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P53 functional abnormality in mesenchymal stem cells promotes osteosarcoma development

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posted on 2016-04-25, 15:58 authored by T. Velletri, N. Xie, Y. Wang, Y. Huang, Q. Yang, X. Chen, Q. Chen, P. Shou, Y. Gan, G. Cao, G. Melino, Y. Shi
It has been shown that p53 has a critical role in the differentiation and functionality of various multipotent progenitor cells. P53 mutations can lead to genome instability and subsequent functional alterations and aberrant transformation of mesenchymal stem cells (MSCs). The significance of p53 in safeguarding our body from developing osteosarcoma (OS) is well recognized. During bone remodeling, p53 has a key role in negatively regulating key factors orchestrating the early stages of osteogenic differentiation of MSCs. Interestingly, changes in the p53 status can compromise bone homeostasis and affect the tumor microenvironment. This review aims to provide a unique opportunity to study the p53 function in MSCs and OS. In the context of loss of function of p53, we provide a model for two sources of OS: MSCs as progenitor cells of osteoblasts and bone tumor microenvironment components. Standing at the bone remodeling point of view, in this review we will first explain the determinant function of p53 in OS development. We will then summarize the role of p53 in monitoring MSC fidelity and in regulating MSC differentiation programs during osteogenesis. Finally, we will discuss the importance of loss of p53 function in tissue microenvironment. We expect that the information provided herein could lead to better understanding and treatment of OS.

History

Citation

Cell Death and Disease (2016) 7, e2015

Version

  • VoR (Version of Record)

Published in

Cell Death and Disease (2016) 7

Publisher

Nature Publishing Group for Associazione Differenziamento e Morte Cellulare

issn

2041-4889

eissn

2041-4889

Acceptance date

2015-11-13

Available date

2016-04-25

Publisher version

http://www.nature.com/cddis/journal/v7/n1/abs/cddis2015367a.html

Language

en

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