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Immunomodulation By Therapeutic Mesenchymal Stromal Cells (MSC) Is Triggered Through Phagocytosis of MSC By Monocytic Cells

机译:通过单核细胞通过MSC的吞噬作用引发治疗性间充质细胞(MSC)的免疫调节

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摘要

Abstract Mesenchymal stem or stromal cells (MSC) are under investigation as a potential immunotherapy. MSC are usually administered via intravenous infusion, after which they are trapped in the lungs and die and disappear within a day. The fate of MSC after their disappearance from the lungs is unknown and it is unclear how MSC realize their immunomodulatory effects in their short lifespan. We examined immunological mechanisms determining the fate of infused MSC and the immunomodulatory response associated with it. Tracking viable and dead human umbilical cord MSC (ucMSC) in mice using Qtracker beads (contained in viable cells) and Hoechst33342 (staining all cells) revealed that viable ucMSC were present in the lungs immediately after infusion. Twentyfour hours later, the majority of ucMSC were dead and found in the lungs and liver where they were contained in monocytic cells of predominantly nonclassical Ly6Clow phenotype. Monocytes containing ucMSC were also detected systemically. In vitro experiments confirmed that human CD14++ /CD16 classical monocytes polarized toward a nonclassical CD14++ CD16+ CD206+ phenotype after phagocytosis of ucMSC and expressed programmed death ligand1 and IL10, while TNF?was reduced. ucMSCprimed monocytes induced Foxp3+ regulatory T cell formation in mixed lymphocyte reactions. These results demonstrate that infused MSC are rapidly phagocytosed by monocytes, which subsequently migrate from the lungs to other body sites. Phagocytosis of ucMSC induces phenotypical and functional changes in monocytes, which subsequently modulate cells of the adaptive immune system. It can be concluded that monocytes play a crucial role in mediating, distributing, and transferring the immunomodulatory effect of MSC. Stem Cells 2018;36:602615
机译:摘要间充质茎或基质细胞(MSC)是作为潜在的免疫疗法进行调查。 MSC通常通过静脉内输注给药,之后它们被困在肺部并在一天内消失并消失。 MSC从肺部消失后的MSC的命运是未知的,目前还不清楚MSC如何在其短时间内实现其免疫调节效果。我们检查了确定注入MSC的命运和与其相关的免疫调节反应的免疫机制。使用Qtracker珠子(包含在活细胞中)和Hoechst33342(染色所有细胞)的鼠标中跟踪可行和死人脐带MSC(UCMSC)显示,输注后立即存在活性UCMSC。 TwentyFour小时后,大多数UCMSC死亡,在肺部和肝脏中发现,其中它们包含在主要的非繁症式Ly6clow表型的单核细胞中。还系统性地检测含有UCMSC的单核细胞。体外实验证实,人CD14 ++ / CD16常态单核细胞偏振于UCMSC的吞噬作用吞噬作用后的非生效CD14 ++ CD16 + CD206 +表型,并表达了编程死亡配体1和IL10,而TNF?减少。 UCMSCPRIMED单核细胞在混合淋巴细胞反应中诱导Foxp3 +调节T细胞形成。这些结果表明,注入的MSC是单核细胞迅速吞噬的,随后从肺部迁移到其他身体部位。 UCMSC的吞噬作用诱导单核细胞的表型和功能变化,随后调节自适应免疫系统的细胞。可以得出结论,单核细胞在介导,分配和转移MSC的免疫调节作用方面发挥着至关重要的作用。干细胞2018; 36:602615

著录项

  • 来源
    《Stem Cells》 |2018年第4期|共14页
  • 作者单位

    Rotterdam Transplant Group Department of Internal MedicineErasmus MCRotterdam The Netherlands;

    Rotterdam Transplant Group Department of Internal MedicineErasmus MCRotterdam The Netherlands;

    Rotterdam Transplant Group Department of Internal MedicineErasmus MCRotterdam The Netherlands;

    BioInVision Inc.Mayfield Village Ohio USA;

    Rotterdam Transplant Group Department of Internal MedicineErasmus MCRotterdam The Netherlands;

    Rotterdam Transplant Group Department of Internal MedicineErasmus MCRotterdam The Netherlands;

    Rotterdam Transplant Group Department of Internal MedicineErasmus MCRotterdam The Netherlands;

    Orbsen Therapeutics Ltd.Galway Ireland;

    Orbsen Therapeutics Ltd.Galway Ireland;

    BioInVision Inc.Mayfield Village Ohio USA;

    Rotterdam Transplant Group Department of Internal MedicineErasmus MCRotterdam The Netherlands;

    National Institute for Health Research Liver Biomedical Research Unit at University Hospitals;

    Rotterdam Transplant Group Department of Internal MedicineErasmus MCRotterdam The Netherlands;

    Rotterdam Transplant Group Department of Internal MedicineErasmus MCRotterdam The Netherlands;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物医学工程;
  • 关键词

    Immunomodulation; Immunotherapy; Mesenchymal stromal cell; Monocytes;

    机译:免疫调节;免疫疗法;间充质基质细胞;单核细胞;

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