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CRISPR-targeted genome editing of mesenchymal stem cell-derived therapies for type 1 diabetes: a path to clinical success?

机译:针对1型糖尿病的间充质干细胞疗法的CRISPR靶向基因组编辑:通往临床成功的道路吗?

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Due to their ease of isolation, differentiation capabilities, and immunomodulatory properties, the therapeutic potential of mesenchymal stem cells (MSCs) has been assessed in numerous pre-clinical and clinical settings. Currently, whole pancreas or islet transplantation is the only cure for people with type 1 diabetes (T1D) and, due to the autoimmune nature of the disease, MSCs have been utilised either natively or transdifferentiated into insulin-producing cells (IPCs) as an alternative treatment. However, the initial success in pre-clinical animal models has not translated into successful clinical outcomes. Thus, this review will summarise the current state of MSC-derived therapies for the treatment of T1D in both the pre-clinical and clinical setting, in particular their use as an immunomodulatory therapy and targets for the generation of IPCs via gene modification. In this review, we highlight the limitations of current clinical trials of MSCs for the treatment of T1D, and suggest the novel clustered regularly interspaced short palindromic repeat (CRISPR) gene-editing technology and improved clinical trial design as strategies to translate pre-clinical success to the clinical setting.
机译:由于其易于分离,分化能力和免疫调节特性,已经在许多临床前和临床环境中评估了间充质干细胞(MSC)的治疗潜力。目前,全胰腺或胰岛移植是1型糖尿病(T1D)患者的唯一治疗方法,由于该疾病的自身免疫性质,MSC已被天然使用或转分化为胰岛素产生细胞(IPC)治疗。但是,临床前动物模型的初步成功并未转化为成功的临床结果。因此,本综述将总结临床前和临床环境中MSC衍生疗法治疗T1D的现状,特别是它们作为免疫调节疗法的用途以及通过基因修饰产生IPC的靶标。在这篇综述中,我们着重介绍了目前用于MSC治疗T1D的临床试验的局限性,并提出了新颖的聚类规则间隔定期短回文重复(CRISPR)基因编辑技术和改进的临床试验设计,作为转化临床前成功的策略到临床环境。

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