成骨不全症伴多发性骨囊肿源于编码骨形成蛋白 2 转录因子(特异性蛋白 7)的 SP7 杂合突变
Juvenile Paget's Disease From Heterozygous Mutation of SP7 Encoding Osterix (Specificity Protein 7, Transcription Factor SP7).
机构信息
Center For Metabolic Bone Disease and Molecular Research, Shriners Hospitals for Children - St. Louis, St. Louis, MO 63110, USA; Division of Bone and Mineral Diseases, Department of Internal Medicine, Washington University School of Medicine, St. Louis, MO 63110, USA.
Department of Pediatrics, University of Montreal, Montreal, Quebec H3T 1C5, Canada.
出版信息
Bone. 2020 Aug;137:115364. doi: 10.1016/j.bone.2020.115364. Epub 2020 Apr 13.
Juvenile Paget's disease (JPD) became in 1974 the commonly used name for ultra-rare heritable occurrences of rapid bone remodeling throughout of the skeleton that present in infancy or early childhood as fractures and deformity hallmarked biochemically by marked elevation of serum alkaline phosphatase (ALP) activity (hyperphosphatasemia). Untreated, JPD can kill during childhood or young adult life. In 2002, we reported that homozygous deletion of the gene called tumor necrosis factor receptor superfamily, member 11B (TNFRSF11B) encoding osteoprotegerin (OPG) explained JPD in Navajos. Soon after, other bi-allelic loss-of-function TNFRSF11B defects were identified in JPD worldwide. OPG inhibits osteoclastogenesis and osteoclast activity by decoying receptor activator of nuclear factor κ-B (RANK) ligand (RANKL) away from its receptor RANK. Then, in 2014, we reported JPD in a Bolivian girl caused by a heterozygous activating duplication within TNFRSF11A encoding RANK. Herein, we identify mutation of a third gene underlying JPD. An infant girl began atraumatic fracturing of her lower extremity long-bones. Skull deformity and mild hearing loss followed. Our single investigation of the patient, when she was 15 years-of-age, showed generalized osteosclerosis and hyperostosis. DXA revealed a Z-score of +5.1 at her lumbar spine and T-score of +3.3 at her non-dominant wrist. Biochemical studies were consistent with positive mineral balance and several markers of bone turnover were elevated and included striking hyperphosphatasemia. Iliac crest histopathology was consistent with rapid skeletal remodeling. Measles virus transcripts, common in classic Paget's disease of bone, were not detected in circulating mononuclear cells. Then, reportedly, she responded to several months of alendronate therapy with less skeletal pain and correction of hyperphosphatasemia but had been lost to our follow-up. After we detected no defect in TNFRSF11A or B, trio exome sequencing revealed a de novo heterozygous missense mutation (c.926C>G; p.S309W) within SP7 encoding the osteoblast transcription factor osterix (specificity protein 7, transcription factor SP7). Thus, mutation of SP7 represents a third genetic cause of JPD.
少年型佩吉特病(JPD)于 1974 年成为通用名称,用于描述极为罕见的遗传性全身骨骼快速重塑,在婴儿期或幼儿期表现为骨折和畸形,其生化特征为血清碱性磷酸酶(ALP)活性显著升高(高磷酸血症)。未经治疗,JPD 可导致儿童或青年期死亡。2002 年,我们报道了编码骨保护素(OPG)的肿瘤坏死因子受体超家族成员 11B(TNFRSF11B)基因的纯合缺失解释了纳瓦霍人的 JPD。此后,在全球范围内的 JPD 中发现了其他双等位基因 TNFRSF11B 功能丧失缺陷。OPG 通过诱饵核因子 κ-B(NF-κB)受体激活剂配体(RANKL)从其受体 RANK 上脱离来抑制破骨细胞生成和破骨细胞活性。然后,在 2014 年,我们报道了玻利维亚一名女孩的 JPD 是由编码 RANK 的 TNFRSF11A 中的杂合激活重复引起的。在此,我们确定了第三个导致 JPD 的基因突变。一名女婴下肢长骨开始出现无创伤性骨折。随后出现颅骨畸形和轻度听力损失。我们对患者的单一调查显示,当她 15 岁时,全身骨骼出现硬化性和骨质增生。DXA 显示腰椎骨 Z 分数为+5.1,非优势腕骨 T 分数为+3.3。生化研究与正性矿物质平衡一致,几种骨转换标志物升高,包括明显的高磷酸血症。髂嵴组织病理学与快速骨骼重塑一致。在循环单核细胞中未检测到常见于经典骨 Paget 病的麻疹病毒转录本。然后,据报道,她对几个月的阿伦膦酸盐治疗有反应,骨骼疼痛减轻,高磷酸血症得到纠正,但已失访。在我们未发现 TNFRSF11A 或 B 缺陷后,三代外显子测序显示 SP7 编码成骨细胞转录因子骨钙素(特异性蛋白 7,转录因子 SP7)中的一个新的杂合错义突变(c.926C>G;p.S309W)。因此,SP7 的突变代表了 JPD 的第三个遗传原因。
Zotero 插件