TNF-α Mediates Diabetes-Enhanced Chondrocyte Apoptosis During Fracture Healing and Stimulates Chondrocyte Apoptosis Through FOXO1

To gain insight into the effect of diabetes on fracture healing, experiments were carried out focusing on chondrocyte apoptosis during the transition from cartilage to bone. Type 1 diabetes was induced in mice by multiple low-dose streptozotocin injections, and simple transverse fractures of the tib...

Descripción completa

Detalles Bibliográficos
Autores principales: Kayal, Rayyan A, Siqueira, Michelle, Alblowi, Jazia, McLean, Jody, Krothapalli, Nanarao, Faibish, Dan, Einhorn, Thomas A, Gerstenfeld, Louis C, Graves, Dana T
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Wiley Subscription Services, Inc., A Wiley Company 2010
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3154002/
https://www.ncbi.nlm.nih.gov/pubmed/20200974
http://dx.doi.org/10.1002/jbmr.59
_version_ 1782209970417172480
author Kayal, Rayyan A
Siqueira, Michelle
Alblowi, Jazia
McLean, Jody
Krothapalli, Nanarao
Faibish, Dan
Einhorn, Thomas A
Gerstenfeld, Louis C
Graves, Dana T
author_facet Kayal, Rayyan A
Siqueira, Michelle
Alblowi, Jazia
McLean, Jody
Krothapalli, Nanarao
Faibish, Dan
Einhorn, Thomas A
Gerstenfeld, Louis C
Graves, Dana T
author_sort Kayal, Rayyan A
collection PubMed
description To gain insight into the effect of diabetes on fracture healing, experiments were carried out focusing on chondrocyte apoptosis during the transition from cartilage to bone. Type 1 diabetes was induced in mice by multiple low-dose streptozotocin injections, and simple transverse fractures of the tibia or femur was carried out. Large-scale transcriptional profiling and gene set enrichment analysis were performed to examine apoptotic pathways on total RNA isolated from fracture calluses on days 12, 16, and 22, a period of endochondral bone formation when cartilage is resorbed and chondrocyte numbers decrease. Tumor necrosis factor α (TNF-α) protein levels were assessed by ELISA and caspase-3 by bioactivity assay. The role of TNF was examined by treating mice with the TNF-specific inhibitor pegsunercept. In vitro studies investigated the proapoptotic transcription factor FOXO1 in regulating TNF-induced apoptosis of chondrogenic ATDC5 and C3H10T1/2 cells as representative of differentiated chondrocytes, which are important during endochondral ossification. mRNA profiling revealed an upregulation of gene sets related to apoptosis in the diabetic group on day 16 when cartilage resorption is active but not day 12 or day 22. This coincided with elevated TNF-α protein levels, chondrocyte apoptosis, enhanced caspase-3 activity, and increased FOXO1 nuclear translocation (p < .05). Inhibition of TNF significantly reduced these parameters in the diabetic mice but not in normoglycemic control mice (p < .05). Silencing FOXO1 using siRNA in vitro significantly reduced TNF-induced apoptosis and caspase activity in differentiated chondrocytes. The mRNA levels of the proapoptotic genes caspase-3, caspase-8, caspase-9, and TRAIL were significantly reduced with silencing of FOXO1 in chondrocytic cells. Inhibiting caspase-8 and caspase-9 significantly reduced TNF-induced apoptosis in chondrogenic cells. These results suggest that diabetes causes an upregulation of proapoptotic genes during the transition from cartilage to bone in fracture healing. Diabetes increased chondrocyte apoptosis through a mechanism that involved enhanced production of TNF-α, which stimulates chondrocyte apoptosis and upregulates mRNA levels of apoptotic genes through FOXO1 activation. © 2010 American Society for Bone and Mineral Research.
format Online
Article
Text
id pubmed-3154002
institution National Center for Biotechnology Information
language English
publishDate 2010
publisher Wiley Subscription Services, Inc., A Wiley Company
record_format MEDLINE/PubMed
spelling pubmed-31540022011-08-19 TNF-α Mediates Diabetes-Enhanced Chondrocyte Apoptosis During Fracture Healing and Stimulates Chondrocyte Apoptosis Through FOXO1 Kayal, Rayyan A Siqueira, Michelle Alblowi, Jazia McLean, Jody Krothapalli, Nanarao Faibish, Dan Einhorn, Thomas A Gerstenfeld, Louis C Graves, Dana T J Bone Miner Res Original Article To gain insight into the effect of diabetes on fracture healing, experiments were carried out focusing on chondrocyte apoptosis during the transition from cartilage to bone. Type 1 diabetes was induced in mice by multiple low-dose streptozotocin injections, and simple transverse fractures of the tibia or femur was carried out. Large-scale transcriptional profiling and gene set enrichment analysis were performed to examine apoptotic pathways on total RNA isolated from fracture calluses on days 12, 16, and 22, a period of