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肝祖细胞在三维培养中形成胆管细胞型上皮极性。

Liver progenitor cells develop cholangiocyte-type epithelial polarity in three-dimensional culture.

作者信息

Tanimizu Naoki, Miyajima Atsushi, Mostov Keith E

机构信息

Department of Anatomy, University of California San Francisco, San Francisco, CA 94143-2140, USA.

出版信息

Mol Biol Cell. 2007 Apr;18(4):1472-9. doi: 10.1091/mbc.e06-09-0848. Epub 2007 Feb 21.

Abstract

Cholangiocytes are cellular components of the bile duct system of the liver, which originate from hepatoblasts during embryonic liver development. Although several transcription factors and signaling molecules have been implicated in bile duct development, its molecular mechanism has not been studied in detail. Here, we applied a three-dimensional (3D) culture technique to a liver progenitor cell line, HPPL, to establish an in vitro culture system in which HPPL acquire differentiated cholangiocyte characteristics. When HPPL were grown in a gel containing Matrigel, which contains extracellular matrix components of basement membrane, HPPL developed apicobasal polarity and formed cysts, which had luminal space inside. In the cysts, F-actin bundles and atypical protein kinase C were at the apical membrane, E-cadherin was localized at the lateral membrane, and beta-catenin and integrin alpha6 were located at the basolateral membrane. HPPL in cysts expressed cholangiocyte markers, including cytokeratin 19, integrin beta4, and aquaporin-1, but not a hepatocyte marker, albumin. Furthermore, HPPL transported rhodamine 123, a substrate for multidrug resistance gene products, from the basal side to the central lumen. These data indicate that HPPL develop cholangiocyte-type epithelial polarity in 3D culture. Phosphatidylinositol 3-kinase signaling was essential for proliferation and survival of HPPL in culture, whereas laminin-1 was a crucial component of Matrigel for inducing epithelial polarization of HPPL. Because HPPL cysts display structural and functional similarities with bile ducts, the 3D culture of HPPL recapitulates in vivo cholangiocyte differentiation and is useful to study the molecular mechanism of bile duct development in vitro.

摘要

胆管细胞是肝脏胆管系统的细胞组成部分,在胚胎肝脏发育过程中起源于肝母细胞。尽管几种转录因子和信号分子与胆管发育有关,但其分子机制尚未得到详细研究。在这里,我们将三维(3D)培养技术应用于肝祖细胞系HPPL,以建立一个体外培养系统,使HPPL获得分化的胆管细胞特征。当HPPL在含有基质胶的凝胶中生长时(基质胶含有基底膜的细胞外基质成分),HPPL形成了顶-基极性并形成囊肿,囊肿内部有管腔空间。在囊肿中,F-肌动蛋白束和非典型蛋白激酶C位于顶端膜,E-钙黏蛋白定位于侧面膜,β-连环蛋白和整合素α6位于基底外侧膜。囊肿中的HPPL表达胆管细胞标志物,包括细胞角蛋白19、整合素β4和水通道蛋白-1,但不表达肝细胞标志物白蛋白。此外,HPPL将罗丹明123(一种多药耐药基因产物的底物)从基底侧转运至中央管腔。这些数据表明,HPPL在3D培养中形成胆管细胞型上皮极性。磷脂酰肌醇3-激酶信号传导对于培养中HPPL的增殖和存活至关重要,而层粘连蛋白-1是基质胶诱导HPPL上皮极化的关键成分。由于HPPL囊肿与胆管在结构和功能上具有相似性,HPPL的3D培养概括了体内胆管细胞分化情况,有助于在体外研究胆管发育的分子机制。

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