Histone acetylation facilitates multidirectional pulp repair through Neuregulin-1 mobilization
Zhiwu Wu, Hui Yang, Shaoying Duan, Qianqian Su, Ran Cheng, Tao Hu

TL;DR
Enhancing histone acetylation helps repair dental pulp by boosting NRG1, which reduces inflammation and promotes tissue regeneration.
Contribution
The study shows that histone acetylation modulates NRG1 to improve pulp repair with anti-inflammatory and regenerative effects.
Findings
NRG1 overexpression reduces inflammation and promotes dentin and nerve regeneration.
HDAC inhibitors like SAHA enhance histone acetylation and NRG1 activation for pulp repair.
H3K9 and H3K27 acetylation levels correlate with NRG1 expression during pulp repair.
Abstract
Appropriate dental pulp repair is based on effective control of inflammation and involves the regeneration of dental pulp nerves, blood vessels (soft tissue), and dentin (hard tissue). Limited evidence has shown how to modulate the uncertainty due to individual variability in dental pulp repair. NRG1, a cytokine modulating nerve injury and repair, was intricately associated with the outcome of pulp repair. Yet, its mobilization in spontaneous pulp repair had individual variability. The study further explored the role of NRG1 during pulp repair as well as an epigenetic way to modulate NRG1 through histone acetylation to enhance pulp repair. Overexpression of NRG1 exhibited the effects of anti-inflammation and integrated regeneration of soft and hard tissue, by inhibiting pro-inflammatory factors IL-1β, IL-8, and promoting the expressions of DSPP, DMP1 (dentin regeneration), and nestin…
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Taxonomy
TopicsWound Healing and Treatments · NF-κB Signaling Pathways · Signaling Pathways in Disease
