首页> 外文期刊>Frontiers in Medicine >Human Hemangioblast-Derived Mesenchymal Stem Cells Promote Islet Engraftment in a Minimal Islet Mass Transplantation Model in Mice
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Human Hemangioblast-Derived Mesenchymal Stem Cells Promote Islet Engraftment in a Minimal Islet Mass Transplantation Model in Mice

机译:人血管素衍生的间充质干细胞促进小鼠最小胰岛大规模移植模型中的胰岛植入

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Islet transplantation can restore glycemic control in patients with type 1 diabetes. Using this procedure, the early stages of engraftment are often crucial to long-term islet function, and outcomes are not always successful. Numerous studies have shown that mesenchymal stem cells (MSCs) facilitate islet graft function. However, experimental data can be inconsistent due to variables associated with MSC generation (including donor characteristics and tissue source), thus, demonstrating the need for a well-characterized and uniform cell product before translation to the clinic. Unlike bone marrow- or adipose tissue-derived MSCs, human embryonic stem cell-derived-MSCs (hESC-MSCs) offer an unlimited source of stable and highly-characterized cells that are easily scalable. Here, we studied the effects of human hemangioblast-derived mesenchymal cells (HMCs), (i.e., MSCs differentiated from hESCs using a hemangioblast intermediate), on islet cell transplantation using a minimal islet mass model. The co-transplantation of the HMCs allowed a mass of islets that was insufficient to correct diabetes on its own to restore glycemic control in all recipients. Our in vitro studies help to elucidate the mechanisms including reduction of cytokine stress by which the HMCs support islet graft protection in vivo . Derivation, stability, and scalability of the HMC source may offer unique advantages for clinical applications, including fewer islets needed for successful islet transplantation.
机译:胰岛移植可以恢复1型糖尿病患者的血糖控制。使用此程序,植入的早期阶段通常对长期胰岛功能至关重要,结果并不总是成功。许多研究表明,间充质干细胞(MSCs)促进了胰岛接枝函数。然而,由于与MSC生成(包括供体特性和组织源)相关的变量,实验数据可以不一致,从而证明在翻译到诊所之前对具有良好表征和均匀细胞产品的变量不一致。与骨髓或脂肪组织衍生的MSCs不同,人胚胎干细胞衍生的MSCs(HESC-MSCs)提供易于可扩展的稳定和高表征细胞的无限源。在这里,我们研究了使用最小胰岛质量模型对胰岛细胞移植的人血管血管衍生的间充质细胞(I.,MSCs,从HMCS)的影响。 HMC的共同移植允许大量的胰岛,这不足以纠正糖尿病,以恢复所有接受者的血糖控制。我们的体外研究有助于阐明包括减少细胞因子应力的机制,其中HMCS支持体内胰岛接枝保护。 HMC源的衍生,稳定性和可扩展性可以为临床应用提供独特的优势,包括成功胰岛移植所需的少量胰岛。

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