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Transient increase of serum IgD levels after allogeneic bone-marrow transplantation.

机译:同种异体骨髓移植后血清IgD水平的短暂升高。

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摘要

Serum IgD levels were followed longitudinally twice a week for up to 100 days in 60 children undergoing allogeneic bone-marrow transplantation (n = 52) or immunosuppression (n = 8) for the treatment of leukaemia, severe aplastic anaemia or severe combined immunodeficiency. In 40 out of the 49 post-transplantation periods analysed (82%), a transient sharp increase of serum IgD was detected, irrespective of initial disease. A similar peak was found in one out of five children after immunosuppressive treatment. A second IgD peak was only recorded in grafted patients (14/49 post-transfusion periods). Peak levels of IgD ranged from 1.3 to 185.7 IU/ml (median 12.2 IU/ml), which represents a 2.6 to 22.4-fold increase over 'baseline' levels. In the transplanted leukaemia and aplastic anaemia patients, the rise of serum IgD occurred at the same time (geometric mean 16 days after transplantation) and was shown to represent heterogeneous polyclonal IgD in six of them. The onset of the serum IgD peak was significantly delayed in children suffering from severe combined immunodeficiency (P less than 0.05) and was demonstrated in one patient to consist of homogeneous IgD. No relation was found between either the occurrence of clinical acute graft-versus-host disease or infections after treatment, and the time of onset of IgD elevations. To detect transient serum IgD peaks as described here, frequent sampling of sera is necessary. The origin of the early IgD peaks seems to reside within the recipient's cells by an unknown mechanism. The late IgD peaks are most probably an expression of gradual reconstitution of the immune system following bone-marrow transplantation.
机译:在60名接受同种异体骨髓移植(n = 52)或免疫抑制(n = 8)治疗白血病,严重再生障碍性贫血或严重合并免疫缺陷的儿童中,每周两次纵向监测血清IgD水平,长达100天。在所分析的49个移植后时期中,有40个(82%)检测到了血清IgD的瞬时急剧升高,而与最初的疾病无关。免疫抑制治疗后五分之一的儿童中发现了相似的峰值。仅在移植患者中记录了第二个IgD峰值(输血后14/49)。 IgD的峰值水平为1.3至185.7 IU / ml(中位数为12.2 IU / ml),比“基线”水平提高了2.6至22.4倍。在移植的白血病和再生障碍性贫血患者中,血清IgD的升高同时发生(移植后16天的几何平均数),并且在其中的6个中表现出异质的多克隆IgD。患有严重合并免疫缺陷的儿童血清IgD峰值的发作显着延迟(P小于0.05),并在一名患者中证实为均质IgD。临床急性移植物抗宿主病的发生或治疗后感染与IgD升高发作时间之间没有关系。如此处所述,要检测短暂的血清IgD峰值,需要频繁采样血清。早期IgD高峰的起源似乎是通过未知机制位于受体细胞内。 IgD晚期峰很可能是骨髓移植后免疫系统逐渐重建的一种表达。

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