使用丙戊酸和/或烟酰胺扩增脐带血造血干细胞和祖细胞(HSPC)的体内和体外效应

IF 3.2 4区 医学 Q2 MEDICINE, RESEARCH & EXPERIMENTAL
Emine Begum Gencer , Hasan Yalim Akin , Selami Kocak Toprak , Eylul Turasan , Mahsa Yousefzadeh , Pinar Yurdakul-Mesutoglu , Murat Cagan , Mehmet Murat Seval , Doruk Cevdi Katlan , Klara Dalva , Mehmet Sinan Beksac , Meral Beksac
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引用次数: 0

摘要

背景脐带血(CB)的自我更新能力强,最易被移植,因此移植成功率高,但造血干细胞和祖细胞(HSPC)数量少,限制了其广泛应用。为了克服这一问题,使用丙戊酸(VPA)或烟酰胺(NAM)等小分子进行体外扩增已被证明是有效的。据我们所知,VPA 和 NAM 对 HSPC 扩增的联合作用还没有进行过研究。本研究的目的是分析 VPA 和 NAM 单独或联合使用对 HSPC 扩增和移植的体内外疗效。为了确定体内外疗效,用 VPA 和/或 NAM 扩增了人 CB CD34+ 细胞,并对扩增的 HSPC 进行了集落形成单位(CFU)检测。同时通过静脉注射扩增的 HSPC 给 NOD-SCID gamma (NSG) 小鼠(n = 22)进行异种移植。根据分布的正态性和分析的组数,采用 t 检验、Mann-Whitney 检验、方差分析或 Kruskal-Wallis 检验分析扩增组或异种移植模型之间差异的显著性。VPA+NAM 的协同效应在孵化 21 天(D21)时达到最大相对扩展倍数 [2.95 (1.00-11.94)] 。VPA 和 VPA+NAM D21 之间无明显差异(p = 0.44)。与仅使用细胞因子组相比,NAM 的菌落形成单位粒细胞-巨噬细胞(CFU-GM)菌落数折合数高于 VPA [1.87 (1.00-3.59) vs 1.00 (1.00-1.81);p < 0.01]。VPA+NAM D21 [1.62 (1.00-2.77)] 也优于 VPA(p < 0.05)。NAM 和 VPA+NAM D21 之间没有明显差异。在小鼠模型中进行人 CB34+ CB 移植(CBT)后,VPA+NAM 扩增细胞的体内白细胞恢复最快(6 ± 2 天),VPA 扩增的 CBT 可检测到最高水平的人 CD45 嵌合(VPA:第 28 天为 5.结论我们的研究结果表明,单独使用 VPA,而不是与 NAM 或 NAM 单用,可以更好、更快地扩增和移植 CB HSPC。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
In vivo and in vitro effects of cord blood hematopoietic stem and progenitor cell (HSPC) expansion using valproic acid and/or nicotinamide

Background

High self-renewal capacity and most permissive nature of umbilical cord blood (CB) results with successful transplant outcomes but low hematopoietic stem and progenitor cell (HSPC) counts limits wider use. In order to overcome this problem ex vivo expansion with small molecules such as Valproic acid (VPA) or Nicotinamide (NAM) have been shown to be effective. To the best of our knowledge, the combinatory effects of VPA and NAM on HSPC expansion has not been studied earlier. The aim of this study was to analyze ex vivo and in vivo efficacy of VPA and NAM either alone or in combination in terms of expansion and engraftment.

Methods

A total of 44 CB units were included in this study. To determine the ex vivo and in vivo efficacy, human CB CD34+ cells were expanded with VPA and/or NAM and colony forming unit (CFU) assay was performed on expanded HSPC. Xenotransplantation was performed simultaneously by intravenous injection of expanded HSPC to NOD-SCID gamma (NSG) mice (n = 22). Significance of the difference between the expansion groups or xenotransplantation models was analyzed using t-test, Mann-Whitney, ANOVA or Kruskal-Wallis tests as appropriate considering the normality of distributions and the number of groups analyzed.

Results

In vitro CD34+ HSPC expansion fold relative to cytokines-only was significantly higher with VPA compared to NAM [2.23 (1.07–5.59) vs 1.48 (1.00–4.40); p < 0.05]. Synergistic effect of VPA+NAM has achieved a maximum relative expansion fold at 21 days (D21) of incubation [2.95 (1.00–11.94)]. There was no significant difference between VPA and VPA+NAM D21 (p = 0.44). Fold number of colony-forming unit granulocyte-macrophage (CFU-GM) colonies relative to the cytokine-only group was in favor of NAM compared to VPA [1.87 (1.00–3.59) vs 1.00 (1.00–1.81); p < 0.01]. VPA+NAM D21 [1.62 (1.00–2.77)] was also superior against VPA (p < 0.05). There was no significant difference between NAM and VPA+NAM D21. Following human CB34+ CB transplantation (CBT) in the mouse model, fastest in vivo leukocyte recovery was observed with VPA+NAM expanded cells (6 ± 2 days) and the highest levels of human CD45 chimerism was detectable with VPA-expanded CBT (VPA: 5.42 % at day 28; NAM: 2.45 % at day 31; VPA+NAM 1.8 % at day 31).

Conclusion

Our study results suggest using VPA alone, rather than in combination with NAM or NAM alone, to achieve better and faster expansion and engraftment of CB HSPC.

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来源期刊
Current Research in Translational Medicine
Current Research in Translational Medicine Biochemistry, Genetics and Molecular Biology-General Biochemistry,Genetics and Molecular Biology
CiteScore
7.00
自引率
4.90%
发文量
51
审稿时长
45 days
期刊介绍: Current Research in Translational Medicine is a peer-reviewed journal, publishing worldwide clinical and basic research in the field of hematology, immunology, infectiology, hematopoietic cell transplantation, and cellular and gene therapy. The journal considers for publication English-language editorials, original articles, reviews, and short reports including case-reports. Contributions are intended to draw attention to experimental medicine and translational research. Current Research in Translational Medicine periodically publishes thematic issues and is indexed in all major international databases (2017 Impact Factor is 1.9). Core areas covered in Current Research in Translational Medicine are: Hematology, Immunology, Infectiology, Hematopoietic, Cell Transplantation, Cellular and Gene Therapy.
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