共查询到19条相似文献,搜索用时 62 毫秒
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肝脏干细胞调控机制的研究进展 总被引:3,自引:0,他引:3
肝脏干细胞在正常肝脏中处于静息状态 ,但当肝脏受到严重损伤和或肝细胞的再生能力受到抑制时 ,肝脏干细胞便活化、增殖并分化为成熟肝细胞及胆管细胞以发挥代偿作用。尽管目前对肝脏干细胞的来源及肝组织内的准确定位还不明确 ,但众多研究己证实肝内肯定存在肝脏干细胞 ,其活化后的子代细胞为卵圆细胞 ,卵圆细胞具备多向分化潜能 ,体内外实验证实其可以分化为肝细胞、胆管细胞、胰腺及肠型上皮 ,1999年Peterson研究证实骨髓细胞可以转化为肝细胞 ,其他学者对骨髓干细胞的体内移植及体外培养的研究中也证实了Peterson的观点… 相似文献
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魏红山 《国外医学:消化系疾病分册》2000,20(3):164-167
尽管肝干细胞研究领域中尚有很多争议,但综合近年来的研究逐步形成以下共识:①肝干细胞定位于胆管系统;②正常肝脏的肝细胞更新和肝损伤修复过程均需肝干细胞参与;③以卵圆细胞为代表的多潜能肝干细胞的功能与肝内微生态平衡密切相关。本综述肝干细胞领域近年来的有关研究进展。 相似文献
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张颖 《国外医学:消化系疾病分册》2002,22(4):224-226
干细胞生物学是人类基因组主这后最有影响力和最有应用前景的生命科学,近年来由于干细胞理论、临床及科研技术的长足发展,在几乎所有的组织中都发现了干细胞。经过多年的研究,特异性肝干细胞的存在已经被广泛接受,本对有关肝干细胞的存在和起源作一综述,并探讨其激活和增殖分化机制及在肝组织修复再生中所起的重要作用。 相似文献
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蒯小玲 《国外医学:消化系疾病分册》2003,23(1):27-29
成年哺乳动物的肝脏中含有许多类型的分化细胞。肝脏干细胞(liver stem cells)是指肝细胞和胆管内皮细胞的前体细胞。它们可以通过自身的对称性和不对称性两种分裂方式进行自我复制,亦即一方面通过分裂产生相同的干细胞维持自身的存在,同时产生肝脏组织中不同发育阶段和不同分化方向的细胞。本不肝脏干细胞的来源、诱导分化、应用等作一综述。 相似文献
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干细胞是指在适当的条件下 ,具有无限自我复制、自我更新以及全能或多能分化能力的细胞群 ,可以分化成多种细胞系并形成各种具有明确功能的组织、器官 ,是形成器官和组织的基础细胞。干细胞分为胚性干细胞和存在于各种组织中的干细胞 ,能在培养液中不断分裂 ,发育成功能各异的细胞 ,如肌肉细胞、神经细胞、心肌细胞、血细胞和其他种类的细胞。一般认为只有取自胚胎的干细胞才有分化成为不同组织的潜力 ,而成年人体内特定部位的干细胞只能发育成为特定组织。干细胞不仅是胚胎细胞必要的组成部分 ,在大多数成熟个体的组织器官中也发现了一定数… 相似文献
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干细胞生物学是人类基因组计划之后最有影响力和最有应用前景的生命科学,近年来由于干细胞理论、临床及科研技术的长足发展,在几乎所有的组织中都发现了干细胞。经过多年的研究,特异性肝干细胞的存在已经被广泛接受,本文对有关肝干细胞的存在和起源作一综述,并探讨其激活和增殖分化机制及在肝组织修复再生中所起的重要作用。 相似文献
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肝干细胞的可塑性及其分化机制的研究在基础和临床应用等方面均有重要意义。一方面,肝干细胞可能参与肝脏损伤的修复与重建,研究肝干细胞的分化机制有助于阐明肝脏的发育机制;另一方面,肝干细胞分化为具有功能的成熟肝细胞,将为肝细胞移植和生物型人工肝提供重要的细胞来源。肝干细胞分化过程和机制较为复杂,肝干细胞分子免疫学的研究将成为肝干细胞研究的一个重要内容,现将其有关近况做一介绍。 相似文献
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肝干细胞的研究现状及其临床应用展望 总被引:5,自引:0,他引:5
1988年Bumgardner等人率先提出了肝细胞移植概念,1993年Mito等在世界上开展了首例人体肝细胞移植。此后,从原位整肝移植到原位肝细胞移植,进而发展到干细胞移植,肝细胞移植治疗技术取得了巨大进展。特别是近年来随着肝干细胞分离、培养、鉴定及其增殖技术的发展和成熟,将多种来源的肝干细胞用作细胞移植、生物人工肝装置以及基因治疗的主要来源细胞,已经引起了广泛关注。 相似文献
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骨髓中主要存在2种主要类型的干细胞:造血干细胞(hematopoietic stem cells,HSC)及非HSC或间充质干细胞(mesenchymal stem cells,MSC)。HSC移植可重建患者造血系统和免疫系统,因此,临床上HSC移植用于治疗各种恶性血液病、遗传性血液病、再生障碍性贫血及免疫缺陷病等。 相似文献
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Toshihiro Mitaka 《Journal of hepato-biliary-pancreatic sciences》2002,9(6):697-703
Recent advances in culture methods, stem cell research, and tissue engineering provide clues for making tissues in vitro that are functionally and structurally similar to hepatic tissues. To reconstruct hepatic organoids, two approaches to establish the methods have been proposed: the use of cells and the combination of cells and a scaffold (called tissue engineering). Recently, the coculture of hepatic cells (mature hepatocytes, small hepatocytes, hepatoblasts) and hepatic nonparenchymal cells has been reported to form hepatic organoids that possess differentiated hepatic functions. On the other hand, hepatocytes in a roller bottle were shown to form specific structures, consisting of biliary epithelial cells, connective tissue, mature hepatocytes, and endothelial cells. In this review, the studies of hepatic tissue formation in vitro will be summarized. 相似文献
