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造血细胞移植后黏多糖贮积症I型患者腕管综合征发生发展的影响因素分析

Analysis of factors affecting development of carpal tunnel syndrome in patients with Hurler syndrome after hematopoietic cell transplantation.

作者信息

Khanna G, Van Heest A E, Agel J, Bjoraker K, Grewal S, Abel S, Krivit W, Peters C, Orchard P J

机构信息

Department of Orthopedic Surgery, University of Minnesota School of Medicine, Minneapolis, MN 55455, USA.

出版信息

Bone Marrow Transplant. 2007 Mar;39(6):331-4. doi: 10.1038/sj.bmt.1705586. Epub 2007 Feb 5.

Abstract

Children with Hurler syndrome (mucopolysaccharidosis type IH (MPSIH)) have skeletal, joint and soft tissue abnormalities that may persist or progress after hematopoietic stem cell transplantation (HSCT). We report our single center experience with development of carpal tunnel syndrome (CTS) in 43 children with MPSIH after HSCT. Twenty-three children (59%) developed CTS following HSCT; 19 of the 39 children with enzyme activity in the normal or heterozygous range developed CTS (49%), whereas all four children with low heterozygous or absent enzyme activity developed CTS after HSCT. Fourteen of 19 related donor marrow recipients, eight of 19 of those receiving an unrelated donor graft and one of five unrelated cord blood recipients developed CTS. The mean age at surgical release was 4.8 years. With each year increase in age at HSCT, there was a 55% increased risk. Age and enzyme activity after HSCT were significant factors in the development of CTS. Transplantation by 2 years of age reduced the risk of developing CTS by 46%; higher enzyme activity led to a 78% reduction in the risk of developing CTS. However, children transplanted for MPSIH remain at risk for the development of CTS, and should be monitored on an ongoing basis by nerve conduction velocity testing.

摘要

患有黏多糖贮积症I型(MPSIH,又称Hurler综合征)的儿童存在骨骼、关节和软组织异常,这些异常在造血干细胞移植(HSCT)后可能持续存在或进展。我们报告了我们单中心关于43例接受HSCT后的MPSIH儿童发生腕管综合征(CTS)的经验。23例儿童(59%)在HSCT后发生了CTS;39例酶活性处于正常或杂合范围的儿童中有19例发生了CTS(49%),而4例酶活性为低杂合或无酶活性的儿童在HSCT后均发生了CTS。19例相关供体骨髓受者中有14例、19例接受非相关供体移植者中有8例以及5例接受非相关脐血移植者中有1例发生了CTS。手术松解的平均年龄为4.8岁。HSCT时年龄每增加一岁,发病风险增加55%。HSCT后的年龄和酶活性是CTS发生的重要因素。2岁前进行移植可使CTS发病风险降低46%;较高的酶活性可使CTS发病风险降低78%。然而,接受MPSIH移植的儿童仍有发生CTS的风险,应通过神经传导速度测试持续进行监测。

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