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人羊膜间充质干细胞及其分泌分子对急性肝衰竭小鼠的治疗潜力。

Therapeutic potential of a distinct population of human amniotic fluid mesenchymal stem cells and their secreted molecules in mice with acute hepatic failure.

机构信息

Cell and Gene Therapy Laboratory, Centre of Basic Research II, Biomedical Research Foundation of the Academy of Athens-BRFAA, Athens, Greece.

出版信息

Gut. 2012 Jun;61(6):894-906. doi: 10.1136/gutjnl-2011-300908. Epub 2011 Oct 13.

DOI:10.1136/gutjnl-2011-300908
PMID:21997562
Abstract

BACKGROUND

There is increasing interest in the therapeutic potential of human mesenchymal stem cells (hMSCs), especially in diseases such as acute hepatic failure (AHF) that are predominantly caused by a variety of drugs and viruses. In previous studies, a distinct population termed human spindle-shaped MSCs were isolated and expanded from second trimester amniotic fluid (AF-MSCs) and characterised based on their phenotype, pluripotency and differentiation potential.

METHODS

AF-MSCs, hepatic progenitor-like (HPL) cells and hepatocyte-like (HL) cells derived from AF-MSCs were transplanted into CCl₄-injured NOD/SCID mice with the AHF phenotype in order to evaluate their therapeutic potential. Conditioned medium (CM) derived from AF-MSCs or HPL cells was then delivered intrahepatically in order to determine whether the engraftment of the cells or their secreted molecules are the most important agents for liver repair.

RESULTS

Both HPL cells and AF-MSCs were incorporated into CCl(4)-injured livers; HPL cell transplantation had a greater therapeutic effect. In contrast, HL cells failed to engraft and contribute to recovery. In addition, HPL-CM was found to be more efficient than CM derived from AF-MSCs in treatment of the liver. Proteome profile analysis of HPL-CM indicated the presence of anti-inflammatory factors such as interleukins IL-10, IL-1ra, IL-13 and IL-27 which may induce liver recovery. Blocking studies of IL-10 secretion from HPL cells confirmed the therapeutic significance of this cytokine in the AHF mouse model.

CONCLUSIONS

Human spindle-shaped AF-MSCs or HPL cells might be valuable tools to induce liver repair and support liver function by cell transplantation. More importantly, the factors they release may also play an important role in cell treatment in diseases of the liver.

摘要

背景

人们对人骨髓间充质干细胞(hMSCs)的治疗潜力越来越感兴趣,特别是在急性肝衰竭(AHF)等主要由各种药物和病毒引起的疾病中。在以前的研究中,从妊娠中期羊水(AF-MSCs)中分离并扩增了一种称为人梭形 MSC 的独特群体,并根据其表型、多能性和分化潜能进行了表征。

方法

将 AF-MSCs、肝祖细胞样(HPL)细胞和源自 AF-MSCs 的肝样(HL)细胞移植到具有 AHF 表型的 CCl4 损伤的 NOD/SCID 小鼠体内,以评估其治疗潜力。然后将源自 AF-MSCs 或 HPL 细胞的条件培养基(CM)肝内递送至以确定细胞的植入或其分泌的分子是否是肝脏修复的最重要的因子。

结果

HPL 细胞和 AF-MSCs 均被整合到 CCl4 损伤的肝脏中;HPL 细胞移植具有更大的治疗效果。相比之下,HL 细胞未能植入并有助于恢复。此外,HPL-CM 被发现比源自 AF-MSCs 的 CM 在治疗肝脏方面更有效。HPL-CM 的蛋白质组谱分析表明存在抗炎因子,如白细胞介素 IL-10、IL-1ra、IL-13 和 IL-27,它们可能诱导肝脏恢复。阻断 HPL 细胞中 IL-10 的分泌研究证实了该细胞因子在 AHF 小鼠模型中的治疗意义。

结论

人梭形 AF-MSCs 或 HPL 细胞可能是通过细胞移植诱导肝脏修复和支持肝功能的有价值的工具。更重要的是,它们释放的因子也可能在肝脏疾病的细胞治疗中发挥重要作用。

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