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基质细胞衍生因子-1和血小板第4因子对体外扩增后脐血CD34+细胞黏附特性和趋化功能的影响
引用本文:李桥川,李云涛,孟恒星,王亚非,万长春,李新,葛薇,李茜,韩俊领,邱录贵.基质细胞衍生因子-1和血小板第4因子对体外扩增后脐血CD34+细胞黏附特性和趋化功能的影响[J].中国实验血液学杂志,2006,14(1):83-88.
作者姓名:李桥川  李云涛  孟恒星  王亚非  万长春  李新  葛薇  李茜  韩俊领  邱录贵
作者单位:1. 中国医学科学院,中国协和医科大学,血液学研究所,血液病医院实验血液学国家重点,实验室,天津,300020
2. 天津脐带血造血干细胞库,天津,300384
基金项目:天津市应用基础研究项目;天津市应用基础研究项目
摘    要:为了研究基质细胞衍生因子-1(SDF—1)和血小板第4因子(PF4)对扩增后脐血CD34^+细胞归巢相关功能的影响,将纯化的脐血CD34^+细胞接种入无血清培养液中,加入不同组合的细胞因子FST(FL+SCF+TPO)、FST+SDF—1、FST+PF4或FST+SDF—1+PF4,分别于培养第7、10、14天检测CD34^+细胞扩增倍数、集落形成能力、细胞的黏附分子表达、总黏附性、趋化功能。结果表明:①加入SDF—1的实验组CD34^+细胞及造血祖细胞集落扩增倍数高于对照组;②加入SDF—1明显上调扩增的CD34^+细胞CD49e的表达,加入PF4明显上调扩增的CD34^+细胞CD49e、CD54的表达,在扩增体系中加入SDF—1或PF4均能够明显提高扩增的CD34^+细胞的总黏附性;③在扩增体系中加入SDF—1能够明显提高扩增的CD34^+细胞的自发迁移率,但导致CXCR-4的表达和SDF—1诱导迁移率降低;而PF4能够明显提高扩增的CD34^+细胞的CXCR-4的表达和SDF—1诱导迁移率;在扩增体系中同时加入SDF—1和PF4能够明显提高扩增的CD34^+细胞自发迁移率和SDF—1诱导迁移率。结论:体外扩增体系中加入SDF—1和PF4能够上调部分归巢相关黏附分子的表达,保持扩增的CD34^+细胞的黏附和迁移能力,有利于降低体外扩增对造血干/祖细胞(HSPC)归巢相关功能的不利影响,维持扩增的HSPC的归巢潜能。

关 键 词:CD34  细胞  脐带血  基质细胞衍生因子-1  血小板第4因子  体外扩增  黏附特性  趋化功能
文章编号:1009-2137(2006)01-0083-06
收稿时间:2005-08-22
修稿时间:2005-12-15

Effects of Stromal Cell-derived Factor 1 and Platelet Factor 4 on the Adhesion Characteristics and Chemotactic Function of Ex Vivo Expanded Umbilical Cord Blood CD34 + Cells
LI Qiao-Chuan,LI Yun-Tao,MENG Heng-Xing,WANG Ya-Fei,WAN Chang-Chun,LI Xin,GE Wei,LI Qian,HAN Jun-Ling,QIU Lu-Gui.Effects of Stromal Cell-derived Factor 1 and Platelet Factor 4 on the Adhesion Characteristics and Chemotactic Function of Ex Vivo Expanded Umbilical Cord Blood CD34 + Cells[J].Journal of Experimental Hematology,2006,14(1):83-88.
Authors:LI Qiao-Chuan  LI Yun-Tao  MENG Heng-Xing  WANG Ya-Fei  WAN Chang-Chun  LI Xin  GE Wei  LI Qian  HAN Jun-Ling  QIU Lu-Gui
Affiliation:State Key Laboratory of Experimental Hematology, Institute of Hematology & Blood Diseases Hospital, Chinese Academy of Medical Sciences and Peking Union Medical College, Tianjin 300020, China.
Abstract:To investigate the effects of stromal cell-derived factor 1 (SDF-1) and platelet factor 4 (PF4) on the homing-related function of expanded ex vivo umbilical cord blood CD34~+ cells, purified cord blood CD34~+ cells were cultured in serum-free medium containing a HGF combination of FL+SCF+TPO (FST) with either 100 ng/ml SDF-1 alone, 100 ng/ml PF4 alone, or both of these 2 cytokines. The expansion rate of CD34~+ cells, colony formation, homing-related functions including expression of homing-related adhesion molecules of expanded CD34~+ cell, adhesion activity and chemotactic function of the re-selected expanded CD34~+ cells were evaluated at different time points. The results showed that expansion rate of CD34~+ cells and expansion multiple of CFU in SDF-1 groups were higher than those in control. The expression of CD49e on the expanded CD34~+ cells was remarkable up-regulated, in contrast, expression of CXCR-4 on the expanded CD34~+ cells was remarkable down-regulated in SDF-1 groups. The expression of CD49e, CD54 and CXCR-4 on the expanded CD34~+ cells were remarkably up-regulated in the PF4 groups. In all the SDF-1 group, PF4 group and SDF-1 plus PF4 group, the ability of expanded CD34~+ cells adhering to fibronectin layer were higher than those in the control on day 10. Spontaneous migration rate of expanded CD34~+ cells in SDF-1 groups were higher than those in control, while SDF-1-induced migration rate were lower than those in control on day 10. SDF-1-induced migration rate in PF4 groups were higher than those in control on day 10. Spontaneous and SDF-1-induced migration rate of expanded CD34~+ cells in the SDF-1 plus PF4 groups were higher than those in control on day 10. It is concluded that, SDF-1 and PF4 can up-regulate expression of adhension molecules on expanded CD34~+ cells, and retain the adherent and migration ability of expanded CD34~+ cells, which is helpful for the homing of expanded CD34~+ cells. In short, SDF-1 and PF4 are helpful for the homing-related function of the expanded UCB HSPC.
Keywords:CD34~+ cell  umbilical cord blod  stromal cell-derived factor 1  platelet factor 4  adhesion characteristics  chemotactic function  ex-vivo expansion
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