endochondral bone formation when cartilage is resorbed and chondrocyte numbers decrease. Tumor necrosis factor α (TNF-α) protein levels were assessed by ELISA and caspase-3 by bioactivity assay. The role of TNF was examined by treating mice with the TNF-specific inhibitor pegsunercept. In vitro studies investigated the proapoptotic transcription factor FOXO1 in regulating TNF-induced apoptosis of chondrogenic ATDC5 and C3H10T1/2 cells as representative of differentiated chondrocytes, which are important during endochondral ossification. mRNA profiling revealed an upregulation of gene sets related to apoptosis in the diabetic group on day 16 when cartilage resorption is active but not day 12 or day 22. This coincided with elevated TNF-α protein levels, chondrocyte apoptosis, enhanced caspase-3 activity, and increased FOXO1 nuclear translocation (p < .05). Inhibition of TNF significantly reduced these parameters in the diabetic mice but not in normoglycemic control mice (p < .05). Silencing FOXO1 using siRNA in vitro significantly reduced TNF-induced apoptosis and caspase activity in differentiated chondrocytes. The mRNA levels of the proapoptotic genes caspase-3, caspase-8, caspase-9, and TRAIL were significantly reduced with silencing of FOXO1 in chondrocytic cells. Inhibiting caspase-8 and caspase-9 significantly reduced TNF-induced apoptosis in chondrogenic cells. These results suggest that diabetes causes an upregulation of proapoptotic genes during the transition from cartilage to bone in fracture healing. Diabetes increased chondrocyte apoptosis through a mechanism that involved enhanced production of TNF-α, which stimulates chondrocyte apoptosis and upregulates mRNA levels of apoptotic genes through FOXO1 activation. © 2010 American Society for Bone and Mineral Research. Wiley Subscription Services, Inc., A Wiley Company 2010-07 2010-02-08 /pmc/articles/PMC3154002/ /pubmed/20200974 http://dx.doi.org/10.1002/jbmr.59 Text en Copyright © 2010 American Society for Bone and Mineral Research http://creativecommons.org/licenses/by/2.5/ Re-use of this article is permitted in accordance with the Creative Commons Deed, Attribution 2.5, which does not permit commercial exploitation.
spellingShingle Original Article
Kayal, Rayyan A
Siqueira, Michelle
Alblowi, Jazia
McLean, Jody
Krothapalli, Nanarao
Faibish, Dan
Einhorn, Thomas A
Gerstenfeld, Louis C
Graves, Dana T
TNF-α Mediates Diabetes-Enhanced Chondrocyte Apoptosis During Fracture Healing and Stimulates Chondrocyte Apoptosis Through FOXO1
title TNF-α Mediates Diabetes-Enhanced Chondrocyte Apoptosis During Fracture Healing and Stimulates Chondrocyte Apoptosis Through FOXO1
title_full TNF-α Mediates Diabetes-Enhanced Chondrocyte Apoptosis During Fracture Healing and Stimulates Chondrocyte Apoptosis Through FOXO1
title_fullStr TNF-α Mediates Diabetes-Enhanced Chondrocyte Apoptosis During Fracture Healing and Stimulates Chondrocyte Apoptosis Through FOXO1
title_full_unstemmed TNF-α Mediates Diabetes-Enhanced Chondrocyte Apoptosis During Fracture Healing and Stimulates Chondrocyte Apoptosis Through FOXO1
title_short TNF-α Mediates Diabetes-Enhanced Chondrocyte Apoptosis During Fracture Healing and Stimulates Chondrocyte Apoptosis Through FOXO1
title_sort tnf-α mediates diabetes-enhanced chondrocyte apoptosis during fracture healing and stimulates chondrocyte apoptosis through foxo1
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3154002/
https://www.ncbi.nlm.nih.gov/pubmed/20200974
http://dx.doi.org/10.1002/jbmr.59
work_keys_str_mv AT kayalrayyana tnfamediatesdiabetesenhancedchondrocyteapoptosisduringfracturehealingandstimulateschondrocyteapoptosisthroughfoxo1
AT siqueiramichelle tnfamediatesdiabetesenhancedchondrocyteapoptosisduringfracturehealingandstimulateschondrocyteapoptosisthroughfoxo1
AT alblowijazia tnfamediatesdiabetesenhancedchondrocyteapoptosisduringfracturehealingandstimulateschondrocyteapoptosisthroughfoxo1
AT mcleanjody tnfamediatesdiabetesenhancedchondrocyteapoptosisduringfracturehealingandstimulateschondrocyteapoptosisthroughfoxo1
AT krothapallinanarao tnfamediatesdiabetesenhancedchondrocyteapoptosisduringfracturehealingandstimulateschondrocyteapoptosisthroughfoxo1
AT faibishdan tnfamediatesdiabetesenhancedchondrocyteapoptosisduringfracturehealingandstimulateschondrocyteapoptosisthroughfoxo1
AT einhornthomasa tnfamediatesdiabetesenhancedchondrocyteapoptosisduringfracturehealingandstimulateschondrocyteapoptosisthroughfoxo1
AT gerstenfeldlouisc tnfamediatesdiabetesenhancedchondrocyteapoptosisduringfracturehealingandstimulateschondrocyteapoptosisthroughfoxo1
AT gravesdanat tnfamediatesdiabetesenhancedchondrocyteapoptosisduringfracturehealingandstimulateschondrocyteapoptosisthroughfoxo1

Ejemplares similares