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Human Wharton's jelly mesenchymal stem cells maintain the expression of key immunomodulatory molecules when subjected to osteogenic, adipogenic and chondrogenic differentiation in vitro: new perspectives for cellular therapy.

机译:沃顿商学院的果冻间充质干细胞在体外进行成骨,成脂和成软骨分化时,可维持关键免疫调节分子的表达:细胞疗法的新观点。

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摘要

Rheumatoid arthritis and osteoarthritis are the main diseases that imply an inflammatory process at the joints involving the articular cartilage. Recently, mesenchymal stem cells (MSCs) derived from perinatal tissues were considered good candidates for cellular therapy of musculoskeletal and orthopaedic diseases, since they can differentiate into multiple cell types and are an easily accessible cellular source. Therefore, several protocols exist on the differentiation of mesenchymal stem cells of different origins into osteoblasts and chondrocytes. Another key feature of MSCs is their capacity to modulate the immune system responses in vitro and in vivo. This may have critical outcomes in diseases of the musculoskeletal system where an inflammatory or autoimmune process is at the basis of the main disease. In the present paper, after isolation of MSCs from Wharton's Jelly (WJ-MSCs), we performed the three standard differentiation protocols. The acquisition of the differentiated phenotype was demonstrated by the specific histological stains. As the main objective of this work, we determined the expression of immunomodulatory molecules (by immunohistochemistry and qualitative RT-PCR), both in undifferentiated cells and after differentiation. We demonstrated for the first time that immune-related molecules (as B7-H3/CD276 and HLA-E) which have been characterized in undifferentiated MSCs, are also expressed by the differentiated progeny. This strongly suggests that also after the acquisition of a mature phenotype, WJ-MSCs-derived cells may maintain their immune privilege. This evidence, which deserves much work to be confirmed in vivo and in other MSCs populations, may provide a formal proof of the good results globally achieved with WJMSCs as cellular therapy vehicle.
机译:类风湿关节炎和骨关节炎是暗示关节软骨关节发炎的主要疾病。近来,源自围产期组织的间充质干细胞(MSC)被认为是肌肉骨骼和骨科疾病细胞治疗的良好候选者,因为它们可以分化为多种细胞类型并且是易于获取的细胞来源。因此,存在关于将不同来源的间充质干细胞分化为成骨细胞和软骨细胞的几种方案。 MSC的另一个关键特征是它们在体外和体内调节免疫系统应答的能力。这在以主要疾病为基础的炎症或自身免疫过程的肌肉骨骼系统疾病中可能会产生关键的后果。在本文中,从沃顿商学院的果冻(WJ-MSC)分离MSC后,我们执行了三种标准的区分方案。特定的组织学染色证明了分化表型的获得。作为这项工作的主要目的,我们确定了未分化细胞和分化后免疫调节分子的表达(通过免疫组织化学和定性RT-PCR)。我们首次证明了在未分化的MSC中表征的免疫相关分子(如B7-H3 / CD276和HLA-E)也由分化后代表达。这有力地表明,在获得成熟的表型后,WJ-MSCs衍生的细胞也可以维持其免疫特权。该证据值得在体内和其他MSCs人群中进行大量工作确认,可以为WJMSCs作为细胞治疗载体在全球范围内取得的良好结果提供正式证明。

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