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白细胞介素-16可与早期起作用的细胞因子协同作用,以体外扩增从脐带血中分离出的CD34+细胞。

IL-16 can synergize with early acting cytokines to expand ex vivo CD34+ isolated from cord blood.

作者信息

Rofani Cristina, Luchetti Luisella, Testa Giuseppe, Lasorella Rosa, Isacchi Giancarlo, Bottazzo Gian Franco, Berardi Anna C

机构信息

Stem Cells Laboratory, Bambino Gesù Children's Hospital, Scientific Institute (IRCCS), Rome, Italy.

出版信息

Stem Cells Dev. 2009 May;18(4):671-82. doi: 10.1089/scd.2008.0187.

Abstract

We previously reported that interleukin (IL)-16 can induce CD34(+) hematopoietic cells to proliferate and differentiate in vitro into phenotypically and functionally mature dendritic cells. In this study, we investigated the effects of IL-16 on the expansion of CD34(+) cells from human cord blood (CB). CD34(+) CB cells were cultured for 14 days in medium containing a basal cocktail (BC) containing stem cell factor, Flt-3 ligand, thrombopoietin, IL-6, and IL-3 with and without IL-16 as a control. Interleukin-16 added to BC significantly enhanced the expansion of CD34(+) cells (66.47 +/- 1.46-fold vs. 36.23 +/- 1.67-fold), as well as CD34(+)CD38(-) early stem cells (106.67 +/- 2.34-fold vs. 63.42 +/- 1.89-fold) and progenitor cells [colony-forming unit (CFU) -mixed -(GEMM)] and multilineage-committed progenitors [burst-forming unit (BFU-E), CFU-granulocyte, macrophage (-GM), CFU-megakaryocyte (-MK)]. Interleukin-16 also significantly increased long-term culture-initiating cells (160.8 +/- 3.45-fold vs. 83 +/- 2.89-fold with BC alone). Moreover, CD34(+) cells expanded with IL-16 maintained the capacity to differentiate into the lymphoid-B and -NK lineage. The addition of IL-16 to BC increased the migratory capacity of expanded CD34(+) cells compared to BC alone, leaving the expression of CXCR4 unaffected, and decreased the percentage of CD34(+)CD4(+) cells. We showed that IL-16 released endogenously affected the ex vivo expansion of CD34(+) cells. Overall, this study suggests that IL-16 may have a new role in promoting the expansion of hematopoietic stem cells and may represent a new tool for the expansion of CD34(+) cells for clinical applications.

摘要

我们之前报道过,白细胞介素(IL)-16能够在体外诱导CD34(+)造血细胞增殖并分化为表型和功能均成熟的树突状细胞。在本研究中,我们调查了IL-16对人脐带血(CB)中CD34(+)细胞扩增的影响。将CD34(+) CB细胞在含有基础细胞因子组合(BC)的培养基中培养14天,该基础细胞因子组合包含干细胞因子、Flt-3配体、血小板生成素、IL-6和IL-3,分别设置添加和不添加IL-16作为对照。添加到BC中的IL-16显著增强了CD34(+)细胞的扩增(66.47±1.46倍 vs. 36.23±1.67倍),以及CD34(+)CD38(-)早期干细胞(106.67±2.34倍 vs. 63.42±1.89倍)和祖细胞[集落形成单位(CFU)-混合-(GEMM)]以及多系定向祖细胞[爆式集落形成单位(BFU-E)、CFU-粒细胞、巨噬细胞(-GM)、CFU-巨核细胞(-MK)]。IL-16还显著增加了长期培养起始细胞(160.8±3.45倍 vs. 单独使用BC时的83±2.89倍)。此外,用IL-16扩增的CD34(+)细胞保持了分化为淋巴B细胞和NK细胞系的能力。与单独使用BC相比,向BC中添加IL-16增加了扩增后的CD34(+)细胞的迁移能力,而不影响CXCR4的表达,并降低了CD34(+)CD4(+)细胞的百分比。我们发现内源性释放的IL-16影响了CD34(+)细胞的体外扩增。总体而言,本研究表明IL-16可能在促进造血干细胞扩增方面具有新作用,并且可能代表一种用于临床应用中扩增CD34(+)细胞的新工具。

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