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同种异体角膜内皮细胞移植的小鼠模型

A mouse model of allogeneic corneal endothelial cell transplantation.

作者信息

Hayashi Takahiko, Yamagami Satoru, Tanaka Kazumi, Yokoo Seiichi, Usui Tomohiko, Amano Shiro, Mizuki Nobuhisa

机构信息

Department of Ophthalmology, Yokohama City University School of Medicine, Yokohama, Kanagawa, Japan.

出版信息

Cornea. 2008 Jul;27(6):699-705. doi: 10.1097/QAI.0b013e31815e722b.

DOI:10.1097/QAI.0b013e31815e722b
PMID:18580263
Abstract

PURPOSE

Corneal endothelial cell (CEC) transplantation should become clinically applicable in the near future. However, the immunologic changes after allo-CEC transplantation are poorly understood at present. We tried to establish a mouse model of allogeneic CEC transplantation for immunologic studies.

METHODS

Benzalkonium chloride was injected into the anterior chamber of the eyes of recipient BALB/c mice to create bullous keratopathy. Full-thickness corneal transplantation was performed by using 4 types of corneas: BALB/c corneas (isograft group), BALB/c corneas denuded of CEC (no endothelium group), C3H/He mouse corneas (allograft group), and corneas reconstituted by seeding immortalized C3H/He mouse CECs onto BALB/c corneas denuded of endothelium (CEC allograft group). Eyes were observed with an operating microscope for 4 weeks after transplantation and were subjected to histologic examination and fluorescein microscopy.

RESULTS

All corneal grafts were transparent in the isograft group (n = 12), whereas none of the grafts were clear by 4 weeks after transplantation in the no endothelium group (n = 13). Corneal grafts were transparent at 4 weeks in 75% of the CEC allograft group (n = 12). The histologic rejection rate was 0% in the CEC allograft group, which was significantly lower than in the allograft group (67%; n = 18; P < 0.01).

CONCLUSIONS

We established a mouse allo-CEC transplantation model by using cultured cells. This model should be useful for studying the immunologic processes after CEC transplantation.

摘要

目的

角膜内皮细胞(CEC)移植在不久的将来应会在临床上得到应用。然而,目前对同种异体CEC移植后的免疫变化了解甚少。我们试图建立一种用于免疫研究的同种异体CEC移植小鼠模型。

方法

将苯扎氯铵注入受体BALB/c小鼠的眼前房以造成大泡性角膜病变。使用4种类型的角膜进行全层角膜移植:BALB/c角膜(同基因移植组)、去除CEC的BALB/c角膜(无内皮组)、C3H/He小鼠角膜(同种异体移植组)以及将永生化C3H/He小鼠CEC接种到去除内皮的BALB/c角膜上重构的角膜(CEC同种异体移植组)。移植后用手术显微镜观察眼睛4周,并进行组织学检查和荧光素显微镜检查。

结果

同基因移植组(n = 12)的所有角膜移植片均透明,而无内皮组(n = 13)在移植后4周时所有移植片均不透明。CEC同种异体移植组(n = 12)在4周时75%的角膜移植片透明。CEC同种异体移植组的组织学排斥率为0%,显著低于同种异体移植组(67%;n = 18;P < 0.01)。

结论

我们利用培养细胞建立了小鼠同种异体CEC移植模型。该模型应有助于研究CEC移植后的免疫过程。

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A mouse model of allogeneic corneal endothelial cell transplantation.同种异体角膜内皮细胞移植的小鼠模型
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Necessary prone position time for human corneal endothelial precursor transplantation in a rabbit endothelial deficiency model.兔角膜内皮细胞缺乏模型中人类角膜内皮前体细胞移植所需的俯卧位时间。
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