转分化
生物
化生
导管细胞
内斯汀
胰腺
细胞生物学
病理
癌症研究
干细胞
内分泌学
医学
神经干细胞
作者
Anna L. Means,Ingrid M. Meszoely,Kazufumi Suzuki,Yoshiharu Miyamoto,Anil K. Rustgi,Robert J. Coffey,Christopher V.E. Wright,Doris A. Stoffers,Steven D. Leach
出处
期刊:Development
[The Company of Biologists]
日期:2005-07-15
卷期号:132 (16): 3767-3776
被引量:329
摘要
Epithelial metaplasia occurs when one predominant cell type in a tissue is replaced by another, and is frequently associated with an increased risk of subsequent neoplasia. In both mouse and human pancreas, acinar-to-ductal metaplasia has been implicated in the generation of cancer precursors. We show that pancreatic epithelial explants undergo spontaneous acinar-to-ductal metaplasia in response to EGFR signaling, and that this change in epithelial character is associated with the appearance of nestin-positive transitional cells. Lineage tracing involving Cre/lox-mediated genetic cell labeling reveals that acinar-to-ductal metaplasia represents a true transdifferentiation event, mediated by initial dedifferentiation of mature exocrine cells to generate a population of nestin-positive precursors, similar to those observed during early pancreatic development. These results demonstrate that a latent precursor potential resides within mature exocrine cells, and that this potential is regulated by EGF receptor signaling. In addition, these observations provide a novel example of rigorously documented transdifferentiation within mature mammalian epithelium, and suggest that plasticity of mature cell types may play a role in the generation of neoplastic precursors.
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