體外實(shí)驗(yàn)表明,適度低氧下MSCs的生長(zhǎng)和存活能力更好,產(chǎn)生集落形成單位的能力顯著增高,且干細(xì)胞標(biāo)志性基因表達(dá)水平更高[7]。氧濃度可以影響MSCs向成骨、成軟骨、成脂的分化傾向,低氧能提高特異性受體和配體相結(jié)合所介導(dǎo)的遷移。低氧誘導(dǎo)因子1信號(hào)通路[8]在MSCs對(duì)缺氧反應(yīng)的分子機(jī)制中占重要地位。
對(duì)缺氧反應(yīng)的分子機(jī)制本實(shí)驗(yàn)主要研究了CMS患者骨髓MSC的形態(tài)、表型、傳代能力、生長(zhǎng)曲線及擴(kuò)增能力等特征,其結(jié)果為CMS的研究提供了重要信息。但研究報(bào)道例數(shù)尚較少,結(jié)論還需要深入的體內(nèi)實(shí)驗(yàn)及分子生物學(xué)研究支持。
【參考文獻(xiàn)】
[1] Yukari M,TakashiY,Hiroko M.Reconstitution of the functional human hematopoietic microenvironment derived from human mesenchymal stem cells in the murine bone marrow compartment[J].Blood,2006,107:18781887
[2] 國(guó)際高原醫(yī)學(xué)會(huì)慢性高原病專家小組.慢性高原病青海診斷標(biāo)準(zhǔn)[J].青海醫(yī)學(xué)院學(xué)報(bào),2005,26:35
[3] Zhu W,Chen J,Cong X,et al.Hypoxia and serum deprivationinduced apoptosis in mesenchymal stem cells[J].Stem Cells,2006,4:416425
[4] LeBlanc K, Rasmusson I, SundbergB, et al.Treatment of severe acute graftversushost disease with third party haploidentical mesenchymal stem cells[J].Lancet,2004, 363:14391441
[5]Lee OK,Kuo TK,Chen WM,et al.Isolation of multipotent mesenchymal stem cells from umbilical cord blood[J].Blood, 2004,103:16691675
[6]Pittenger MF,Mackay AM,Beck SC,et al.Multilineage potential of adult human mesenchymal stemcells[J].Science,1999,284:143醫(yī).學(xué)全.在.線網(wǎng)站quanxiangyun.cn
[7] Bosch P, Pratt SL, Stice SL. Isolation, characterization, gene modification, and nuclear reprogramming of porcine mesenchymal stem cells[J]. Biol Reprod, 2006, 74:4657
[8] Bracken CP,Fedele AO,Linke S,et al.Cellspecific regulation of HIF1 alpha and HIF2 alpha:Stabilization and transactivation in a graded oxygen environment[J].J Biol Chem,2006,281:2257522585