首页> 外文期刊>Transfusion: The Journal of the American Association of Blood Banks >Whole-blood leuko-depletion filters as a source of CD 34+ progenitors potentially usable in cell therapy.
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Whole-blood leuko-depletion filters as a source of CD 34+ progenitors potentially usable in cell therapy.

机译:全血白细胞耗竭过滤器作为CD 34+祖细胞的来源,可用于细胞治疗。

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BACKGROUND: Used leuko-depletion filters (LDFs), containing billions of white blood cells (WBCs), are discarded. Because the steady-state blood contains low quantities of stem and progenitor cells that are retained in LDFs, the viability and the functional properties of mononuclear cells (MNCs) and CD 34+ cells recovered from LDFs were investigated. STUDY DESIGN AND METHODS: WBCs were recovered from LDFs by use of a closed system. MNCs and CD 34+ cells were isolated from freshly LDF-recovered WBCs or after their overnight incubation. The CD 34+ cells were enumerated, as well as the number of colony-forming unit (CFU)-granulocyte-macrophage, burst-forming unit-erythroid, and CFU-Mixed. The expansion in clinical-scale volume cultures (serum-free medium plus stem cell factor, granulocyte-colony-stimulating factor, and megakaryocyte growth and development factor) was performed starting from MNCs, freshly isolated CD 34+ cells, and CD 34+ cells isolated after overnight incubation of WBCs. The erythroid, megakaryocytic, eosinophilic, and monocyte-myelocytic lineage differentiation of LDF-recovered CD 34+ cells was challenged in liquid cultures by adding relevant cytokines. RESULTS: Nearly 450 x 10(3) viable CD 34+ cells were recovered per LDF. These cells exhibit unimpaired colony-forming ability. It is possible to expand these cells ex vivo, but their response to cytokines is different compared to mobilized peripheral blood and cord blood CD 34+ cells. Thus, further work is necessary to optimize their ex vivo expansion. These cells give rise to the mature cells and precursors of erythroid, megakaryocytic, eosinophilic, and monomyelocytic lineage in liquid cultures. CONCLUSION: MNCs and CD 34+ cells recovered from the LDFs exhibit unimpaired functional capacities. Recent development of ex vivo technologies for expansion, retro-differentiation, and differentiation reinforces the value in cell therapy of these LDG-recovered peripheral blood progenitor cells that are routinely discarded.
机译:背景:丢弃了包含数十亿白细胞(WBC)的用过的白细胞耗竭滤镜(LDF)。由于稳态血液中含有少量保留在LDF中的干细胞和祖细胞,因此对从LDF中回收的单核细胞(MNC)和CD 34+细胞的活力和功能特性进行了研究。研究设计和方法:通过封闭系统从LDF中回收白细胞。从新鲜的LDF回收的WBC中或隔夜孵育后,分离MNC和CD 34+细胞。计数CD 34+细胞,以及菌落形成单位(CFU)-粒细胞巨噬细胞,爆发形成单位红系和CFU-混合的数量。从MNC,新鲜分离的CD 34+细胞和CD 34+细胞开始进行临床规模的体积培养(无血清培养基加干细胞因子,粒细胞集落刺激因子和巨核细胞生长和发育因子)的扩增WBC孵育过夜后分离。 LDF回收的CD 34+细胞的红系,巨核细胞,嗜酸性和单核细胞系分化通过添加相关细胞因子在液体培养物中受到挑战。结果:每个LDF回收了将近450 x 10(3)个CD 34+活细胞。这些细胞表现出不受损害的集落形成能力。可以离体扩增这些细胞,但与动员的外周血和脐带血CD 34+细胞相比,它们对细胞因子的反应不同。因此,需要进一步的工作以优化其离体扩增。这些细胞在液体培养物中产生红细胞,巨核细胞,嗜酸性和单核细胞谱系的成熟细胞和前体。结论:从LDF中回收的MNC和CD 34 +细胞显示出未受损的功能能力。用于扩增,逆向分化和分化的离体技术的最新发展增强了常规丢弃的这些经LDG回收的外周血祖细胞在细胞治疗中的价值。

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