BMP2-induced Adam12+ Fibroblasts Dictate Wound-associated Skin Scarring and Fibrosis
Jun-Yi Chen, Jin-Ru Song, Ke-Ai Li, Xue-Yan Xu, Ding-Heng Zhu, Lian Zhang, Zi-Shuo Chen, Qing Cheng, Liu-Yi Yao, Yi-Qi Shen, Zhili Rong, Bin Yang, Cheng-Cheng Deng

TL;DR
This study identifies a key role for Adam12+ fibroblasts in skin scarring and shows how BMP2 signaling controls their formation and function.
Contribution
The study reveals BMP2 as a critical upstream signal for Adam12+ fibroblast generation and its role in skin scarring and fibrosis.
Findings
BMP2 signaling is essential for generating Adam12+ fibroblasts from resident fibroblasts.
Pharmacological inhibition of BMP2 reduces pathological scarring and fibrosis.
BMP2, periostin, and Adam12+ fibroblasts are elevated in pathological scars.
Abstract
Skin wounds typically undergo healing through scar formation, a fibrotic process mainly mediated by fibroblasts. Cumulative evidence from our group and others has established that Adam12+ fibroblasts were upregulated following skin injury and played a crucial role in scar formation. However, the molecular mechanisms governing the origin and pathogenesis of Adam12+ fibroblasts during skin scarring remain elusive. Here, we demonstrated that Adam12+ fibroblasts were necessary for wound-associated skin scarring and fibrosis. We identified BMP2 as the essential upstream signal for the generation of Adam12+ fibroblasts from resident fibroblasts and periostin as the key downstream effectors. Fibroblast-specific conditional knockout of BMP2 receptor significantly reduced Adam12+ fibroblast population, periostin expression, and ultimately skin scarring and fibrosis post-injury. BMP2, periostin…
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Taxonomy
TopicsTGF-β signaling in diseases · Connective Tissue Growth Factor Research · Wound Healing and Treatments
