Meldgaard Knudsen L, Jensen L, Jarlbaek L, Hansen P G, Hansen S W, Drivsholm L, Nikolaisen K, Gaarsdal E, Johnsen H E
Department of Haematology L, Herlev Hospital, University of Copenhagen, DK - 2730 Herlev, Denmark.
Haematologica. 1999 Jun;84(6):517-24.
Randomized clinical trials have shown that peripheral blood stem cell transplantations (PBSCT) with appropriate doses of CD34+ cells are associated with rapid, complete and sustained recovery of marrow functions. Nevertheless, in a minority af patients delayed platelet recovery may occur and it remains to be established whether analysis of transplanted CD34+ cell subsets may demonstrate correlation with this phenomenon. We studied a series of 80 consecutive transplanted patients with the aim of evaluating the effect of CD34+ stem cell numbers and, in a subgroup of 32 patients, the effect of the lineage specific subset numbers on time to platelet engraftment (i.e. time to platelet counts higher than 20x10(9)/L for two consecutive days without the need for platelet transfusions).
Different clinical and paraclinical factors were examined in a multivariate analysis for effect on platelet engraftment in 80 patients.
The number of CD34+ cells/kg infused was the most important factor predicting the time to platelet engraftment. Patients receiving more than 10x10(6) CD34+ cells/kg had prompt platelet engraftment. The majority of the patients (78%) received fewer than 10x10(3) CD34+ cells/kg and 17/62 (27%) of these patients experienced delayed platelet engraftment. In 32 patients receiving fewer than 10x10(6) CD34+ cells/kg we focused on the content of different lineage specific CD34+ subsets in the PBSC products. The most significant correlation was recognized for CD34+/CD61+ megakaryocytic cell number and platelet engraftment. An inverse correlation between the CD34+/CD38Eth subset and platelet engraftment was found, indicating that a high number of CD34+/CD38Eth in the PBSC product might increase the risk for delayed engraftment. These results were further confirmed by the observation that patients who experienced platelet engraftment after day 20 had significantly more CD34+/CD38Eth cells/kg infused than patients with fast engraftment.
The number of total CD34+ cells/kg infused was the most important factor predicting time to platelet engraftment. CD34+ subset analysis in a subgroup of patients suggests that a high number of uncommitted progenitors may be associated with slower platelet recovery than transplantation with a higher fraction of more committed peripheral blood stem cells.
随机临床试验表明,给予适当剂量的CD34+细胞进行外周血干细胞移植(PBSCT)与骨髓功能快速、完全且持续的恢复相关。然而,少数患者可能会出现血小板恢复延迟的情况,移植的CD34+细胞亚群分析是否与这一现象相关仍有待确定。我们研究了连续80例移植患者,旨在评估CD34+干细胞数量的影响,并且在32例患者的亚组中,评估谱系特异性亚群数量对血小板植入时间(即血小板计数连续两天高于20×10⁹/L且无需血小板输注的时间)的影响。
在一项多变量分析中检查了80例患者中不同的临床和临床旁因素对血小板植入的影响。
每千克输注的CD34+细胞数量是预测血小板植入时间的最重要因素。接受超过10×10⁶个CD34+细胞/千克的患者血小板植入迅速。大多数患者(78%)接受的CD34+细胞少于10×10³个/千克,其中17/62(27%)的患者出现血小板植入延迟。在32例接受少于10×10⁶个CD34+细胞/千克的患者中,我们关注了PBSC产品中不同谱系特异性CD34+亚群的含量。CD34+/CD61+巨核细胞数量与血小板植入的相关性最为显著。发现CD34+/CD38Eth亚群与血小板植入呈负相关,这表明PBSC产品中大量的CD34+/CD38Eth可能会增加植入延迟的风险。在第20天之后出现血小板植入的患者比植入迅速的患者每千克输注的CD34+/CD38Eth细胞明显更多,这一观察结果进一步证实了这些结果。
每千克输注的总CD34+细胞数量是预测血小板植入时间的最重要因素。对患者亚组的CD34+亚群分析表明,与移植更多比例的更定向的外周血干细胞相比,大量未定向祖细胞可能与血小板恢复较慢有关。
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