FAM20A缺陷驱动牙龈成纤维细胞转录组失调和功能损伤。

IF 5.6 1区生物学 Q2 CELL BIOLOGY

Cell Proliferation Pub Date : 2025-07-22 DOI:10.1111/cpr.70096

Kanokwan Sriwattanapong, Sermporn Thaweesapphithak, Chompak Khamwachirapitak, Pannagorn Sae-Ear, Sasiprapa Prommanee, Noppadol Sa-Ard-Iam, Suphalak Phothichailert, Han Sung Jung, Vorasuk Shotelersuk, Thantrira Porntaveetus

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引用次数: 0

摘要

Amelogenesis imperfecta type 1G (AI1G)，也被称为珐琅-肾脏-牙龈综合征（ERGS），是一种常染色体隐性遗传病，由FAM20A变异引起，FAM20A编码高尔基体蛋白，对蛋白质加工和分泌至关重要。AI1G表现为牙釉质缺损、肾钙质沉着和牙龈增生。基于我们之前的研究结果，证明FAM20A不足对乳牙髓细胞的影响，本研究探讨了AI1G牙龈纤维瘤病的分子机制。一名AI1G患者的牙龈成纤维细胞的RNA测序显示广泛的差异基因表达（DEG）。基因本体（Gene Ontology， GO）分析表明，在细胞粘附、分化、增殖（包括正调控和细胞分裂）、细胞周期调控、细胞凋亡和信号转导等生物过程中，DEGs富集。通路分析（Reactome和KEGG）进一步强调了信号通路的失调，包括Wnt、TGF-β、细胞周期、DNA复制、Rho GTPase信号传导和细胞外基质组织。功能分析证实了这些发现，发现fam20a不足的成纤维细胞初始附着和扩散延迟，成骨分化受损（DLX5、OCN、RUNX2和OPN矿化减少和下调），细胞周期进程和增殖增强（集落大小和增殖率增加，从G0/G1期向G2/M期转变），细胞凋亡受到抑制。这些结果表明，FAM20A在牙龈成纤维细胞的基本过程中起着关键的调节作用，其不足通过破坏细胞的粘附、分化、增殖和凋亡，导致AI1G中观察到的牙龈纤维瘤病表型。这项研究对AI1G的发病机制提出了新的见解，并强调了这种复杂疾病的潜在治疗靶点。

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FAM20A Deficiency Drives Transcriptomic Dysregulation and Functional Impairment in Gingival Fibroblasts.

Amelogenesis imperfecta type 1G (AI1G), also known as Enamel-Renal-Gingival Syndrome (ERGS), is an autosomal recessive disorder caused by variants in FAM20A, encoding a Golgi apparatus protein crucial for protein processing and secretion. AI1G presents with enamel defects, nephrocalcinosis and gingival overgrowth. Building upon our previous findings demonstrating the impact of FAM20A insufficiency on deciduous dental pulp cells, this study investigated the molecular mechanisms underlying gingival fibromatosis in AI1G. RNA sequencing of gingival fibroblasts from an AI1G patient revealed widespread differential gene expression (DEG). Gene Ontology (GO) analysis demonstrated enrichment of DEGs in biological processes related to cell adhesion, differentiation, proliferation (including positive regulation and cell division), cell cycle regulation, apoptosis and signal transduction. Pathway analysis (Reactome and KEGG) further highlighted the dysregulation of signalling pathways, including Wnt, TGF-β, cell cycle, DNA replication, Rho GTPase signalling and extracellular matrix organisation. Functional assays confirmed these findings, revealing delayed initial attachment and spreading, impaired osteogenic differentiation (evidenced by reduced mineralization and downregulation of DLX5, OCN, RUNX2 and OPN), enhanced cell cycle progression and proliferation (increased colony size and proliferation rates, along with a shift from G0/G1 to G2/M phase) and suppressed apoptosis in FAM20A-insufficient fibroblasts. These results suggest that FAM20A plays a critical role in regulating fundamental processes in gingival fibroblasts, and its insufficiency contributes to the gingival fibromatosis phenotype observed in AI1G through the disruption of cell adhesion, differentiation, proliferation and apoptosis. This study proposes novel insights into the pathogenesis of AI1G and highlights potential therapeutic targets for this complex disorder.

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来源期刊

Cell Proliferation 生物-细胞生物学

CiteScore

14.80

自引率

2.40%

发文量

198

审稿时长

1 months

期刊介绍： Cell Proliferation Focus: Devoted to studies into all aspects of cell proliferation and differentiation. Covers normal and abnormal states. Explores control systems and mechanisms at various levels: inter- and intracellular, molecular, and genetic. Investigates modification by and interactions with chemical and physical agents. Includes mathematical modeling and the development of new techniques. Publication Content: Original research papers Invited review articles Book reviews Letters commenting on previously published papers and/or topics of general interest By organizing the information in this manner, readers can quickly grasp the scope, focus, and publication content of Cell Proliferation.