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利用两栖动物和小鼠未分化细胞的多器官体外诱导系统阐明激活素在器官发生中的作用。

Elucidation of the role of activin in organogenesis using a multiple organ induction system with amphibian and mouse undifferentiated cells in vitro.

作者信息

Asashima Makoto, Michiue Tatsuo, Kurisaki Akira

机构信息

Organ Development Research Laboratory, National Institute of Advanced Industrial Science and Technology (AIST) 1-1-1, Higashi, Tsukuba-city, Ibaraki, Japan.

出版信息

Dev Growth Differ. 2008 Jun;50 Suppl 1:S35-45. doi: 10.1111/j.1440-169X.2008.00990.x. Epub 2008 Apr 22.

Abstract

Studies performed over the last century have clarified the mechanisms of organ and tissue formation. Mesoderm formation is one of the most important events in early body pattern determination during embryogenesis. In 1988, we found that activin A has mesoderm-inducing activity. As activin A could induce dorsal mesoderm formation, unlike fibroblast growth factor and bone morphogenetic protein, this factor was thought to be the molecular entity of the Spemann-Mangold organizer. Subsequently, the mechanisms of early embryogenesis have been clarified using molecular biological techniques, resulting in the identification of many genes that are involved in organ and tissue development. This finding that activin A could induce dorsal mesoderm formation spurred research into the application of agents that induce organs and tissues in vitro. In this regard, we have shown that many organ types can be induced by activin A in vitro. Moreover, we have found that other types of organs can be induced by changing the conditions of treatment. To date, more than 20 different types of tissues and organs have been successfully induced from Xenopus undifferentiated cells in vitro. In recent years, we have applied these protocols to mouse embryonic stem cells, and we have successfully induced several tissues, such as the pancreas and cardiomyocytes. We are also investigating how the pluripotency of undifferentiated stem cells is regulated. In this review, we summarize the current knowledge regarding activin as a mesoderm-inducing factor and its application for the induction of tissues and organs from undifferentiated cells. Moreover, we provide some examples of in vitro tissue differentiation from mouse embryonic stem cells, which may prove useful in regenerative medicine.

摘要

过去一个世纪进行的研究阐明了器官和组织形成的机制。中胚层形成是胚胎发育早期身体模式确定过程中最重要的事件之一。1988年,我们发现激活素A具有诱导中胚层的活性。由于激活素A能够诱导背侧中胚层形成,与成纤维细胞生长因子和骨形态发生蛋白不同,该因子被认为是施佩曼-曼戈尔德组织者的分子实体。随后,利用分子生物学技术阐明了早期胚胎发育的机制,从而鉴定出许多参与器官和组织发育的基因。激活素A能够诱导背侧中胚层形成这一发现激发了对体外诱导器官和组织的试剂应用的研究。在这方面,我们已经表明激活素A在体外能够诱导多种器官类型。此外,我们发现通过改变处理条件可以诱导其他类型的器官。迄今为止,已经成功地从非洲爪蟾未分化细胞体外诱导出20多种不同类型的组织和器官。近年来,我们将这些方案应用于小鼠胚胎干细胞,并成功诱导出了几种组织,如胰腺和心肌细胞。我们还在研究未分化干细胞的多能性是如何被调控的。在这篇综述中,我们总结了关于激活素作为中胚层诱导因子的当前知识及其在从未分化细胞诱导组织和器官方面的应用。此外,我们提供了一些从小鼠胚胎干细胞进行体外组织分化的例子,这可能在再生医学中证明是有用的。

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