Department of Surgery, VA Greater Los Angeles Health Care System, Los Angeles, California 90073, USA.
J Surg Res. 2011 Aug;169(2):169-78. doi: 10.1016/j.jss.2009.11.719. Epub 2009 Dec 16.
Production of tissue engineered small intestine (TESI) has been limited by the relatively large amount of native tissue required to generate neomucosa. The influence of growth factors and three-dimensional (3D) extracellular matrices on TESI has been studied both in vitro and in vivo, and positive growth effects on tissue mass and differentiation were noted. The present study investigates the impact of single doses of glucagon-like peptide-2 (GLP-2), hepatocyte growth factor (HGF), or holo-transferrin adsorbed onto a polyglycolic (PGA) mesh scaffold using a rat small-intestinal organoid transplant model. In Experiment I, intestinal organoids were seeded onto PGA mesh discs, suspended in either Matrigel (n=8) or a vehicle control (n=8), and implanted into syngenic recipients. In Experiment II, GLP-2 (n=8), HGF (n=8), or transferrin (n=8) were adsorbed onto PGA mesh discs. Intestinal organoids were then suspended in Matrigel and seeded onto each growth factor-loaded PGA disc or onto control discs without growth factors (n=12). In addition, organoids were suspended in vehicle and seeded onto control discs (n=12). All discs were implanted into syngenic recipients. After 4 wk, histologic analysis of the samples revealed significantly greater neomucosal surface area (3.62±0.33 mm(2)versus 0.92±0.11 mm(2), P<0.0001) and cyst diameter (2.83±0.14 mm versus 2.06±0.07 mm, P<0.0001) in groups treated with Matrigel compared with vehicle controls. The addition of holo-transferrin to the scaffolds further augmented neomucosal surface area (9.11±0.66 mm(2)versus 3.01±0.22 mm(2), P<0.01), whereas that of GLP-2 stimulated the formation of increased numbers of cysts (8.88±0.46 versus 4.18±0.25, P<0.01). These data suggest that Matrigel and growth factors adsorbed to polymer scaffolds can be used to manipulate the morphology of TESI.
组织工程小肠(TESI)的生产受到生成新黏膜所需的相对大量天然组织的限制。生长因子和三维(3D)细胞外基质对 TESI 的影响已在体外和体内进行了研究,并且观察到对组织质量和分化的积极生长作用。本研究使用大鼠小肠类器官移植模型研究了单次给予胰高血糖素样肽-2(GLP-2)、肝细胞生长因子(HGF)或全转铁蛋白吸附在聚乙醇酸(PGA)网片支架上的影响。在实验 I 中,将肠类器官接种到 PGA 网片上,悬浮在 Matrigel(n=8)或载体对照(n=8)中,并植入同基因受体。在实验 II 中,将 GLP-2(n=8)、HGF(n=8)或转铁蛋白(n=8)吸附到 PGA 网片上。然后将肠类器官悬浮在 Matrigel 中并接种到每种生长因子负载的 PGA 片上或没有生长因子的对照片上(n=12)。此外,将类器官悬浮在载体中并接种到对照片上(n=12)。所有的片子都被植入同基因受体中。4 周后,对样本的组织学分析显示,与载体对照相比,用 Matrigel 处理的组的新黏膜表面积(3.62±0.33 mm(2)与 0.92±0.11 mm(2),P<0.0001)和囊泡直径(2.83±0.14 mm 与 2.06±0.07 mm,P<0.0001)显著增加。将全转铁蛋白添加到支架中进一步增加了新黏膜表面积(9.11±0.66 mm(2)与 3.01±0.22 mm(2),P<0.01),而 GLP-2 刺激形成了更多数量的囊泡(8.88±0.46 与 4.18±0.25,P<0.01)。这些数据表明,Matrigel 和吸附在聚合物支架上的生长因子可用于操纵 TESI 的形态。
