细胞因子治疗可优化脐带间充质干细胞对炎症性肝病的免疫治疗效果。
Cytokine treatment optimises the immunotherapeutic effects of umbilical cord-derived MSC for treatment of inflammatory liver disease.
作者信息
de Witte Samantha F H, Merino Ana M, Franquesa Marcella, Strini Tanja, van Zoggel Johanna A A, Korevaar Sander S, Luk Franka, Gargesha Madhu, O'Flynn Lisa, Roy Debashish, Elliman Steve J, Newsome Philip N, Baan Carla C, Hoogduijn Martin J
机构信息
Nephrology and Transplantation, Department of Internal Medicine, Erasmus MC, Postbus 2040, 3000 CA, Rotterdam, The Netherlands.
Experimental Urology Department, Department of Internal Medicine, Erasmus MC, Rotterdam, The Netherlands.
出版信息
Stem Cell Res Ther. 2017 Jun 8;8(1):140. doi: 10.1186/s13287-017-0590-6.
BACKGROUND
Mesenchymal stromal cells (MSC) possess immunomodulatory properties and low immunogenicity, both crucial properties for their development into an effective cellular immunotherapy. They have shown benefit in clinical trials targeting liver diseases; however the efficacy of MSC therapy will benefit from improvement of the immunomodulatory and immunogenic properties of MSC.
METHODS
MSC derived from human umbilical cords (ucMSC) were treated for 3 days in vitro with various inflammatory factors, interleukins, vitamins and serum deprivation. Their immunogenicity and immunomodulatory capacity were examined by gene-expression analysis, surface-marker expressions, IDO activity, PGE secretion and inhibition of T cell proliferation and IFNγ production. Furthermore, their activation of NK cell cytotoxicity was investigated via CD107a expression on NK cells. The immunomodulatory capacity, biodistribution and survival of pre-treated ucMSC were investigated in a CCl-induced liver disease mouse model. In addition, capacity of pre-treated MSC to ameliorate liver inflammation was examined in an ex vivo liver inflammation co-culture model.
RESULTS
IFN-γ and a multiple cytokine cocktail (MC) consisting of IFN-γ, TGFβ and retinoic acid upregulated the expression of immunomodulatory factor PD-L1 and IDO activity. Subsequently, both treatments enhanced the capacity of ucMSC to inhibit CD4 and CD8 T cell proliferation and IFN-γ production. The susceptibility of ucMSC for NK cell lysis was decreased by IFN-β, TGFβ and MC treatment. In vivo, no immunomodulation was observed by the ucMSC. Four hours after intravenous infusion in mice with CCl-induced inflammatory liver injury, the majority of ucMSC were trapped in the lungs. Rapid clearance of ucMSC(VitB), ucMSC(Starv + VitB) and ucMSC(MC) and altered bio-distribution of ucMSC(TGFβ) compared to untreated ucMSC was observed. In the ex vivo co-culture system with inflammatory liver slices ucMSC(MC) showed significantly enhanced modulatory capacity compared to untreated ucMSC.
CONCLUSIONS
The present study demonstrates the responsiveness of ucMSC to in vitro optimisation treatment. The observed improvements in immunomodulatory capacity as well as immunogenicity after MC treatment may improve the efficacy of ucMSC as immunotherapy targeted towards liver inflammation.
背景
间充质基质细胞(MSC)具有免疫调节特性和低免疫原性,这两种特性对于其发展成为有效的细胞免疫疗法至关重要。它们在针对肝脏疾病的临床试验中已显示出益处;然而,MSC疗法的疗效将受益于MSC免疫调节和免疫原性特性的改善。
方法
源自人脐带的MSC(ucMSC)在体外分别用各种炎性因子、白细胞介素、维生素处理3天以及进行血清饥饿处理。通过基因表达分析、表面标志物表达、吲哚胺2,3-双加氧酶(IDO)活性、前列腺素E(PGE)分泌以及对T细胞增殖和γ干扰素(IFNγ)产生的抑制作用来检测它们的免疫原性和免疫调节能力。此外,通过NK细胞上CD107a的表达来研究它们对NK细胞细胞毒性的激活作用。在四氯化碳(CCl)诱导的肝脏疾病小鼠模型中研究预处理的ucMSC的免疫调节能力、生物分布和存活情况。另外,在体外肝脏炎症共培养模型中检测预处理的MSC改善肝脏炎症的能力。
结果
干扰素γ(IFN-γ)以及由IFN-γ、转化生长因子β(TGFβ)和视黄酸组成的多种细胞因子混合物(MC)上调了免疫调节因子程序性死亡受体配体1(PD-L1)的表达和IDO活性。随后,两种处理均增强了ucMSC抑制CD4和CD8 T细胞增殖以及IFN-γ产生的能力。IFN-β、TGFβ和MC处理降低了ucMSC对NK细胞裂解的敏感性。在体内,未观察到ucMSC的免疫调节作用。在CCl诱导的炎性肝损伤小鼠中静脉注射4小时后,大多数ucMSC被困在肺部。与未处理的ucMSC相比,观察到ucMSC(维生素B)、ucMSC(饥饿+维生素B)和ucMSC(MC)的快速清除以及ucMSC(TGFβ)生物分布的改变。在与炎性肝切片的体外共培养系统中,与未处理的ucMSC相比,ucMSC(MC)显示出显著增强的调节能力。
结论
本研究证明了ucMSC对体外优化处理的反应性。MC处理后观察到的免疫调节能力以及免疫原性的改善可能会提高ucMSC作为针对肝脏炎症的免疫疗法的疗效。
Zotero 插件