体外扩增CD34+/AC133+选择的自体外周血祖细胞(PBPC)在接受强化化疗的高危乳腺癌患者中的应用

J Vávrová, S Filip, D Vokurková, M Bláha, J Vanásek, L Jebavý
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引用次数: 12

摘要

AC133抗体为移植情况下移植所需细胞的选择和表征提供了CD34的替代品。我们研究了干细胞因子(SCF)、白细胞介素3 (IL-3)和白细胞介素11 (IL-11)对人CD34+/AC133+祖细胞体外扩增的影响,这些祖细胞是从化疗加粒细胞集落刺激因子(G-CSF)动员的成人供者的白细胞分离产物中分离出来的。MiniMACS AC133+分离细胞平均含有85%(80-90)的AC133+细胞。富集的AC133+细胞共表达CD34+ 80%、CD71low 36.6%和CD33+ 6.6%。SCF + IL-3 + IL-11体外培养7天后,细胞数量增加了19倍。这些细胞平均表达12%的CD34+和74%的CD71+ (CD71高23%)和59%的CD33+。这意味着CD34+细胞的绝对数量略有增加,CD33+的数量增加了100倍,出现了高密度cd71高(23%)的细胞。这些细胞代表红细胞分化的细胞。我们将讨论细胞因子SCF + Il-3 + IL-11的不同组合对CFU-GM数量的增加。体外培养7天后,在SCF + IL-3 + IL-11的存在下,CFU-GM的数量增加了45倍。
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Ex vivo expansion CD34+/AC133+-selected autologous peripheral blood progenitor cells (PBPC) in high-risk breast cancer patients receiving intensive chemotherapy.

AC133 antibody provides an alternative to CD34 for the selection and characterization of cells necessary for engraftment in transplant situations. We studied the effect of stem cell factor (SCF), interleukin 3 (IL-3) and interleukin 11 (IL-11) on the ex vivo expansion of human CD34+/AC133+ progenitors isolated from leukapheresis products from chemotherapy plus granulocyte-colony-stimulating factor (G-CSF) -mobilized adult donors. MiniMACS AC133+ isolated cells contained a mean of 85% (80-90) AC133+ cells. Enriched AC133+ cells co-expressed CD34+ 80%, CD71low 36.6% and CD33+ 6.6%. After a seven-day ex vivo expansion in the presence of SCF + IL-3 + IL-11, the number of cells increased 19 times. These cells expressed a mean 12% CD34+ and 74% CD71+ (23% CD 71high) and 59% CD33+. This means that the absolute number of CD34+ cells increased slightly, the number of CD33+ increased 100 times and cells with high density CD71high (23%) appeared. These cells represent the cells committed to erythroid differentiation. The increase in the number of CFU-GM with various combinations of cytokines SCF + Il-3 + IL-11 will be discussed. The number of CFU-GM in culture after a seven-day ex vivo expansion in the presence of SCF + IL-3 + IL-11 increased 45 times.

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