同种异体造血干细胞移植后先天性免疫缺陷患者非骨质疏松性骨病。
Non-osteopenic Bone Pathology After Allo-hematopoietic Stem Cell Transplantation in Patients with Inborn Errors of Immunity.
机构信息
Department of Immunology, Great Ormond Street Hospital for Children NHS Foundation Trust, Great Ormond Street, London, WC1N 3JH, UK.
UCL Great Ormond Street Institute of Child Health, London, UK.
出版信息
J Clin Immunol. 2023 Jul;43(5):1019-1031. doi: 10.1007/s10875-023-01465-z. Epub 2023 Mar 17.
PURPOSE
There is a lack of data on post-HSCT non-osteopenic bone pathology specifically for children with inborn errors of immunity (IEI). We collected data on non-osteopenic bone pathology in children with IEI post-HSCT over two decades in a large tertiary pediatric immunology center.
METHODS
Descriptive study with data analysis of bone pathology in allo-HSCT for IEI was performed between 1/1/2000 to 31/12/2018 including patients alive at follow-up to July 2022. Records were analyzed for bone pathology and risk factors. Exclusion criteria included isolated reduced bone density, fractures, and skeletal anomalies due to underlying IEI and short stature without other bone pathology. Bone pathologies were divided into 5 categories: bone tumors; skeletal dysplasia; avascular necrosis; evolving bone deformities; slipped upper femoral epiphysis.
RESULTS
A total of 429 children received HSCT between 2000 and 2018; 340 are alive at last assessment. Non-osteopenic bone pathology was observed post-HSCT in 9.4% of patients (32/340, mean 7.8 years post-HSCT). Eleven patients (34%) had > 1 category of bone pathology. Seventeen patients (17/32; 53%) presented with bilateral bone pathology. The majority of patients received treosulfan-based conditioning (26/32; 81.2%). Totally, 65.6% (21/32) of patients had a history of prolonged steroid use (> 6 months). Pain was the presenting symptom in 66% of patients, and surgical intervention was required in 43.7%. The highest incidence of bone pathologies was seen in Wiskott-Aldrich syndrome (WAS) (n = 8/34; 23.5%) followed by hemophagocytic lymphohistiocytosis patients (n = 3/16; 18.8%).
CONCLUSION
Non-osteopenic bone pathology in long-term survivors of allo-HSCT for IEI is not rare. Most patients did not present with complaints until at least 5 years post-HSCT highlighting the need for ongoing bone health assessment for patients with IEI. Children presenting with stunted growth and bone pathology post-HSCT should undergo skeletal survey to rule out development of post-HSCT skeletal dysplasia. Increased rates and complexity of bone pathology were seen amongst patients with Wiskott-Aldrich syndrome.
目的
目前缺乏关于骨髓移植后非骨质疏松性骨病理学的具体数据,尤其是针对先天性免疫缺陷(IEI)儿童。我们在一家大型儿科免疫中心收集了 20 多年来接受骨髓移植的 IEI 儿童的非骨质疏松性骨病理学数据。
方法
对 2000 年 1 月 1 日至 2018 年 12 月 31 日期间接受异基因骨髓移植的 IEI 患者进行骨病理学数据的描述性研究,包括随访至 2022 年 7 月仍存活的患者。分析记录骨病理学和危险因素。排除标准包括孤立性骨密度降低、骨折和骨骼异常、由于基础 IEI 导致的身材矮小和无其他骨病理学。骨病理学分为 5 类:骨肿瘤;骨骼发育不良;骨坏死;进行性骨畸形;股骨上端滑脱。
结果
2000 年至 2018 年间共有 429 名儿童接受骨髓移植;340 名在最后一次评估时仍存活。340 名患者中有 9.4%(32/340)在骨髓移植后出现非骨质疏松性骨病理学,平均在骨髓移植后 7.8 年。11 名患者(34%)存在超过 1 种骨病理学类别。17 名患者(17/32;53%)表现为双侧骨病理学。大多数患者接受了以三氟胸苷为基础的预处理(26/32;81.2%)。总共 65.6%(21/32)的患者有长期使用激素(>6 个月)的病史。66%的患者以疼痛为首发症状,43.7%需要手术干预。骨病理学发病率最高的是 Wiskott-Aldrich 综合征(WAS)(n=8/34;23.5%),其次是噬血细胞性淋巴组织细胞增生症患者(n=3/16;18.8%)。
结论
IEI 患者异基因骨髓移植后的非骨质疏松性骨病理学并不少见。大多数患者直到骨髓移植后至少 5 年才出现症状,这突出表明需要对 IEI 患者进行持续的骨骼健康评估。骨髓移植后出现生长迟缓且骨骼病理学异常的儿童应进行骨骼检查以排除骨髓移植后骨骼发育不良的发生。WAS 患者的骨病理学发生率和复杂性增加。
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