首页> 美国卫生研究院文献>British Journal of Cancer >Effective mobilisation of peripheral blood progenitor cells with Dexa-BEAM and G-CSF: timing of harvesting and composition of the leukapheresis product.
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Effective mobilisation of peripheral blood progenitor cells with Dexa-BEAM and G-CSF: timing of harvesting and composition of the leukapheresis product.

机译:用 Dexa-BEAM和G-CSF有效地动员外周血祖细胞:白细胞分离术产品的采集时机和组成。

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摘要

The mini-BEAM regimen (BCNU, etoposide, cytarabine, melphalan) and its modification 'Dexa-BEAM' are effective salvage protocols for relapsed Hodgkin's disease and non-Hodgkin's lymphoma. Since many patients with relapsed lymphoma are eligible for high-dose chemotherapy with autologous stem cell rescue, we were interested in the suitability of these second line regimens for mobilising peripheral blood progenitor cells (PBPC). The kinetics of PBPC were studied in 15 patients treated with Dexa-BEAM and granulocyte colony-stimulating factor (G-CSF). Leukocytes started to rise from < 0.5 nL-1 on day 18 (16-22) after Dexa-BEAM, and exceeded 10 nL-1 on day 20 (18-28). Peripheral blood CFU-GM peaked on day 21 (19-28) and declined slowly thereafter; the median leukocyte count was 18.7 nL-1 (12.2-60) on the day of CFU-GM-peak. The maximum number of CFU-GM circulating in peripheral blood was inversely correlated to the duration of leukopenia after Dexa-BEAM. Measurement of CD34+ cells with the monoclonal antibody 8G12-PE (HPCA-2) predicted the number of CFU-GM precisely in both peripheral blood and leukapheresis products (r = 0.90-0.95). Two to six leukapheresis procedures yielded 6.39 x 10(8) mononuclear cells kg-1 (1.82-13.49) containing 44.4 x 10(4) CFU-GM kg-1 (2.2-213.8). Immunophenotypical analysis revealed that the percentage of CD19+ B cells was very low in all collection products (less than 1%). Nine patients were autografted with PBPC (15.4-213.8 x 10(4) CFU-GM kg-1) after myeloablative chemotherapy and experienced rapid and sustained engraftment (Platelets > 50 nL-1 on day +13 [9-22]). We conclude that PBPC can be mobilised effectively by Dexa-BEAM plus G-CSF. An adequate timing of PBPC collection (when the leukocyte count has exceeded 10 nL-1) and evaluation of the progenitor content of the leukapheresis products with 8G12-PE will allow to minimise the number of leukaphereses.
机译:mini-BEAM方案(BCNU,依托泊苷,阿糖胞苷,美法仑)及其修饰的“ Dexa-BEAM”是复发性霍奇金病和非霍奇金淋巴瘤的有效挽救方案。由于许多复发性淋巴瘤患者都有资格进行自体干细胞抢救的大剂量化疗,因此我们对这些二线方案对动员外周血祖细胞(PBPC)的适用性感兴趣。在Dexa-BEAM和粒细胞集落刺激因子(G-CSF)治疗的15例患者中研究了PBPC的动力学。 Dexa-BEAM后第18天(16-22),白细胞从<0.5 nL-1开始上升,并在第20天(18-28)超过10 nL-1。外周血CFU-GM在第21天(19-28)达到峰值,此后缓慢下降。在CFU-GM高峰日,白细胞计数中位数为18.7 nL-1(12.2-60)。外周血中循环的CFU-GM的最大数量与Dexa-BEAM后白细胞减少的持续时间成反比。用单克隆抗体8G12-PE(HPCA-2)测量CD34 +细胞可准确预测外周血和白细胞分离产物中CFU-GM的数量(r = 0.90-0.95)。两到六个白细胞去除程序产生了6.39 x 10(8)个单核细胞kg-1(1.82-13.49),其中包含44.4 x 10(4)CFU-GM kg-1(2.2-213.8)。免疫表型分析显示,所有收集产品中CD19 + B细胞的百分比都非常低(不到1%)。九名患者在清髓性化学疗法后自体移植了PBPC(15.4-213.8 x 10(4)CFU-GM kg-1),并经历了快速而持续的移植(第13天时血小板> 50 nL-1 [9-22])。我们得出结论,Dexa-BEAM加G-CSF可以有效地调动PBPC。 PBPC收集的适当时机(当白细胞计数超过10 nL-1时),并用8G12-PE评估白细胞分离产物的祖细胞含量,将使白细胞减少。

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