造血祖细胞的体外扩增:乳腺癌的初步结果。

I McNiece, R Jones, P Cagnoni, S Bearman, Y Nieto, E J Shpall
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引用次数: 35

摘要

体外扩增祖细胞被认为是支持大剂量化疗的细胞来源,并减少或消除移植后的中性粒细胞减少期。迄今为止,还没有使用体外扩增细胞的临床研究表明中性粒细胞或血小板恢复的时间有任何减少,尽管已经进行了一些使用各种生长因子鸡尾酒和培养条件的临床研究。在过去的6年中,我们开发了一种静态培养系统,可使骨髓祖细胞达到最佳扩增。我们已经启动了一项临床研究,以评估该培养系统在接受外周血祖细胞(PBPC)支持大剂量化疗的乳腺癌患者中的应用。CD34选择的细胞在800 ml的指定培养基(Amgen Inc.)中培养10天,其中rhSCF, rhG-CSF和rhMGDF各含有100 ng/ml,并在1L特氟隆袋(American Fluoroseal)中培养2万至5万个细胞/ml。培养后,用3体积PBS洗涤细胞以去除所有培养基和生长因子,移植第0天重新输注,然后每天给药rhG-CSF。第1天,患者接受未扩展的PBPC产品,以确保移植物的耐久性。移植扩增PBPC细胞的患者早在移植后第4天恢复中性粒细胞计数(ANC > 500/微升),中位数为6天(范围为4至14天)。相比之下,我们的历史对照组(N=175)患者进行中性粒细胞移植的中位时间为9天(范围为7至24天)。第二组患者单独移植扩增细胞,获得了类似的快速植入。第一批患者在移植后70多天内进行了持久的植入。迄今为止,在任何患者中未观察到对血小板恢复的影响。这些数据表明,在规定的条件下扩大PBPC可以显着缩短中性粒细胞的植入时间。
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Ex-vivo expansion of hematopoietic progenitor cells: preliminary results in breast cancer.

Ex-vivo expanded progenitor cells have been proposed as a source of cells to support high-dose chemotherapy and to decrease or eliminate the period of neutropenia following transplantation. To date, no clinical studies using ex vivo expanded cells, have demonstrated any decrease in the time to neutrophil or platelet recovery, although a number of clinical studies have been performed using a variety of growth factor cocktails and culture conditions. Over the past 6 years we have developed a static culture system that results in optimal expansion of myeloid progenitor cells. We have initiated a clinical study to evaluate this culture system in breast cancer patients receiving peripheral blood progenitor cells (PBPC) to support high-dose chemotherapy. CD34 selected cells were cultured for 10 days in 800 ml of defined media (Amgen Inc.) containing 100 ng/ml each of rhSCF, rhG-CSF and rhMGDF in 1L teflon bags (American Fluoroseal) at 20,000 to 50,000 cells per ml. After culture the cells were washed with 3 volumes of PBS to remove all media and growth factors and reinfused on day 0 of transplant followed by daily administration of rhG-CSF. On day +1 the patients received an unexpanded PBPC product to ensure the durability of the graft. Patients transplanted with expanded PBPC cells recovered neutrophil counts (ANC > 500/microl) as early as day 4 post transplant with a median of 6 days (range 4 to 14 days). In comparison, our historical control group of patients (N=175) had a median time to neutrophil engraftment of 9 days (range 7 to 24 days). A second cohort of patients were transplanted with expanded cells alone and a similar rapid engraftment was obtained. The first patients are now over 70 days post transplant with durable engraftment. No effect on platelet recovery has been observed in any patients to date. These data demonstrate that PBPC expanded under the conditions defined can significantly shorten the time to engraftment of neutrophils.

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