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甘露糖结合凝集素与异基因造血干细胞移植后的感染

Mannose-binding lectin and infection following allogeneic hemopoietic stem cell transplantation.

作者信息

Mullighan Charles G, Bardy Peter G

机构信息

Division of Haematology, Institute of Medical and Veterinary Science, PO Box 14, Rundle Mall, Adelaide, SA, 5000 Australia.

出版信息

Leuk Lymphoma. 2004 Feb;45(2):247-56. doi: 10.1080/1042819031000146983.

Abstract

Major infection remains a major barrier to the success of allogeneic hemopoietic stem cell transplantation (SCT). There is growing interest in the importance of innate immunity in host defense, particularly when adaptive immunity is compromised. Furthermore, many host defense genes are polymorphic, and immunogenetic factors are known to influence the risk of other transplant complications, such as graft-versus-host disease. Mannose-binding lectin (MBL) has emerged as an important innate host defense molecule. MBL binds a wide range of pathogens independently of antibody and activates complement leading to lysis and phagocytosis. Genetically determined MBL deficiency is common and results in an increased risk of infection in a variety of clinical settings, especially in individuals already immunocompromised for other reasons. We conducted a retrospective study examining associations between polymorphisms in the gene encoding MBL, MBL2 and risk of major infection post-SCT in 96 related myeloablative transplants. This showed that "low-producing" MBL2 coding alleles, when present in the donor, were significantly associated with increased risk of major infection in the recipient following neutrophil count recovery. Furthermore, a "high-producing" MBL2 haplotype, HYA, when present in the recipient, was protective against infection. As MBL is under development as a therapeutic agent, these findings suggest that administration of MBL may reduce the risk of infection post-transplant. Prior to embarking upon trials of MBL replacement therapy in SCT, further work is required to confirm these results, to examine the kinetics of MBL synthesis peri-transplant, to correlate MBL2 genotype with blood MBL levels, and to examine the role of MBL in other settings, such as transplantation using reduced intensity conditioning regimens, and unrelated donor transplants. These results are the first report of a genetic determinant of risk of infection post-SCT, and highlight the importance of non-HLA genetic factors in determining the risk of transplant complications. Further studies examining other host defence genes are warranted, and are in progress.

摘要

严重感染仍然是异基因造血干细胞移植(SCT)成功的主要障碍。宿主防御中固有免疫的重要性日益受到关注,尤其是在适应性免疫受损时。此外,许多宿主防御基因具有多态性,已知免疫遗传因素会影响其他移植并发症的风险,如移植物抗宿主病。甘露糖结合凝集素(MBL)已成为一种重要的固有宿主防御分子。MBL可独立于抗体结合多种病原体并激活补体,导致病原体裂解和吞噬。基因决定的MBL缺陷很常见,会导致在各种临床情况下感染风险增加,尤其是在因其他原因已经免疫受损的个体中。我们进行了一项回顾性研究,检测了96例相关清髓性移植中,编码MBL的基因MBL2的多态性与SCT后严重感染风险之间的关联。结果显示,当供体存在“低产生”的MBL2编码等位基因时,中性粒细胞计数恢复后,受者发生严重感染的风险显著增加。此外,当受者存在“高产生”的MBL2单倍型HYA时,可预防感染。由于MBL正作为一种治疗药物进行研发,这些发现表明给予MBL可能会降低移植后感染风险。在开展SCT中MBL替代疗法的试验之前,需要进一步开展工作以确认这些结果,检测移植前后MBL合成的动力学,将MBL2基因型与血液MBL水平相关联,并检测MBL在其他情况下的作用,如使用减低剂量预处理方案的移植和无关供体移植。这些结果是关于SCT后感染风险遗传决定因素的首次报告,并突出了非HLA遗传因素在确定移植并发症风险中的重要性。有必要对其他宿主防御基因进行进一步研究,相关研究正在进行中。

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