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Update on hepatic stem cells 总被引:28,自引:0,他引:28
The liver, like most organs in an adult healthy body, maintains a perfect balance between cell gain and cell loss. Though normally proliferatively quiescent, simple hepatocyte loss such as that caused by partial hepatectomy, uncomplicated by virus infection or inflammation, invokes a rapid regenerative response to restore liver mass. This restoration of moderate cell loss and 'wear and tear' renewal is largely achieved by hepatocyte self-replication. Furthermore, cell transplant models have shown that hepatocytes can undergo significant clonal expansion. Such observations indicate that hepatocytes are the functional stem cells of the liver. More severe liver injury activates a facultative stem cell compartment located within the intrahepatic biliary tree, giving rise to cords of biliary epithelia within the lobules before these cells differentiate into hepatocytes. A third population of stem cells with hepatic potential resides in the bone marrow; these haematopoietic stem cells can contribute to the albeit low renewal rate of hepatocytes, make a more significant contribution to regeneration, and even completely restore normal function in a murine model of hereditary tyrosinaemia. How these three stem cell populations integrate to achieve a homeostatic balance is not understood. This review focuses on three aspects of liver stem cell biology: 1) the hepatic stem cell candidates; 2) models of cell transplantation into the liver; and 3) the therapeutic potential of hepatic stem cells. 相似文献
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Abstract: The liver, like most organs in an adult healthy body, maintains a perfect balance between cell gain and cell loss. Though normally proliferatively quiescent, simple hepatocyte loss such as that caused by partial hepatectomy, uncomplicated by virus infection or inflammation, invokes a rapid regenerative response to restore liver mass. This restoration of moderate cell loss and ‘wear and tear’ renewal is largely achieved by hepatocyte self‐replication. Furthermore, cell transplant models have shown that hepatocytes can undergo significant clonal expansion. Such observations indicate that hepatocytes are the functional stem cells of the liver. More severe liver injury activates a facultative stem cell compartment located within the intrahepatic biliary tree, giving rise to cords of biliary epithelia within the lobules before these cells differentiate into hepatocytes. A third population of stem cells with hepatic potential resides in the bone marrow; these haematopoietic stem cells can contribute to the albeit low renewal rate of hepatocytes, make a more significant contribution to regeneration, and even completely restore normal function in a murine model of hereditary tyrosinaemia. How these three stem cell populations integrate to achieve a homeostatic balance is not understood. This review focuses on three aspects of liver stem cell biology: 1) the hepatic stem cell candidates; 2) models of cell transplantation into the liver; and 3) the therapeutic potential of hepatic stem cells. 相似文献