Multi-omics analyses reveal aberrant differentiation trajectory with WNT1 loss-of-function in type XV osteogenesis imperfecta.

IF 5.1 1区 医学 Q1 ENDOCRINOLOGY & METABOLISM Journal of Bone and Mineral Research Pub Date : 2024-09-02 DOI:10.1093/jbmr/zjae123
Zhijia Tan, Peikai Chen, Jianan Zhang, Hiu Tung Shek, Zeluan Li, Xinlin Zhou, Yapeng Zhou, Shijie Yin, Lina Dong, Lin Feng, Janus Siu Him Wong, Bo Gao, Michael Kai Tsun To
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Abstract

Osteogenesis imperfecta (OI) is a group of severe genetic bone disorders characterized by congenital low bone mass, deformity, and frequent fractures. Type XV OI is a moderate to severe form of skeletal dysplasia caused by WNT1 variants. In this cohort study from southern China, we summarized the clinical phenotypes of patients with WNT1 variants and found that the proportion of type XV patients was around 10.3% (25 out of 243) with a diverse spectrum of phenotypes. Functional assays indicated that variants of WNT1 significantly impaired its secretion and effective activity, leading to moderate to severe clinical manifestations, porous bone structure, and enhanced osteoclastic activities. Analysis of proteomic data from human skeleton indicated that the expression of SOST (sclerostin) was dramatically reduced in type XV patients compared to patients with COL1A1 quantitative variants. Single-cell transcriptome data generated from human tibia samples of patients diagnosed with type XV OI and leg-length discrepancy, respectively, revealed aberrant differentiation trajectories of skeletal progenitors and impaired maturation of osteocytes with loss of WNT1, resulting in excessive CXCL12+ progenitors, fewer mature osteocytes, and the existence of abnormal cell populations with adipogenic characteristics. The integration of multi-omics data from human skeleton delineates how WNT1 regulates the differentiation and maturation of skeletal progenitors, which will provide a new direction for the treatment strategy of type XV OI and relative low bone mass diseases such as early onset osteoporosis.

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多组学分析揭示了在XV型成骨不全症中WNT1功能缺失导致的异常分化轨迹。
成骨不全症(OI)是一组严重的遗传性骨骼疾病,以先天性低骨量、畸形和频繁骨折为特征。XV 型 OI 是一种由 WNT1 变异引起的中重度骨骼发育不良。在这项来自中国南方的队列研究中,我们总结了 WNT1 变体患者的临床表型,发现 XV 型患者的比例约为 10.3%(243 人中有 25 人),其表型多种多样。功能测试表明,WNT1变体会显著影响其分泌和有效活性,导致中重度临床表现、多孔骨结构和破骨活性增强。对人体骨骼蛋白质组数据的分析表明,与 COL1A1 定量变异型患者相比,XV 型患者的 SOST 表达量大幅减少。分别从确诊为第十五型OI和腿长不一致患者的人体胫骨样本中生成的单细胞转录组数据显示,由于WNT1缺失,骨骼祖细胞的分化轨迹出现异常,成骨细胞的成熟度受损,导致CXCL12+祖细胞过多,成熟成骨细胞较少,并存在具有脂肪生成特征的异常细胞群。整合人体骨骼的多组学数据,阐明了WNT1如何调控骨骼祖细胞的分化和成熟,这将为XV型成骨不全症和相对低骨量疾病(如早发骨质疏松症)的治疗策略提供新的方向。
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来源期刊
Journal of Bone and Mineral Research
Journal of Bone and Mineral Research 医学-内分泌学与代谢
CiteScore
11.30
自引率
6.50%
发文量
257
审稿时长
2 months
期刊介绍: The Journal of Bone and Mineral Research (JBMR) publishes highly impactful original manuscripts, reviews, and special articles on basic, translational and clinical investigations relevant to the musculoskeletal system and mineral metabolism. Specifically, the journal is interested in original research on the biology and physiology of skeletal tissues, interdisciplinary research spanning the musculoskeletal and other systems, including but not limited to immunology, hematology, energy metabolism, cancer biology, and neurology, and systems biology topics using large scale “-omics” approaches. The journal welcomes clinical research on the pathophysiology, treatment and prevention of osteoporosis and fractures, as well as sarcopenia, disorders of bone and mineral metabolism, and rare or genetically determined bone diseases.
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