Single-cell transcriptomics identifies PDGFRA+ progenitors orchestrating angiogenesis and periodontal tissue regeneration

IF 12.2 1区医学 Q1 DENTISTRY, ORAL SURGERY & MEDICINE

International Journal of Oral Science Pub Date : 2025-07-24 DOI:10.1038/s41368-025-00384-6

Jianing Liu, Junxi He, Ziqi Zhang, Lu Liu, Yuan Cao, Xiaohui Zhang, Xinyue Cai, Xinyan Luo, Xiao Lei, Nan Zhang, Hao Wang, Ji Chen, Peisheng Liu, Jiongyi Tian, Jiexi Liu, Yuru Gao, Haokun Xu, Chao Ma, Shengfeng Bai, Yubohan Zhang, Yan Jin, Chenxi Zheng, Bingdong Sui, Fang Jin

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引用次数: 0

Abstract

Periodontal bone defects, primarily caused by periodontitis, are highly prevalent in clinical settings and manifest as bone fenestration, dehiscence, or attachment loss, presenting a significant challenge to oral health. In regenerative medicine, harnessing developmental principles for tissue repair offers promising therapeutic potential. Of particular interest is the condensation of progenitor cells, an essential event in organogenesis that has inspired clinically effective cell aggregation approaches in dental regeneration. However, the precise cellular coordination mechanisms during condensation and regeneration remain elusive. Here, taking the tooth as a model organ, we employed single-cell RNA sequencing to dissect the cellular composition and heterogeneity of human dental follicle and dental papilla, revealing a distinct Platelet-derived growth factor receptor alpha (PDGFRA) mesenchymal stem/stromal cell (MSC) population with remarkable odontogenic potential. Interestingly, a reciprocal paracrine interaction between PDGFRA⁺ dental follicle stem cells (DFSCs) and CD31⁺ Endomucin⁺ endothelial cells (ECs) was mediated by Vascular endothelial growth factor A (VEGFA) and Platelet-derived growth factor subunit BB (PDGFBB). This crosstalk not only maintains the functionality of PDGFRA⁺ DFSCs but also drives specialized angiogenesis. In vivo periodontal bone regeneration experiments further reveal that communication between PDGFRA⁺ DFSC aggregates and recipient ECs is essential for effective angiogenic-osteogenic coupling and rapid tissue repair. Collectively, our results unravel the importance of MSC-EC crosstalk mediated by the VEGFA and PDGFBB-PDGFRA reciprocal signaling in orchestrating angiogenesis and osteogenesis. These findings not only establish a framework for deciphering and promoting periodontal bone regeneration in potential clinical applications but also offer insights for future therapeutic strategies in dental or broader regenerative medicine.

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单细胞转录组学鉴定PDGFRA+祖细胞协调血管生成和牙周组织再生

牙周骨缺损主要由牙周炎引起，在临床上非常普遍，表现为骨开窗、开裂或附着丧失，对口腔健康构成重大挑战。在再生医学中，利用组织修复的发育原理提供了有希望的治疗潜力。特别令人感兴趣的是祖细胞的凝聚，这是器官发生中的一个重要事件，激发了临床上有效的牙齿再生细胞聚集方法。然而，在凝结和再生过程中，精确的细胞协调机制仍然是难以捉摸的。本研究以牙齿为模型器官，采用单细胞RNA测序分析了人类牙毛囊和牙乳头的细胞组成和异质性，揭示了一个独特的血小板衍生生长因子受体α (PDGFRA)间充质干细胞/间质细胞（MSC）群体，具有显著的成牙潜能。有趣的是，PDGFRA+牙滤泡干细胞（DFSCs）和CD31+内皮细胞（ECs）之间的互惠旁分泌相互作用是由血管内皮生长因子a （VEGFA）和血小板衍生生长因子亚单位BB （PDGFBB）介导的。这种串扰不仅维持了PDGFRA+ DFSCs的功能，而且还驱动了特化血管生成。体内牙周骨再生实验进一步表明，PDGFRA+ DFSC聚集体与受体内皮细胞之间的通信对于有效的血管生成-成骨耦合和快速组织修复至关重要。总之，我们的研究结果揭示了由VEGFA和PDGFBB-PDGFRA相互信号介导的MSC-EC串扰在协调血管生成和成骨过程中的重要性。这些发现不仅为研究和促进牙周骨再生的潜在临床应用建立了框架，而且为牙科或更广泛的再生医学的未来治疗策略提供了见解。

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来源期刊

International Journal of Oral Science DENTISTRY, ORAL SURGERY & MEDICINE-

CiteScore

31.80

自引率

1.30%

发文量

审稿时长

>12 weeks

期刊介绍： The International Journal of Oral Science covers various aspects of oral science and interdisciplinary fields, encompassing basic, applied, and clinical research. Topics include, but are not limited to: Oral microbiology Oral and maxillofacial oncology Cariology Oral inflammation and infection Dental stem cells and regenerative medicine Craniofacial surgery Dental material Oral biomechanics Oral, dental, and maxillofacial genetic and developmental diseases Craniofacial bone research Craniofacial-related biomaterials Temporomandibular joint disorder and osteoarthritis The journal publishes peer-reviewed Articles presenting new research results and Review Articles offering concise summaries of specific areas in oral science.