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Dopa-responsive dystonia: recent advances and remaining issues to be addressed (editorial)

机译:多巴反应性肌张力障碍:最新进展和尚待解决的问题(编辑)

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It is evident from this review that there is much that we know and much that we still do not know about DRD. In terms of diagnosis and clinical management, there is general agreement that patients with childhood-onset dystonic symptoms of unknown etiology should be treated initially with levodopa with the later addition, if necessary, of other medications (for example, BH4, 5-hydroxytryptophan). Although the results of molecular genetic and CSF studies are, at this time, unlikely to significantly alter clinical management of the patient, these analyses could be useful in providing information on prognosis (that is, DRD versus progressive neurodegenerative disorders or more severe metabolic disorders). It is also clear that notwithstanding the discovery of GCH1 and hTH mutations responsible for DRD, there remain many important unresolved issues regarding this disorder, including questions of female predominance, phenotypic heterogeneity, and presence of childhood-onset dystonia versus the expected parkinsonism resulting from a striatal DA deficit. We are confident that answers to these interesting questions on DRD will, in addition to providing clarification of the mechanisms of this disorder, provide exciting information relating to the pathogenesis of other types of dystonia as well as PD and to long-standing issues regarding a role of DA and serotonin in normal human brain development.
机译:从这次审查中可以明显看出,我们对DRD有很多了解,而我们仍然不了解。在诊断和临床管理方面,人们普遍认为,病因不明的童年性肌张力障碍症状的患者应首先用左旋多巴治疗,必要时再加其他药物(例如BH4、5-羟色氨酸)。 。尽管目前分子遗传学和CSF研究的结果不太可能显着改变患者的临床治疗,但这些分析可能有助于提供有关预后的信息(即DRD与进行性神经退行性疾病或更严重的代谢性疾病) 。同样清楚的是,尽管发现了导致DRD的GCH1和hTH突变,但仍存在许多与该疾病有关的未解决的重要问题,包括女性占优势,表型异质性,儿童期肌张力障碍与预期的帕金森病(由帕金森病引起)的问题。纹状体DA缺陷。我们相信,对于DRD上这些有趣问题的答案,除了可以澄清这种疾病的机制外,还将提供与其他类型的肌张力障碍以及PD的发病机理以及与作用有关的长期问题相关的令人兴奋的信息。和5-羟色胺在正常人脑发育中的作用

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