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体外分化肝细胞的形态学研究。

A morphological study of differentiated hepatocytes in vitro.

作者信息

Arterburn L M, Zurlo J, Yager J D, Overton R M, Heifetz A H

机构信息

W. R. Grace & Co.-Conn., Research Division, Columbia, MD 21044, USA.

出版信息

Hepatology. 1995 Jul;22(1):175-87.

PMID:7601410
Abstract

A problem traditionally encountered with primary hepatocyte cultures is their rapid dedifferentiation, which is reflected not only in decreased liver-specific functions, but also in dedifferentiated morphology: the cells flatten, depolarize, and lose many of the surface characteristics of normal hepatocytes in vivo. However, culture conditions that maintain primary rat hepatocytes in a healthy and highly differentiated state were recently developed: the hepatocytes are cultured in Chee's Medium supplemented with dexamethasone and dimethyl sulfoxide (DMSO) on collagen-coated Permanox dishes. In addition to retaining labile hepatocyte-specific functions (e.g., P450 activity and albumin synthesis), these hepatocytes also have a differentiated morphology. They have numerous microvilli and are cuboidal and cluster into cords reminiscent of hepatic trabeculae. Their subcellular organelles have normal morphology, and specialized junctions and bile canaliculi form within the membranes of adjacent cells. Actin fibers cluster at these canalicular surfaces. These hepatocytes also synthesize blood clotting factors, which aggregate into fibrin meshworks between cells. Taken together, these morphological data suggest that these hepatocytes are polarized and generally have an appearance very similar to parenchymal cells in the liver, and that the same culture conditions that promote retention of liver-specific functions are also critical to the maintenance of physiological morphology. In contrast to other hepatocyte cultures, this differentiated morphology, including the polarized nature of the cells, is established without the use of serum or flexible or complex extracellular matrices and shows a close link between cellular architecture and tissue-specific function.

摘要

原代肝细胞培养传统上遇到的一个问题是其迅速去分化,这不仅体现在肝脏特异性功能的下降,还体现在去分化的形态上:细胞变平、去极化,并失去了体内正常肝细胞的许多表面特征。然而,最近开发出了能使原代大鼠肝细胞维持在健康且高度分化状态的培养条件:肝细胞在补充了地塞米松和二甲基亚砜(DMSO)的Chee培养基中,于胶原包被的Permanox培养皿上进行培养。除了保留不稳定的肝细胞特异性功能(如细胞色素P450活性和白蛋白合成)外,这些肝细胞还具有分化的形态。它们有许多微绒毛,呈立方形,聚集成索状,让人联想到肝小梁。它们的亚细胞器形态正常,相邻细胞的膜内形成了特殊的连接和胆小管。肌动蛋白纤维聚集在这些胆小管表面。这些肝细胞还合成血液凝固因子,这些因子在细胞间聚集成纤维蛋白网络。综合这些形态学数据表明,这些肝细胞是极化的,总体外观与肝脏实质细胞非常相似,并且促进肝脏特异性功能保留的相同培养条件对于维持生理形态也至关重要。与其他肝细胞培养不同,这种分化的形态,包括细胞的极化性质,是在不使用血清或灵活或复杂的细胞外基质的情况下建立的,并且显示出细胞结构与组织特异性功能之间的紧密联系。

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