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肝脏临床异种移植的未来何在?

[What future for clinical xenograft of the liver?].

作者信息

Meriggi F, Forni E, Bismuth H

机构信息

Clinica Chirurgica Generale, Università degli Studi di Pavia.

出版信息

G Chir. 1994 Apr;15(4):183-9.

PMID:8086309
Abstract

In the cyclosporine era liver orthotopic allotransplantation has shown to be very effective in the treatment of many end-stage liver diseases. Currently, the major limitation in clinical transplantation is the shortage of donor organs unlikely solvable by alternative policies or approaches such as living donors and artificial organs. Animals have been considered as an alternative source of organs offering the following advantages: availability of a predictable and ready supply of donor organs, opportunity to practice transplantation as an elective procedure, possibility to match the size of the graft recipient. However, immunologic barriers are thought to make xenotransplantation impractical between widely divergent (discordant) species. Hyperacute xenograft rejection, in fact, consists of an immediate, diffuse intravascular coagulopathy followed by an aggressive cellular reaction. Recipient preformed natural antibodies and complement are involved in the humoral phase of hyperacute rejection. The violence of this reaction depends on the titer of natural antibodies and on the divergency of the species involved. Species more closely related (concordant) exhibit a less aggressive reaction characterized by an acute cellular rejection. Hepatic allografts and xenografts, though, are unusually resistant to humoral injury and undergo a combination of both humoral and cellular rejection. Preliminary studies have demonstrated a prolonged reduction in natural antibodies accomplished by plasmapheresis and cyclophosphamide combined treatment. Furthermore, new therapeutic agents such as FK 506, rapamycin and deoxyspergualin may find widespread application in clinical transplantation. FK 506 has shown to possess a remarkable efficacy in reversing refractory hepatic allograft rejection as well as ability to inhibit humorally mediated immunity.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在环孢素时代,原位肝同种异体移植已被证明在治疗许多终末期肝病方面非常有效。目前,临床移植的主要限制是供体器官短缺,不太可能通过活体供体和人工器官等替代政策或方法来解决。动物已被视为器官的替代来源,具有以下优点:可获得可预测且现成的供体器官供应,有机会将移植作为一种选择性手术进行实践,有可能使移植物与受体的大小相匹配。然而,免疫屏障被认为使得在差异很大(不匹配)的物种之间进行异种移植不切实际。事实上,超急性异种移植排斥反应包括立即发生的弥漫性血管内凝血,随后是强烈的细胞反应。受体预先形成的天然抗体和补体参与超急性排斥反应的体液阶段。这种反应的剧烈程度取决于天然抗体的滴度和所涉及物种的差异程度。关系更密切(匹配)的物种表现出较弱的反应,其特征为急性细胞排斥反应。不过,肝同种异体移植和异种移植对体液损伤具有异常的抵抗力,会经历体液和细胞排斥反应的组合。初步研究表明,通过血浆置换和环磷酰胺联合治疗可使天然抗体水平长期降低。此外,新的治疗药物如FK 506、雷帕霉素和去氧精胍菌素可能会在临床移植中得到广泛应用。FK 506已显示出在逆转难治性肝同种异体移植排斥反应方面具有显著疗效,以及抑制体液介导免疫的能力。(摘要截选至250词)

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G Chir. 1994 Apr;15(4):183-9.
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