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影响原始和定向造血祖细胞动员至癌症患者外周血的因素。

Factors affecting the mobilization of primitive and committed hematopoietic progenitors into the peripheral blood of cancer patients.

作者信息

Schneider J G, Crown J P, Wasserheit C, Kritz A, Wong G, Reich L, Norton L, Moore M A

机构信息

Memorial Sloan-Kettering Cancer Center, New York.

出版信息

Bone Marrow Transplant. 1994 Dec;14(6):877-84.

PMID:7536069
Abstract

Rapid hematopoietic reconstitution following peripheral blood progenitor cell (PBPC) autotransplantation is thought to result from reinfusion of committed progenitor cells. This has raised concern that PBPC autografts might be rich in committed hematopoietic progentors responsible for early engraftment, but deficient in more primitive progenitors required for long-term hematopoietic reconstitution. The granulomonocytic colony-forming unit (CFU-GM) assay measures committed progenitors responsive to a single species of colony-stimulating activity such as granulocyte-macrophage colony-stimulating factor (GM-CSF), whereas the pre-CFU assay identifies more primitive progenitors by measuring interleukin-3 (IL-3) and kit ligand (KL) induced generation of secondary CFU-GM from CD34+, 4-hydroperoxycyclophosphamide resistant progenitors that require multiple cytokine stimuli. Paired bone marrow (BM) and PBPC samples from 17 breast and ovarian cancer patients participating in four separate clinical trials were compared in these assay systems. In seven of nine patients, PBPC autografts mobilized with cyclophosphamide rebound and G-CSF compared favorably with paired BM autografts in both committed and primitive progenitor capacity. Failure to mobilize substantial primitive progenitor cell numbers occurred in two of nine patients undergoing this mobilization regimen and could not have been predicted by either circulating CFU-GM or CD34+ cell number. Prior myelosuppressive treatment experiences reduced peripheral progenitor yields somewhat, but still allowed for the collection of PBPC autografts which compared favorably with BM autografts in total CFU-GM and Pre-CFU. Mobilization of PBPC with G-CSF or GM-CSF alone in patients who had received prior myelosuppressive therapies produced autografts which were relatively deficient in committed progenitors, but absolutely deficient in primitive progenitors. We conclude that optimization of patient characteristics and mobilization parameters can achieve PBPC autografts rich in both the primitive and committed hematopoietic progenitor cells.

摘要

外周血祖细胞(PBPC)自体移植后快速的造血重建被认为是由定向祖细胞的回输所致。这引发了人们的担忧,即PBPC自体移植物可能富含负责早期植入的定向造血祖细胞,但缺乏长期造血重建所需的更原始祖细胞。粒细胞单核细胞集落形成单位(CFU-GM)测定法可测量对单一类型集落刺激活性(如粒细胞-巨噬细胞集落刺激因子(GM-CSF))有反应的定向祖细胞,而前CFU测定法则通过测量白细胞介素-3(IL-3)和干细胞因子(KL)诱导从需要多种细胞因子刺激的CD34+、4-氢过氧环磷酰胺抗性祖细胞产生次级CFU-GM来鉴定更原始的祖细胞。在这些测定系统中,对参与四项独立临床试验的17例乳腺癌和卵巢癌患者的配对骨髓(BM)和PBPC样本进行了比较。在9例患者中的7例中,用环磷酰胺和G-CSF动员的PBPC自体移植物在定向和原始祖细胞能力方面与配对的BM自体移植物相比具有优势。在接受这种动员方案的9例患者中的2例中,未能动员出大量原始祖细胞,并且循环CFU-GM或CD34+细胞数量均无法预测这一情况。先前的骨髓抑制治疗经历在一定程度上降低了外周祖细胞产量,但仍能采集到PBPC自体移植物,其在总CFU-GM和前CFU方面与BM自体移植物相比具有优势。在接受过先前骨髓抑制治疗的患者中,单独使用G-CSF或GM-CSF动员PBPC产生的自体移植物中定向祖细胞相对缺乏,但原始祖细胞绝对缺乏。我们得出结论,优化患者特征和动员参数可以获得富含原始和定向造血祖细胞的PBPC自体移植物。

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