Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, Texas, USA.
Texas Children's Hospital, Houston, Texas, USA.
J Clin Invest. 2022 Apr 1;132(7). doi: 10.1172/JCI152571.
BACKGROUNDCurrently, there is no disease-specific therapy for osteogenesis imperfecta (OI). Preclinical studies demonstrate that excessive TGF-β signaling is a pathogenic mechanism in OI. Here, we evaluated TGF-β signaling in children with OI and conducted a phase I clinical trial of TGF-β inhibition in adults with OI.METHODSHistology and RNA-Seq were performed on bones obtained from children. Gene Ontology (GO) enrichment assay, gene set enrichment analysis (GSEA), and Ingenuity Pathway Analysis (IPA) were used to identify dysregulated pathways. Reverse-phase protein array, Western blot, and IHC were performed to evaluate protein expression. A phase I study of fresolimumab, a TGF-β neutralizing antibody, was conducted in 8 adults with OI. Safety and effects on bone remodeling markers and lumbar spine areal bone mineral density (LS aBMD) were assessed.RESULTSOI bone demonstrated woven structure, increased osteocytes, high turnover, and reduced maturation. SMAD phosphorylation was the most significantly upregulated GO molecular event. GSEA identified the TGF-β pathway as the top activated signaling pathway, and IPA showed that TGF-β1 was the most significant activated upstream regulator mediating the global changes identified in OI bone. Treatment with fresolimumab was well-tolerated and associated with increases in LS aBMD in participants with OI type IV, whereas participants with OI type III and VIII had unchanged or decreased LS aBMD.CONCLUSIONIncreased TGF-β signaling is a driver pathogenic mechanism in OI. Anti-TGF-β therapy could be a potential disease-specific therapy, with dose-dependent effects on bone mass and turnover.TRIAL REGISTRATIONClinicalTrials.gov NCT03064074.FUNDINGBrittle Bone Disorders Consortium (U54AR068069), Clinical Translational Core of Baylor College of Medicine Intellectual and Developmental Disabilities Research Center (P50HD103555) from National Institute of Child Health and Human Development, USDA/ARS (cooperative agreement 58-6250-6-001), and Sanofi Genzyme.
目前,成骨不全症(OI)尚无特异性治疗方法。临床前研究表明,TGF-β信号过度激活是 OI 的一种致病机制。在此,我们评估了 OI 患儿的 TGF-β信号,并对 OI 成人进行了 TGF-β抑制的 I 期临床试验。
对取自儿童的骨骼进行组织学和 RNA-Seq 分析。采用基因本体论(GO)富集分析、基因集富集分析(GSEA)和 IPA 分析鉴定失调通路。进行反相蛋白阵列、Western blot 和 IHC 以评估蛋白表达。对 8 名 OI 成人进行 fresolimumab(一种 TGF-β中和抗体)的 I 期研究。评估安全性以及对骨重塑标志物和腰椎骨面积骨密度(LS aBMD)的影响。
OI 骨表现为编织结构、骨细胞增多、高转换率和成熟度降低。SMAD 磷酸化是最显著上调的 GO 分子事件。GSEA 鉴定出 TGF-β 通路为最活跃的信号通路,IPA 表明 TGF-β1 是介导 OI 骨中全局变化的最显著激活的上游调节因子。fresolimumab 治疗耐受性良好,与 OI 型 IV 患者的 LS aBMD 增加相关,而 OI 型 III 和 VIII 患者的 LS aBMD 无变化或降低。
TGF-β信号的增加是 OI 的一种驱动性致病机制。抗 TGF-β 治疗可能是一种潜在的特异性疾病治疗方法,对骨量和转换具有剂量依赖性作用。
ClinicalTrials.gov NCT03064074。
脆性骨疾病联盟(U54AR068069)、贝勒医学院智力和发育障碍研究中心临床转化核心(P50HD103555),来自国家儿童健康与人类发育研究所,美国农业部/农业研究服务局(合作协议 58-6250-6-001)和赛诺菲健赞。
Zotero 插件
