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首页> 外文期刊>Cornea >Mechanisms of corneal graft rejection: the sixth annual Thygeson Lecture, presented at the Ocular Microbiology and Immunology Group meeting, October 21, 2000.
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Mechanisms of corneal graft rejection: the sixth annual Thygeson Lecture, presented at the Ocular Microbiology and Immunology Group meeting, October 21, 2000.

机译:角膜移植排斥的机制:第六届年度Thygeson讲座,于2000年10月21日在眼部微生物学和免疫学小组会议上发表。

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The history of corneal transplantation reaches back over 150 years. Kissam performed one of the first penetrating keratoplasties when he transplanted a pig cornea onto a human in 1838. Only two interrupted sutures were used, and the surgery was performed without anesthesia! In retrospect, no one would be surprised to learn that the porcine corneal xenograft was rejected. Thirty years later, May transplanted rabbit corneal grafts to humans, but concluded that the failures in the first 24 attempts were the result of "imperfect technique and the inability to keep the eyes properly bandaged." The first documented report of a successful penetrating keratoplasty in a human subject was performed by Zirm in 1905. As we enter the new millennium, corneal transplantation remains the oldest, most common, and, arguably, the most successful form of solid tissue transplantation. In the United States alone, approximately 36,000 corneal transplants are performed each year. The success rate for corneal transplants is in excess of 90% in uncomplicated cases, even though HLA tissue typing is not performed and systemic immunosuppressive drugs are not administered. In spite of this extraordinary success, immune rejection remains the leading cause of corneal graft failure. Many inferences about the immunobiology of corneal graft rejection have been based on clinical observations; however, confirmation of these hypotheses requires prospective studies under controlled settings. The prudent use of animal models has fostered analytic studies on the immunobiology of corneal allografts without the complicating and confounding effects of topical steroids that are typically used on most keratoplasty patients. Although animal models of penetrating keratoplasty have been in use for almost a half-century, until recently, progress in understanding the immune mechanisms of corneal graft rejection has been slow. However, the widespread use of rodent models of orthotopic corneal transplantation has shed new light on the pathogenesis of corneal graft rejection.
机译:角膜移植的历史可以追溯到150年前。基桑在1838年将猪角膜移植到人身上时进行了最早的穿透性角膜移植手术之一。仅使用了两根间断的缝合线,而且该手术无需麻醉!回想起来,没有人会惊讶地发现猪角膜异种移植被拒绝了。 30年后,May将兔角膜移植物移植到人类身上,但得出的结论是,前24次尝试均失败是“技术不完善和无法正确包扎眼睛的结果”。 Zirm于1905年首次完成了在人类受试者中成功进行角膜移植手术的书面报告。随着新千年的到来,角膜移植仍是最古老,最常见也是最成功的实体组织移植形式。仅在美国,每年就进行约36,000例角膜移植。即使不进行HLA组织分型并且不使用全身性免疫抑制药物,在简单情况下角膜移植的成功率也超过90%。尽管取得了巨大成功,但免疫排斥仍然是角膜移植失败的主要原因。关于角膜移植排斥反应的免疫生物学的许多推论都是基于临床观察。但是,要确认这些假设,就需要在受控条件下进行前瞻性研究。动物模型的审慎使用促进了对角膜同种异体移植物免疫生物学分析的研究,而没有通常在大多数角膜移植患者中使用的局部类固醇的复杂和混杂作用。尽管穿透性角膜移植的动物模型已经使用了近半个世纪,但直到最近,人们对角膜移植排斥反应的免疫机制的了解仍很缓慢。然而,原位角膜移植的啮齿动物模型的广泛使用为角膜移植排斥反应的发病机理提供了新的思路。

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