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人体组织工程气管中的氧传递。

Oxygen mass transfer in a human tissue-engineered trachea.

机构信息

Institute on Membrane Technology, National Research Council of Italy, ITM-CNR, c/o University of Calabria, Via P. Bucci cubo 17/C, I-87030 Rende (CS), Italy.

出版信息

Biomaterials. 2010 Jul;31(19):5131-6. doi: 10.1016/j.biomaterials.2010.03.013. Epub 2010 Apr 8.

Abstract

On June 2008, the first human tissue-engineered trachea replacement was performed using decellularized (de-antigenised) cadaveric donor trachea, seeded with recipient epithelial cells on the internal surface of the graft and mesenchymal stem-cell-derived chondrocytes on the external. During the follow-up, cytological analysis at 4 postoperative days showed a migration of the stem-cells derived chondrocytes from the outer to the inner surface of the first 2 cm of the graft length. With the aim to rationalize these clinical findings, and under the hypothesis that cellular migration is driven by the oxygen gradients developing from the external part of the construct (exposed to O(2) deficiency) towards the better oxygenated epithelial region, an accurate computational model of oxygen transport in the trachea engineered construct was developed and solved using finite element method (FEM). Results confirm that critical limitation to oxygen transport prevalently occurs from proximal to middle section, within the first 2.8 cm of longitudinal length, in good agreement with experimental observation. In the proximal section, recognized as the most critical part of the engineered construct, the severe O(2) mass transfer limitation causes a drastic reduction of the diffusive flux within a distance of 650 microm. At cell density of 1 x 10(7)cells/cm(3), the 30% c.a of the total section area is under oxygen deficiency (O(2) partial pressure below the critical threshold of 38 mmHg). Along the whole tracheal construct, the Thiele modulus ranges within 2.3 and 3.7 in the external chondrocyte compartment, confirming thus the importance of the mass transfer limitation to oxygen diffusion rate. In general, the efficiency of the O(2) transport reduces considerably in the region close to proximal section.

摘要

2008 年 6 月,首次使用脱细胞(去抗原)尸体供体气管进行了人类组织工程气管置换,在移植物的内部表面接种受体上皮细胞,并在外部接种间充质干细胞衍生的软骨细胞。在随访期间,术后 4 天的细胞学分析显示,干细胞衍生的软骨细胞从移植物长度的前 2 厘米的外表面向内表面迁移。为了合理化这些临床发现,并假设细胞迁移是由从构建物外部(暴露于缺氧)向更好氧的上皮区域发展的氧梯度驱动的,我们开发了一种气管工程构建物中氧传输的精确计算模型,并使用有限元方法 (FEM) 进行了解决。结果证实,氧气传输的主要限制主要发生在近端到中段,在第一个 2.8 厘米的纵向长度内,与实验观察结果非常吻合。在近端部分,被认为是工程构建物最关键的部分,严重的 O(2)质量传递限制导致扩散通量在距离 650 微米的范围内急剧下降。在细胞密度为 1 x 10(7)cells/cm(3)时,总截面积的 30% c.a 处于缺氧状态(O(2)分压低于 38 mmHg 的临界阈值)。在整个气管构建物中,外部软骨细胞区的 Thiele 模量在 2.3 到 3.7 之间,这证实了质量传递限制对氧扩散率的重要性。一般来说,靠近近端的区域,O(2)传输的效率会大大降低。

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