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In vivo vascularization and islet function in a microwell device for pancreatic islet transplantation

机译:在微孔装置中的体内血管化和胰岛功能,用于胰岛移植

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Islet encapsulation in membrane-based devices could allow for transplantation of donor islet tissue in the absence of immunosuppression. To achieve long-term survival of islets, the device should allow rapid exchange of essential nutrients and be vascularized to guarantee continued support of islet function. Recently, we have proposed a membrane-based macroencapsulation device consisting of a microwell membrane for islet separation covered by a micropatterned membrane lid. The device can prevent islet aggregation and support functional islet survival in vitro. Here, based on previous modeling studies, we develop an improved device with smaller microwell dimensions, decreased spacing between the microwells and reduced membrane thickness and investigate its performance in vitro and in vivo. This improved device allows for encapsulating higher islet numbers without islet aggregation and by applying an in vivo imaging system we demonstrate very good perfusion of the device when implanted intraperitoneally in mice. Besides, when it is implanted subcutaneously in mice, islet viability is maintained and a vascular network in close proximity to the device is developed. All these important findings demonstrate the potential of this device for islet transplantation.
机译:在基于膜的器件中的胰岛封装可以允许在没有免疫抑制的情况下移植供体胰岛组织。为了达到胰岛的长期存活,该装置应允许快速交换必需营养,并致血管化,以保证对胰岛功能的持续支持。最近,我们提出了一种基于膜的宏观型涂布装置,其由微孔膜组成,用于被微型膜盖覆盖的胰岛分离。该装置可以防止胰岛聚集并在体外支持功能性胰岛存活。这里,基于先前的建模研究,我们开发一种具有较小微孔尺寸的改进装置,微孔之间的间距降低,膜厚度降低,并在体外和体内调查其性能。该改进的装置允许在没有胰岛聚集的情况下封装更高的胰岛编号,并且通过在体内成像系统中应用,我们在小鼠中植入腹膜内植入时,我们证明了装置的非常好的灌注。此外,当皮下植入小鼠中时,胰岛活力被保持,并且开发了近距离该装置的血管网络。所有这些重要的研究结果都证明了该装置对胰岛移植的潜力。

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