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Functional Maintenance of Differentiated Embryoid Bodies in Microfluidic Systems: A Platform for Personalized Medicine

机译:微流控系统中分化的类胚体功能维持:个性化医学平台

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摘要

Hormone replacement therapies have become important for treating diseases such as premature ovarian failure or menopausal complications. The clinical use of bioidentical hormones might significantly reduce some of the potential risks reportedly associated with the use of synthetic hormones. In the present study, we demonstrate the utility and advantage of a microfluidic chip culture system to enhance the development of personalized, on-demand, treatment modules using embryoid bodies (EBs). Functional EBs cultured on microfluidic chips represent a platform for personalized, patient-specific treatment cassettes that can be cryopreserved until required for treatment. We assessed the viability, differentiation, and functionality of EBs cultured and cryopreserved in this system. During extended microfluidic culture, estradiol, progesterone, testosterone, and anti-müllerian hormone levels were measured, and the expression of differentiated steroidogenic cells was confirmed by immunocytochemistry assay for the ovarian tissue markers anti-müllerian hormone receptor type II, follicle-stimulating hormone receptor, and inhibin β-A and the estrogen biosynthesis enzyme aromatase. Our studies showed that under microfluidic conditions, differentiated steroidogenic EBs continued to secrete estradiol and progesterone at physiologically relevant concentrations (30–120 pg/ml and 150–450 pg/ml, respectively) for up to 21 days. Collectively, we have demonstrated for the first time the feasibility of using a microfluidic chip system with continuous flow for the differentiation and extended culture of functional steroidogenic stem cell-derived EBs, the differentiation of EBs into cells expressing ovarian antigens in a microfluidic system, and the ability to cryopreserve this system with restoration of growth and functionality on thawing. These results present a platform for the development of a new therapeutic system for personalized medicine.
机译:激素替代疗法对于治疗诸如卵巢早衰或更年期并发症等疾病已变得重要。生化激素的临床使用可能会大大减少据报道与使用合成激素相关的一些潜在风险。在本研究中,我们证明了微流控芯片培养系统的实用性和优势,可利用类胚体(EB)增强个性化按需治疗模块的开发。培养在微流控芯片上的功能性EB代表了个性化,针对患者的治疗盒的平台,可以将其冷冻保存直至需要治疗。我们评估了在该系统中培养和冷冻保存的EB的活力,分化和功能。在延长的微流控培养过程中,测量了雌二醇,孕酮,睾丸激素和抗苗勒管激素的水平,并通过免疫细胞化学法检测了卵巢组织标志物II型苗勒管激素受体,促卵泡激素受体的表达,从而证实了类固醇生成细胞的表达。 ,抑制β-A和雌激素生物合成酶芳香酶。我们的研究表明,在微流体条件下,分化的类固醇生成的EBs在生理相关浓度(分别为30–120 pg / ml和150–450 pg / ml)下继续分泌雌二醇和孕酮,长达21天。总的来说,我们首次证明了使用具有连续流的微流控芯片系统进行功能性类固醇生成干细胞衍生的EBs的分化和扩展培养,将EBs分化为在微流体系统中表达卵巢抗原的细胞的可行性,以及能够通过解冻恢复生长和功能来冷冻保存该系统。这些结果为开发用于个性化医学的新治疗系统提供了平台。

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