Adult mesenchymal stem cells: is there a role for purine receptors in their osteogenic differentiation?

被引:0
|
作者
Marzia Carluccio
Sihana Ziberi
Mariachiara Zuccarini
Patricia Giuliani
Francesco Caciagli
Patrizia Di Iorio
Renata Ciccarelli
机构
[1] University of Chieti-Pescara,Department of Medical, Oral and Biotechnological Sciences
[2] University of Chieti-Pescara,Center for Advanced Studies and Technologies (CAST)
[3] StemTeCh Group,undefined
[4] Via L. Polacchi,undefined
来源
Purinergic Signalling | 2020年 / 16卷
关键词
Mesenchymal stem cells/multipotent stromal cells; Bone regenerative medicine; Osteogenic differentiation; Bone repair; Purine receptors;
D O I
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中图分类号
学科分类号
摘要
The role played by mesenchymal stem cells (MSCs) in contributing to adult tissue homeostasis and damage repair thanks to their differentiation capabilities has raised a great interest, mainly in bone regenerative medicine. The growth/function of these undifferentiated cells of mesodermal origin, located in specialized structures (niches) of differentiated organs is influenced by substances present in this microenvironment. Among them, ancestral and ubiquitous molecules such as adenine-based purines, i.e., ATP and adenosine, may be included. Notably, extracellular purine concentrations greatly increase during tissue injury; thus, MSCs are exposed to effects mediated by these agents interacting with their own receptors when they act/migrate in vivo or are transplanted into a damaged tissue. Here, we reported that ATP modulates MSC osteogenic differentiation via different P2Y and P2X receptors, but data are often inconclusive/contradictory so that the ATP receptor importance for MSC physiology/differentiation into osteoblasts is yet undetermined. An exception is represented by P2X7 receptors, whose expression was shown at various differentiation stages of bone cells resulting essential for differentiation/survival of both osteoclasts and osteoblasts. As well, adenosine, usually derived from extracellular ATP metabolism, can promote osteogenesis, likely via A2B receptors, even though findings from human MSCs should be implemented and confirmed in preclinical models. Therefore, although many data have revealed possible effects caused by extracellular purines in bone healing/remodeling, further studies, hopefully performed in in vivo models, are necessary to identify defined roles for these compounds in favoring/increasing the pro-osteogenic properties of MSCs and thereby their usefulness in bone regenerative medicine.
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页码:263 / 287
页数:24
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