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转铁蛋白与牙齿形态发生:器官培养中小鼠胚胎牙齿对转铁蛋白的保留

Transferrin and tooth morphogenesis: retention of transferrin by mouse embryonic teeth in organ culture.

作者信息

Partanen A M, Thesleff I

出版信息

Differentiation. 1987;34(1):25-31. doi: 10.1111/j.1432-0436.1987.tb00047.x.

DOI:10.1111/j.1432-0436.1987.tb00047.x
PMID:3609531
Abstract

Transferrin is the only serum protein that is required for the early morphogenesis of mouse embryonic teeth in organ culture. Transferrin is able to support tooth morphogenesis and dental cell differentiation by stimulating cell proliferation. Its role in this process is restricted exclusively to iron transport, which takes place by receptor-mediated endocytosis of iron-loaded transferrin. A lipophilic iron chelator, pyridoxal isonicotinoyl hydrazone (PIH), can replace transferrin and support tooth morphogenesis in organ culture. We studied the effects of these two iron transporters on cell proliferation in tooth germs during culture. We found that Fe-PIH and transferrin stimulate proliferation to a similar extent in early cap-stage teeth of 14-day mouse embryos, but have no effect on cell proliferation in bell-stage teeth of 16-day mouse embryos. Day-16 teeth undergo morphogenesis in unsupplemented chemically defined medium, whereas transferrin or Fe-PIH is needed for the morphogenesis of day-14 teeth. Although the need for exogenous iron-transport molecules is lost with advancing development, the level of mitotic activity is still fairly high in bell-stage teeth. The abundant binding of transferrin in areas of active cell proliferation in bell-stage teeth also suggests that transferrin is still needed and used for the transport of iron into proliferating cells. Transferrin is not degraded by the process of receptor-mediated endocytosis. After releasing iron into a cell, transferrin is returned to the extracellular space and is reused. We therefore studied whether the transferrin needed by bell-stage teeth could be adequately supplied by endogenous transferrin synthesized or stored in tissue explants.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

转铁蛋白是器官培养中小鼠胚胎牙齿早期形态发生所必需的唯一血清蛋白。转铁蛋白能够通过刺激细胞增殖来支持牙齿形态发生和牙细胞分化。其在这一过程中的作用仅局限于铁转运,铁转运通过铁负载转铁蛋白的受体介导内吞作用进行。一种亲脂性铁螯合剂,吡哆醛异烟酰腙(PIH),可以替代转铁蛋白并支持器官培养中的牙齿形态发生。我们研究了这两种铁转运蛋白在培养过程中对牙胚细胞增殖的影响。我们发现,在14天龄小鼠胚胎的早期帽状期牙齿中,Fe-PIH和转铁蛋白对增殖的刺激程度相似,但对16天龄小鼠胚胎钟状期牙齿的细胞增殖没有影响。16天龄的牙齿在未添加成分的化学限定培养基中进行形态发生,而14天龄牙齿的形态发生则需要转铁蛋白或Fe-PIH。尽管随着发育进程对外部铁转运分子的需求消失,但钟状期牙齿中的有丝分裂活性水平仍然相当高。转铁蛋白在钟状期牙齿活跃细胞增殖区域的大量结合也表明,转铁蛋白仍然是必需的,并用于将铁转运到增殖细胞中。转铁蛋白不会通过受体介导的内吞作用过程被降解。将铁释放到细胞中后,转铁蛋白会回到细胞外空间并被重新利用。因此,我们研究了钟状期牙齿所需的转铁蛋白是否可以由组织外植体合成或储存的内源性转铁蛋白充分提供。(摘要截取自250词)

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