Varying butyric acid amounts induce different stress- and cell death-related signals in nerve growth factor-treated PC12 cells: implications in neuropathic pain absence during periodontal disease progression

Varying butyric acid amounts induce different stress- and cell death-related signals in nerve growth factor-treated PC12 cells: implications in neuropathic pain absence during periodontal disease progression

Neuropathic pain is absent from the early stages of periodontal disease possibly due to neurite retraction. Butyric acid (BA) is a periodontopathic metabolite that activates several stress-related signals and, likewise, induce neurite retraction. Neuronal cell death is associated to neurite retracti...

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Veröffentlicht in:Apoptosis (London) 2016-06, Vol.21 (6), p.699-707
Hauptverfasser: Seki, Keisuke, Cueno, Marni E., Kamio, Noriaki, Saito, Yuko, Kamimoto, Atsushi, Kurita-Ochiai, Tomoko, Ochiai, Kuniyasu
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Apoptosis
Biochemistry
Biomedical and Life Sciences
Biomedicine
Butyric Acid - metabolism
Cancer Research
Cell Biology
Cell death
Chromatin
Disease Progression
Hydrogen peroxide
Metabolites
Mortality
Nerve growth factor
Nerve Growth Factor - metabolism
Neuralgia - metabolism
Neuralgia - pathology
Neurites - metabolism
Neurons
Oncology
Oxidative Stress
Pain
PC12 Cells
Periodontal diseases
Periodontal Diseases - metabolism
Periodontal Diseases - pathology
Rats
Saturated fatty acids
Signal Transduction
Transcription Factor CHOP - metabolism
Virology
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Zusammenfassung:Neuropathic pain is absent from the early stages of periodontal disease possibly due to neurite retraction. Butyric acid (BA) is a periodontopathic metabolite that activates several stress-related signals and, likewise, induce neurite retraction. Neuronal cell death is associated to neurite retraction which would suggest that BA-induced neurite retraction is ascribable to neuronal cell death. However, the underlying mechanism of BA-related cell death signaling remains unknown. In this study, we exposed NGF-treated PC12 cells to varying BA concentrations [0 (control), 0.5, 1.0, 5.0 mM] and determined selected stress-related (H 2 O 2 , glutathione reductase, calcium (Ca 2+ ), plasma membrane Ca 2+ ATPase (PMCA), and GADD153/CHOPS) and cell death-associated (extrinsic: FasL, TNF-α, TWEAK, and TRAIL; intrinsic: cytochrome C (CytC), NF- k B, CASP8, CASP9, CASP10, and CASP3) signals. Similarly, we confirmed cell death execution by chromatin condensation. Our results showed that low (0.5 mM) and high (1.0 and 5.0 mM) BA levels differ in stress and cell death signaling. Moreover, at periodontal disease-level BA concentration (5 mM), we observed that only FasL amounts were affected and occurred concurrently with chromatin condensation insinuating that cells have fully committed to neurodegeneration. Thus, we believe that both stress and cell death signaling in NGF-treated PC12 cells are affected differently depending on BA concentration. In a periodontal disease scenario, we hypothesize that during the early stages, low BA amounts accumulate resulting to both stress- and cell death-related signals that favor neurite non-proliferation, whereas, during the later stages, high BA amounts accumulate resulting to both stress- and cell death-related signals that favor neurodegeneration. More importantly, we propose that neuropathic pain absence at any stage of periodontal disease progression is ascribable to BA accumulation regardless of amount.
ISSN:1360-8185
1573-675X
DOI:10.1007/s10495-016-1235-4