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在糖尿病 Wistar 大鼠模型中,探讨间充质干细胞存在时,高血糖症和胰岛包封对生物人工胰腺内氧合的影响。

The impact of hyperglycemia and the presence of encapsulated islets on oxygenation within a bioartificial pancreas in the presence of mesenchymal stem cells in a diabetic Wistar rat model.

机构信息

Aspirant of FRS-FNRS, Belgium.

出版信息

Biomaterials. 2011 Sep;32(26):5945-56. doi: 10.1016/j.biomaterials.2011.02.061. Epub 2011 Jun 14.

Abstract

This study investigates the potential of bone marrow (BM-MSCs) versus adipose mesenchymal stem cells (AMSCs) to potentiate the oxygenation of encapsulated islets in a subcutaneous bioartificial pancreas. Oxygen pressures (inside subcutaneous implants) were followed in vivo (by electronic paramagnetic resonance) in non-diabetic/diabetic rats transplanted with encapsulated porcine islets or empty implants up to 4 weeks post-transplantation. After graft explantation, neoangiogenesis surrounding the implants was assessed by histomorphometry. Angiogenic properties of BM-MSCs and AMSCs were first assessed in vitro by incubation of the cells in hypoxia chambers, under normoxic/hypoxic and hypo-/hyperglycemic conditions, followed by quantification of vascular endothelial growth factor (VEGF) release. Second, the in vivo aspect was studied by subcutaneous transplantation of encapsulated BM-MSCs and AMSCs in diabetic rats and assessment of the cells' angiogenic properties as described above. Diabetic state and islet encapsulation induced a significant decrease of oxygenation of the subcutaneous implant and an increased number of cells expressing VEGF. AMSCs demonstrated a significantly higher VEGF secretion than BM-MSCs in vitro. In vivo, AMSCs improved the implant's oxygenation and vascularization. Diabetes and islet encapsulation significantly reduced the oxygenation of a subcutaneous bioartificial pancreas. AMSCs can improve oxygenation by VEGF release in hypoxia and hyperglycemia states.

摘要

本研究旨在探讨骨髓间充质干细胞(BM-MSCs)与脂肪间充质干细胞(AMSCs)在皮下生物人工胰腺中增强包封胰岛氧合的潜力。通过电子顺磁共振在非糖尿病/糖尿病大鼠体内(体内)跟踪移植有或无包封猪胰岛的皮下植入物的氧压,直到移植后 4 周。在移植物取出后,通过组织形态计量学评估植入物周围的新生血管形成。首先通过将细胞在缺氧室中孵育,在常氧/缺氧和低/高血糖条件下,评估 BM-MSCs 和 AMSCs 的血管生成特性,然后定量释放血管内皮生长因子(VEGF),体外评估 BM-MSCs 和 AMSCs 的血管生成特性。其次,通过将包封的 BM-MSCs 和 AMSCs 皮下移植到糖尿病大鼠中,并评估上述细胞的血管生成特性,研究体内情况。糖尿病状态和胰岛包封显著降低了皮下植入物的氧合作用,并增加了表达 VEGF 的细胞数量。AMSCs 在体外比 BM-MSCs 分泌更高的 VEGF。在体内,AMSCs 改善了植入物的氧合和血管化。糖尿病和胰岛包封显著降低了皮下生物人工胰腺的氧合作用。AMSCs 可以通过在缺氧和高血糖状态下释放 VEGF 来改善氧合作用。

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