in each quadrant. (3) 40 rabbits with corneal neovascularization beyond three quadrants were received a unilateral 7 mm diameter central PK. The 40 were divided into four treatment groups: Group A, control group and received no therapy; Group B, 1 mg PGLC carrier was implanted in the anterior chamber; Group C, 1% RAPA eye drops was applied four times daily; Group D, 0.5 mg RAPA DDS was implanted in the anterior chamber. (4) Postoperative examination: The cornea allografts (opacity, edema and neovascularization) were examined by the slit-lamp biomicroscopy for ninety days. Rejection index (RI) and neovascularization index (NI) of these animal models were recorded. RAPA concentration in the aqueous humor was detected on 2, 4, 8 and 12 weeks in group C and D after surgery; the expressions of IL-2R, MCP-1, Fas/FasL in samples were detected with in situ hybridization; TNF-alpha and VEGF were detected with immuno-histochemical technique three weeks after the operation in all groups. Histochemical method was carried out on the procured specimens of cornea, retina, liver and kidney at ninety days.

RESULTS

(1) Allografts rejection: Mean survival times in 4 trial groups were (16.5 +/- 2.5), (16.0 +/- 2.6), (47.1 +/- 13.2), (87.6 +/- 5.8) d respectively (P = 0.000). (2) Corneal neovascularization: Mean NI was 2.4 +/- 0.7, 2.1 +/- 0.5, 0.6 +/- 0.5, 0.3 +/- 0.5 (P = 0.000) 2 weeks after the operation, and the NI value was 3.8 +/- 0.5, 3.8 +/- 0.4, 0.8 +/- 0.7, 0.4 +/- 0.8 (P = 0.000) 12 weeks after the operation in groups A, B, C and D respectively. (3) RAPA concentration in aqueous humor: Mean RAPA concentration in aqueous humor was 10.7, 12.0, 9.2, 7.0 ng/ml in group D in the 2, 4, 8 and 12 weeks after the operation respectively. RAPA can not be detected in group C. (4) Cytokine expression: IL-2R, MCP-1, TNF-alpha and VEGF were overexpression in group A and B, and undetectable in group C and D. Fas and FasL were negative in all groups. (5) No inflammatory cell infiltration was found in retina, liver and kidney tissue ninety days after the surgery.

CONCLUSIONS

Sustained RAPA DDS and eyedrops can prolong allograft survival and inhibit cornea neovascularization in rabbit model. However, RAPA DDS is better than eyedrops.

摘要

目的

评估雷帕霉素给药系统(RAPA DDS)在穿透性角膜移植术(PK)高风险兔模型中的免疫抑制和抗血管生成作用。

方法

(1)RAPA DDS制备:将50 mg聚谷氨酸苄酯(PGLC)与50 mg雷帕霉素混合制成RAPA给药系统。(2)高风险兔模型:对45只新西兰白兔(45只眼),通过在角膜基质的每个象限穿过5-0丝线诱导角膜血管化。(3)40只角膜新生血管超过三个象限的兔子接受单侧直径7 mm的中央PK。这40只兔子分为四个治疗组:A组为对照组,不接受治疗;B组,将1 mg PGLC载体植入前房;C组,每天4次应用1%雷帕霉素滴眼液;D组,将0.5 mg RAPA DDS植入前房。(4)术后检查:用裂隙灯显微镜检查角膜移植片(混浊、水肿和新生血管)90天。记录这些动物模型的排斥指数(RI)和新生血管指数(NI)。术后第2、4、8和12周检测C组和D组房水中雷帕霉素浓度;用原位杂交检测样本中IL-2R、MCP-1、Fas/FasL的表达;术后3周用免疫组织化学技术检测所有组中的TNF-α和VEGF。术后90天对获取的角膜、视网膜、肝脏和肾脏标本进行组织化学方法检测。

结果

(1)同种异体移植排斥:4个试验组的平均存活时间分别为(16.5±2.5)、(16.0±2.6)(47.1±13.2)、(87.6±5.8)天(P = 0.000)。(2)角膜新生血管:术后2周,A、B、C、D组的平均NI分别为2.4±0.7、2.1±0.5、0.6±0.5、0.3±0.5(P = 0.……

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