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首页> 外文期刊>Tissue engineering, Part C. Methods >In vivo generation of thick, vascularized hepatic tissue from collagen hydrogel-based hepatic units.
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In vivo generation of thick, vascularized hepatic tissue from collagen hydrogel-based hepatic units.

机译:从基于胶原水凝胶的肝单位体内生成厚厚的血管化肝组织。

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In vivo engineering of hepatic tissue based on primary hepatocytes offers new perspectives for the treatment of liver diseases. However, generation of thick, three-dimensional liver tissue has been limited by the lack of vasculature in the tissue-engineered constructs. Here, we used collagen hydrogel as a matrix to generate engineered hepatic units to reconstitute three-dimensional, vascularized hepatic tissue in vivo. Hepatocytes harvested from Sprague-Dawley rats were mixed with liquid type I collagen, concentrated Dulbecco's modified Eagle's medium (2 x), and hepatocyte maintenance medium to create hepatocyte/collagen hydrogel constructs. The constructs were then dissociated into cylindrical hepatic units (diameter/height: 2000-4000 microm/500-1000 microm). Stacking of hepatic units under the subcutaneous space resulted in significant cell engraftment, with the formation of large fused hepatic system (more than 0.5 cm thickness) containing blood vessels. In contrast, only less cell engraftment could be achieved when hepatocytes were transplanted in a manner of whole constructs. Functional maintenance of the engineered hepatic tissue was confirmed by the expression of liver-specific mRNA and proteins. The engineered hepatic tissue has the ability to respond to the regenerative stimulus. In conclusion, large hepatic tissue containing blood vessels could be engineered in vivo by merging small hepatic units. This approach for tissue engineering is simple and represents an efficient way to engineer hepatic tissue in vivo.
机译:基于原代肝细胞的肝组织的体内工程化为肝病的治疗提供了新的视角。但是,由于组织工程构造中缺少脉管系统,因此无法形成厚厚的三维肝脏组织。在这里,我们使用胶原蛋白水凝胶作为基质来生成工程肝单位,以在体内重建三维血管化肝组织。将从Sprague-Dawley大鼠收获的肝细胞与液态I型胶原蛋白,浓缩的Dulbecco改良的Eagle培养基(2 x)和肝细胞维持培养基混合,以创建肝细胞/胶原水凝胶构建体。然后将构建体解离成圆柱形肝单位(直径/高度:2000-4000微米/ 500-1000微米)。皮下空间下肝单位的堆叠导致大量细胞植入,并形成包含血管的大融合肝系统(厚度超过0.5厘米)。相反,当以完整构建体的方式移植肝细胞时,只能实现较少的细胞植入。肝特异性mRNA和蛋白的表达证实了工程肝组织的功能维持。工程肝组织具有对再生刺激作出反应的能力。总之,可以通过合并小的肝单位在体内工程改造包含血管的大肝组织。这种用于组织工程的方法很简单,代表了一种在体内工程化肝组织的有效方法。

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