Inflammation as death or life signal in diabetic fracture healing

Röszer, Tamás

doi:10.1007/s00011-010-0246-9

Cited by 54 publications

(54 citation statements)

References 96 publications

(131 reference statements)

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“…It is probably not the only MAPK pathway involved, since we were unable to completely abrogate the apoptosis of BMSCs with the p38 inhibitor. Since we found no indication that the activation of NF-kB is involved in this process, as it was not attenuated by SN50, other pathways, particularly JNK (Shen et al 2010, Roszer 2011, Shi et al 2013, must be further evaluated.…”

Section: Discussionmentioning

confidence: 88%

“…Previously, AGEs have been shown to induce the production of TNFa in many cell types, including osteoblastic cells (Franke et al 2011, Fernández et al 2013, chondrocytes (Nah et al 2007), and endothelial cells (Rashid et al 2004), so that the idea that AGEs induce the apoptosis of BMSCs via the induction of TNFa expression and secretion seems feasible (Roszer 2011) and is certainly supported by data obtained with pirfenidone treatment.…”

Section: Discussionmentioning

confidence: 88%

“…Navarro & Mora-Fernández (2006), Roszer (2011) and Xu et al (2013)). In addition to TNFa, AGE-BSA increased the mRNA levels of other apoptogenic ligands, such as lymphotoxin alpha (Etemadi et al 2013) and TRAIL (Falschlehner et al 2007).…”

Section: Discussionmentioning

confidence: 99%

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AGEs induce caspase-mediated apoptosis of rat BMSCs via TNFα production and oxidative stress

Weinberg¹,

Maymon²,

Weinreb³

2013

Journal of Molecular Endocrinology

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Diabetic humans and animals exhibit lower bone mass and healing, resulting from diminished bone formation. We have recently reported that type 1 diabetic rats have fewer bone marrow osteoprogenitor cells, and since the formation of advanced glycation end products (AGEs) in bone increases in diabetes, we explored possible mechanisms involved in AGE-induced apoptosis of rat bone marrow stromal cells (BMSCs). BMSCs isolated from 4-month-old rats were exposed to 10-400 mg/ml AGE-BSA for 16 h and apoptosis was quantified with PI/annexin V staining and flow cytometry. Signaling mechanisms were evaluated by preincubating the cells with appropriate inhibitors. The formation of reactive oxygen species (ROS) was quantified by flow cytometric analysis of DCFDA fluorescence and the expression of genes by RT-PCR analysis. AGE-BSA at a concentration of 400 mg/ml increased the apoptosis of BMSCs two-to threefold, an effect completely blocked by a pan-caspase inhibitor. BSA or high concentrations of glucose had no effect. AGE-BSA-induced BMSC apoptosis was attenuated by a p38 inhibitor but not by an NF-kB inhibitor. Treatment with AGE-BSA induced the expression of several pro-apoptotic ligands and receptors, most notably tumor necrosis factor a (TNFa), TRAIL, lymphotoxin alpha, CD40, and TNFR2. Furthermore, AGE-BSA-induced apoptosis was completely blocked by pirfenidone, an inhibitor of TNFa production/secretion. Finally, AGE-BSA increased the production of ROS in BMSCs, and its apoptogenic effect was blocked by the antioxidant N-acetylcysteine (N-acetyl-L-cysteine). Thus, AGE-BSA increases the apoptosis of rat BMSCs via the activation of caspases, involving TNFa production/ secretion, p38 MAPK signaling, and oxidative stress. We propose that increased protein glycation, such as that occurring under hyperglycemia, causes the apoptosis of BMSCs, which might significantly contribute to the development of osteopenia in diabetic animals.

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Section: Discussionmentioning

confidence: 88%

Section: Discussionmentioning

confidence: 88%

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AGEs induce caspase-mediated apoptosis of rat BMSCs via TNFα production and oxidative stress

Weinberg¹,

Maymon²,

Weinreb³

2013

Journal of Molecular Endocrinology

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“…Elevated FOXO1 activity in chondrocytes was observed during impaired fracture healing in diabetic rodents, suggesting an enhanced inflammatory response and osteoclastogenesis [29]. FOXO1 may also regulate tumor necrosis factor (TNF alpha), which encourages cell death and inflammatory cytokines [30]. Therefore, elevated FOXO during fracture healing in diabetic patients may result in elevated inflammation, osteoclast activity, and chondrocyte apoptosis, possibly contributing to impaired healing.…”

Section: Insulin Treatment In Type 1 Diabetes Mellitus and Bone Fracturementioning

confidence: 99%

Determining the Role of Sost and Sostdc1 During Fracture Healing

Yee¹

2016

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“…For example, disorders such as diabetes mellitus that are associated with an inflammatory state are also characterized by impaired tissue regeneration. 97 TERM strategies for cartilage regeneration may be compromised as a result of dysregulated inflammatory processes and pro-inflammatory mediators in the joint. IL-1b has been reported to reduce collagen type 2 expression and GAG content of human nasal and articular chondrocytes cultured on a type 1 collagen scaffold, 98 and both IL-1b and TNF-a have been shown to impact the integration of engineered cartilage with native tissue.…”

Section: The Effect Of Inflammation On Tissue Engineered Cartilagementioning

confidence: 99%

Immune Modulation to Improve Tissue Engineering Outcomes for Cartilage Repair in the Osteoarthritic Joint

Fahy

Farrell

Ritter

et al. 2015

Tissue Engineering Part B: Reviews

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Inflammation as death or life signal in diabetic fracture healing

Cited by 54 publications

References 96 publications

AGEs induce caspase-mediated apoptosis of rat BMSCs via TNFα production and oxidative stress

AGEs induce caspase-mediated apoptosis of rat BMSCs via TNFα production and oxidative stress

Determining the Role of Sost and Sostdc1 During Fracture Healing

Immune Modulation to Improve Tissue Engineering Outcomes for Cartilage Repair in the Osteoarthritic Joint

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