Impact of FasL Stimulation on Sclerostin Expression and Osteogenic Profile in IDG-SW3 Osteocytes
The Fas ligand (FasL) is known from programmed cell death, the immune system, and recently also from bone homeostasis. As such, Fas signalling is a potential target of anti-osteoporotic treatment based on the induction of osteoclastic cell death. Less attention has been paid to osteocytes, although...
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doaj-afcd12fa2c4f4030b49268ae57091c552021-08-26T13:32:12ZengMDPI AGBiology2079-77372021-08-011075775710.3390/biology10080757Impact of FasL Stimulation on Sclerostin Expression and Osteogenic Profile in IDG-SW3 OsteocytesAdela Kratochvilova0Alice Ramesova1Barbora Vesela2Eva Svandova3Herve Lesot4Reinhard Gruber5Eva Matalova6Laboratory of Odontogenesis and Osteogenesis, Institute of Animal Physiology and Genetics, Academy of Sciences, 60200 Brno, Czech RepublicLaboratory of Odontogenesis and Osteogenesis, Institute of Animal Physiology and Genetics, Academy of Sciences, 60200 Brno, Czech RepublicLaboratory of Odontogenesis and Osteogenesis, Institute of Animal Physiology and Genetics, Academy of Sciences, 60200 Brno, Czech RepublicLaboratory of Odontogenesis and Osteogenesis, Institute of Animal Physiology and Genetics, Academy of Sciences, 60200 Brno, Czech RepublicLaboratory of Odontogenesis and Osteogenesis, Institute of Animal Physiology and Genetics, Academy of Sciences, 60200 Brno, Czech RepublicDepartment of Oral Biology, University Clinic of Dentistry, Medical University Vienna, Sensengasse 2a, 1090 Vienna, AustriaLaboratory of Odontogenesis and Osteogenesis, Institute of Animal Physiology and Genetics, Academy of Sciences, 60200 Brno, Czech RepublicThe Fas ligand (FasL) is known from programmed cell death, the immune system, and recently also from bone homeostasis. As such, Fas signalling is a potential target of anti-osteoporotic treatment based on the induction of osteoclastic cell death. Less attention has been paid to osteocytes, although they represent the majority of cells within the mature bone and are the key regulators. To determine the impact of FasL stimulation on osteocytes, differentiated IDG-SW3 cells were challenged by FasL, and their osteogenic expression profiles were evaluated by a pre-designed PCR array. Notably, the most downregulated gene was the one for sclerostin, which is the major marker of osteocytes and a negative regulator of bone formation. FasL stimulation also led to significant changes (over 10-fold) in the expression of other osteogenic markers: Gdf10, Gli1, Ihh, Mmp10, and Phex. To determine whether these alterations involved caspase-dependent or caspase-independent mechanisms, the IDG-SW3 cells were stimulated by FasL with and without a caspase inhibitor: Q-VD-OPh. The alterations were also detected in the samples treated by FasL along with Q-VD-OPh, pointing to the caspase-independent impact of FasL stimulation. These results contribute to an understanding of the recently emerging pleiotropic effects of Fas/FasL signalling and specify its functions in bone cells.https://www.mdpi.com/2079-7737/10/8/757boneFas/FasL signallingcaspasesosteocyte differentiationnon-apoptotic |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Adela Kratochvilova Alice Ramesova Barbora Vesela Eva Svandova Herve Lesot Reinhard Gruber Eva Matalova |
spellingShingle |
Adela Kratochvilova Alice Ramesova Barbora Vesela Eva Svandova Herve Lesot Reinhard Gruber Eva Matalova Impact of FasL Stimulation on Sclerostin Expression and Osteogenic Profile in IDG-SW3 Osteocytes Biology bone Fas/FasL signalling caspases osteocyte differentiation non-apoptotic |
author_facet |
Adela Kratochvilova Alice Ramesova Barbora Vesela Eva Svandova Herve Lesot Reinhard Gruber Eva Matalova |
author_sort |
Adela Kratochvilova |
title |
Impact of FasL Stimulation on Sclerostin Expression and Osteogenic Profile in IDG-SW3 Osteocytes |
title_short |
Impact of FasL Stimulation on Sclerostin Expression and Osteogenic Profile in IDG-SW3 Osteocytes |
title_full |
Impact of FasL Stimulation on Sclerostin Expression and Osteogenic Profile in IDG-SW3 Osteocytes |
title_fullStr |
Impact of FasL Stimulation on Sclerostin Expression and Osteogenic Profile in IDG-SW3 Osteocytes |
title_full_unstemmed |
Impact of FasL Stimulation on Sclerostin Expression and Osteogenic Profile in IDG-SW3 Osteocytes |
title_sort |
impact of fasl stimulation on sclerostin expression and osteogenic profile in idg-sw3 osteocytes |
publisher |
MDPI AG |
series |
Biology |
issn |
2079-7737 |
publishDate |
2021-08-01 |
description |
The Fas ligand (FasL) is known from programmed cell death, the immune system, and recently also from bone homeostasis. As such, Fas signalling is a potential target of anti-osteoporotic treatment based on the induction of osteoclastic cell death. Less attention has been paid to osteocytes, although they represent the majority of cells within the mature bone and are the key regulators. To determine the impact of FasL stimulation on osteocytes, differentiated IDG-SW3 cells were challenged by FasL, and their osteogenic expression profiles were evaluated by a pre-designed PCR array. Notably, the most downregulated gene was the one for sclerostin, which is the major marker of osteocytes and a negative regulator of bone formation. FasL stimulation also led to significant changes (over 10-fold) in the expression of other osteogenic markers: Gdf10, Gli1, Ihh, Mmp10, and Phex. To determine whether these alterations involved caspase-dependent or caspase-independent mechanisms, the IDG-SW3 cells were stimulated by FasL with and without a caspase inhibitor: Q-VD-OPh. The alterations were also detected in the samples treated by FasL along with Q-VD-OPh, pointing to the caspase-independent impact of FasL stimulation. These results contribute to an understanding of the recently emerging pleiotropic effects of Fas/FasL signalling and specify its functions in bone cells. |
topic |
bone Fas/FasL signalling caspases osteocyte differentiation non-apoptotic |
url |
https://www.mdpi.com/2079-7737/10/8/757 |
work_keys_str_mv |
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