来那度胺治疗自闭症的初步研究的安全性和观察。

Autism Research and Treatment Pub Date : 2012-01-01 Epub Date: 2012-09-11 DOI:10.1155/2012/291601
Michael Chez, Renee Low, Carol Parise, Tammy Donnel
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引用次数: 16

摘要

在美国,有1.88名儿童患有自闭症。自身免疫性疾病的家族史,当有一个以上的自闭症后代时,母亲血清中的自身抗体,以及自闭症患者脑脊液和脑组织中的神经胶质反应表明,免疫变量可能与这种情况有关。来那度胺有可能引起TNF-α的变化,但毒性比沙利度胺小。这项初步研究评估来那度胺在降低TNF-α和改善自闭症儿童TNF-α升高的行为和语言方面的作用。TNF-α升高的受试者每天给予2.5 mg来那度胺,持续12周。进行了药效学和安全性评价。在6周和12周后测量了语言和自闭症行为的变化。虽然大多数措施没有达到统计意义,但有改善的趋势。6周后,接受性语言的平均值从60.67±12.06上升至65.00±15.10 (P = 0.11),自闭症症状下降(40.75±5.96比38.67±7.90,P = 0.068)。12周后,CSF-TNF-α由80.5±41.03降至38.0±31.27,下降57%±25% (P = 0.068)。血清TNF-α下降57%(92.50±68.92)至40.25±44.53 (P = 0.048)。这项研究表明,来那度胺作为一种治疗自闭症儿童的药物是耐受性的,应该进一步研究作为细胞活素炎症的潜在药物。
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Safety and observations in a pilot study of lenalidomide for treatment in autism.

Autism affects 1 : 88 children in the United States. Familial history of autoimmune disease, autoantibodies in the serum of mothers when there is more than one autistic offspring, and neuroglial response in CSF and brain tissue in autistic patients suggest an immunological variable may be associated with this condition. Lenalidomide has the potential to invoke changes in TNF-α with less toxicity than thalidomide. This pilot study evaluated lenalidomide at reduction of TNF-α and improvement of behavior and language in children with autism with elevated TNF-α. Subjects with elevated TNF-α were given 2.5 mgs lenalidomide daily for 12-weeks. Pharmacodynamics and safety was evaluated. Changes in language and autistic behaviors after six and twelve weeks were measured. Although statistical significance was not achieved for most measures, there were trends toward improvement. After 6-weeks, mean receptive language increased: 60.67 ± 12.06 to 65.00 ± 15.10 (P = 0.11) and symptoms of autism decreased (40.75 ± 5.96 versus 38.67 ± 7.90, P = 0.068). After 12-weeks, CSF-TNF-α declined 57% ± 25% from 80.5 ± 41.03 to 38.0 ± 31.27 (P = 0.068). Serum TNF-α declined 57% (92.50 ± 68.92 to 40.25 ± 44.53 (P = 0.048). This study suggests that lenalidomide is tolerated as a treatment by children with autism and should be further studied as a potential agent for cytockine inflammation.

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