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首页> 外文期刊>Bone marrow transplantation >Autografting of highly purified peripheral blood progenitor cells following myeloablative therapy in patients with lymphoma: a prospective study of the long-term effects on tumor eradication, reconstitution of hematopoiesis and immune recovery.
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Autografting of highly purified peripheral blood progenitor cells following myeloablative therapy in patients with lymphoma: a prospective study of the long-term effects on tumor eradication, reconstitution of hematopoiesis and immune recovery.

机译:淋巴瘤患者清髓治疗后自体移植高度纯化的外周血祖细胞:对根除肿瘤,造血重建和免疫恢复的长期影响的前瞻性研究。

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In a prospective study, we have investigated CD34+ selection of peripheral blood progenitor cells (PBPC) for autotransplantation in patients with lymphoma. Twenty-six consecutive patients (10 follicular lymphomas, seven mantle cell lymphomas, seven B-CLL, two immunocytomas) were mobilized using chemotherapy plus G-CSF. Sufficient numbers of PBPC could be collected from 24 patients and were immunoselected with the semiautomated Isolex 300 (n = 17) or the fully integrated Isolex 300i (n = 7) devices. The selection products were assayed by PCR amplification of clonal CDRIII or t(14;18) rearrangements for residual tumor cell content. Residual disease and long-term hematopoietic and immune recovery were studied by assessing the following parameters at 3, 6, and 12 months post-transplant: CDRIII or t(14;18) PCR, platelet count, lymphocyte subsets, serum IgG, serum IgA, and measles titer. With the Isolex 300 device 26% (10-65) of input CD34+ cells were recovered with a median purity of 89.2% (49.4-98.9) after CD34+ selection. The Isolex 300i device allowed significantly better recoveries (46% (22-86)) and purities of CD34+ cells (98.8% (92.2-99.2)). The overall purging efficacy was 3.2 (0.6-5.1) log. Twenty patients have been reinfused with CD34+ selected grafts after myeloablative preparation. Rapid engraftment occurred in all patients. With a median follow-up of 28 (19-42) months, 14 patients are alive without clinical or molecular evidence of disease recurrence, whereas five have relapsed and one additional patient shows persistent presence of the disease-specific molecular marker without clinical progression. Cellular and serological parameters of hematopoietic and immune functions were largely normal at 12 months post-transplant including the measles titer which was present in all patients. Kinetics of immunohematopoietic recovery were similar to those of 12 control patients who had received unmanipulated PBPC during the same time period except for the recovery of CD4+ CD45RA+ T cells which was significantly delayed in the CD34+ group. During the first year post-transplant, transient monoclonal or oligoclonal gammopathies were observed in seven of 16 study patients. We conclude that CD34+ selection with the Isolex system allows preparation of highly purified CD34+ fractions and effective tumor cell depletion. The CD34+ products can be reinfused safely after myeloablative treatment and result in sustained hematopoietic and immune recovery. The fact that all patients retained their specific measles immunity suggests that myeloablative treatment with reinfusion of highly purified CD34+ PBPC is not immunoablative.
机译:在一项前瞻性研究中,我们研究了CD34 +选择用于淋巴瘤患者自体移植的外周血祖细胞(PBPC)。使用化学疗法加G-CSF调动了26例连续患者(10例滤泡性淋巴瘤,7例套细胞淋巴瘤,7例B-CLL,2例免疫细胞瘤)。可以从24位患者中收集到足够数量的PBPC,并使用半自动Isolex 300(n = 17)或完全集成的Isolex 300i(n = 7)设备进行免疫选择。选择产物通过克隆CDRIII或t(14; 18)重排的PCR扩增来测定残留肿瘤细胞含量。通过评估移植后3、6和12个月的以下参数研究残存疾病以及长期造血和免疫恢复:CDRIII或t(14; 18)PCR,血小板计数,淋巴细胞亚群,血清IgG,血清IgA和麻疹滴度。使用Isolex 300装置,选择CD34 +后,回收了26%(10-65)的输入CD34 +细胞,中位纯度为89.2%(49.4-98.9)。 Isolex 300i装置可显着提高回收率(46%(22-86))和CD34 +细胞纯度(98.8%(92.2-99.2))。总体清除效果为3.2(0.6-5.1)log。进行清髓准备后,已经向20位患者重新注入了CD34 +选择的移植物。所有患者均发生快速植入。中位随访期为28(19-42)个月,有14例患者存活,没有临床或分子证据表明疾病复发,而5例已经复发,另有1例患者显示疾病特异性分子标记物持续存在而无临床进展。造血和免疫功能的细胞和血清学参数在移植后12个月基本正常,包括所有患者中存在的麻疹滴度。免疫造血恢复的动力学与在同一时期接受未操作的PBPC的12例对照患者相似,但CD34 +组的CD4 + CD45RA + T细胞的恢复明显延迟。在移植后的第一年,在16位研究患者中有7位观察到了短暂的单克隆或寡克隆性同种病。我们得出的结论是,使用Isolex系统进行CD34 +选择可以制备高度纯化的CD34 +馏分并有效清除肿瘤细胞。 CD34 +产品可在清髓治疗后安全地重新输注,并导致持续的造血和免疫恢复。所有患者均保留了其特定的麻疹免疫力这一事实表明,重新输注高度纯化的CD34 + PBPC的清髓性治疗不是免疫性的。

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