Block G D, Locker J, Bowen W C, Petersen B E, Katyal S, Strom S C, Riley T, Howard T A, Michalopoulos G K
Department of Pathology, University of Pittsburgh Medical School, Pennsylvania 15261, USA.
J Cell Biol. 1996 Mar;132(6):1133-49. doi: 10.1083/jcb.132.6.1133.
Mature adult parenchymal hepatocytes, typically of restricted capacity to proliferate in culture, can now enter into clonal growth under the influence of hepatocyte growth factor (scatter factor) (HGF/SF), epidermal growth factor (EGF), and transforming growth factor alpha (TGFalpha) in the presence of a new chemically defined medium (HGM). The expanding populations of hepatocytes lose expression of hepatocyte specific genes (albumin, cytochrome P450 IIB1), acquire expression of markers expressed by bile duct epithelium (cytokeratin 19), produce TGFalpha and acidic FGF and assume a very simplified morphologic phenotype by electron microscopy. A major change associated with this transition is the decrease in ratio between transcription factors C/EBPalpha and C/EBPbeta, as well as the emergence in the proliferating hepatocytes of transcription factors AP1, NFkappaB. The liver associated transcription factors HNFI, HNF3, and HNF4 are preserved throughout this process. After population expansion and clonal growth, the proliferating hepatocytes can return to mature hepatocyte phenotype in the presence of EHS gel (Matrigel). This includes complete restoration of electron microscopic structure and albumin expression. The hepatocyte cultures however can instead be induced to form acinar/ductular structures akin to bile ductules (in the presence of HGF/SF and type I collagen). These transformations affect the entire population of the hepatocytes and occur even when DNA synthesis is inhibited. Similar acinar/ductular structures are seen in embryonic liver when HGF/SF and its receptor are expressed at high levels. These findings strongly support the hypothesis that mature hepatocytes can function as or be a source of bipotential facultative hepatic stem cells (hepatoblasts). These studies also provide evidence for the growth factor and matrix signals that govern these complex phenotypic transitions of facultative stem cells which are crucial for recovery from acute and chronic liver injury.
成熟的成年实质肝细胞通常在培养中增殖能力有限,现在在一种新的化学成分明确的培养基(HGM)存在下,在肝细胞生长因子(散射因子)(HGF/SF)、表皮生长因子(EGF)和转化生长因子α(TGFα)的影响下能够进入克隆生长。不断扩增的肝细胞群体失去肝细胞特异性基因(白蛋白、细胞色素P450 IIB1)的表达,获得胆管上皮表达的标志物(细胞角蛋白19)的表达,产生TGFα和酸性FGF,并通过电子显微镜呈现出非常简化的形态表型。与这种转变相关的一个主要变化是转录因子C/EBPα和C/EBPβ之间的比例下降,以及增殖肝细胞中出现转录因子AP1、NFκB。肝脏相关转录因子HNFI、HNF3和HNF4在整个过程中得以保留。在群体扩增和克隆生长后,增殖的肝细胞在EHS凝胶(基质胶)存在下可恢复为成熟肝细胞表型。这包括电子显微镜结构和白蛋白表达的完全恢复。然而,肝细胞培养物反而可被诱导形成类似于胆小管的腺泡/导管样结构(在HGF/SF和I型胶原存在下)。这些转变影响整个肝细胞群体,甚至在DNA合成受到抑制时也会发生。当HGF/SF及其受体高水平表达时,在胚胎肝脏中可见类似的腺泡/导管样结构。这些发现有力地支持了这样一种假说,即成熟肝细胞可作为双能兼性肝干细胞(成肝细胞)发挥作用或成为其来源。这些研究还为控制兼性干细胞这些复杂表型转变的生长因子和基质信号提供了证据,这些转变对于急性和慢性肝损伤的恢复至关重要。
