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脆性X综合征的神经精神症状:病理生理学与药物治疗

Neuropsychiatric symptoms of fragile X syndrome: pathophysiology and pharmacotherapy.

作者信息

Tsiouris John A, Brown W Ted

机构信息

George A. Jervis Clinic, New York State Institute for Basic Research in Developmental Disabilities, Staten Island, New York 10314, USA.

出版信息

CNS Drugs. 2004;18(11):687-703. doi: 10.2165/00023210-200418110-00001.

Abstract

Fragile X syndrome is the leading inherited form of mental retardation, and second only to Down's syndrome as a cause of mental retardation attributable to an identifiable genetic abnormality. Fragile X syndrome is caused by a defect in the fragile X mental retardation 1 gene (FMR1), located near the end of the long arm of the X chromosome. FMR1 normally synthesises the fragile X protein (FMRP), but mutations in FMR1 lead to a lack of FMRP synthesis, resulting in fragile X syndrome. While the specific function of FMRP is not yet fully understood, the protein is known to be important for normal brain development. The physical, cognitive and behavioural features of individuals with fragile X syndrome depend on gender (females have two X chromosomes, one active and one inactive) and the molecular status of the mutation (premutation, full mutation or mosaic). Features of the behavioural profile of individuals with fragile X syndrome include hypersensitivity to stimuli, overarousability, inattention, hyperactivity and (mostly in men) explosive and aggressive behaviour to others or self. Social anxiety, other anxiety disorders, depression, impulse control disorder and mood disorders are the most common psychiatric disorders diagnosed in individuals with fragile X syndrome, although no formal studies have been undertaken. There have been very few psychopharmacological studies of the treatment of behaviours associated with fragile X syndrome. These limited studies and surveys of psychotropic drugs used in individuals with fragile X syndrome suggest that stimulants are helpful for hyperactivity, that alpha(2)-adrenoceptor agonists and beta-adrenoceptor antagonists help to control overarousability, impulsivity and aggressiveness, and that SSRIs can control anxiety, impulsivity and irritability, alleviate depressive symptoms and decrease aggressive and self-injurious behaviour. Typical and atypical antipsychotics in combination with other psychotropics have been used for control of psychotic disorders and severe aggressive behaviours. Mood stabilisers have been found to be useful when mood dysregulation or mood disorders are present with or without aggressive behaviour. Folic acid and L-acetylcarnitine (levacecarnine) have not been found to improve deficits or behaviours. As there is no specific psychotropic drug for any of the deficits or behaviours associated with fragile X syndrome, clinicians are advised to diagnose any psychiatric syndromes or disorders present and treat them with the appropriate psychotropic drug. If no psychiatric disorder can be diagnosed and the patient's challenging behaviours cannot be controlled with environmental manipulation or behaviour modification techniques, the most benign psychotropic drug should be used. Antipsychotics should be reserved for psychotic disorders, for impulse control disorders (used in combination with other psychotropics), or when challenging behaviours constitute an emergency. In the future, new medications targeting molecules implicated in the modulation of anxiety, fear and fear responding will be useful for treating the social anxiety and overarousability exhibited by individuals with fragile X syndrome.

摘要

脆性X综合征是智力障碍最主要的遗传性形式,在可识别的基因异常所致智力障碍中仅次于唐氏综合征。脆性X综合征由位于X染色体长臂末端附近的脆性X智力低下1基因(FMR1)缺陷引起。FMR1通常合成脆性X蛋白(FMRP),但FMR1的突变导致FMRP合成缺乏,从而引发脆性X综合征。虽然FMRP的具体功能尚未完全明确,但已知该蛋白对正常大脑发育很重要。脆性X综合征患者的身体、认知和行为特征取决于性别(女性有两条X染色体,一条活跃,一条不活跃)以及突变的分子状态(前突变、全突变或嵌合体)。脆性X综合征患者行为特征包括对刺激高度敏感、过度易激惹、注意力不集中、多动以及(主要在男性中)对他人或自身爆发性和攻击性行为。社交焦虑、其他焦虑症、抑郁症、冲动控制障碍和情绪障碍是脆性X综合征患者中最常见的精神障碍诊断类型,尽管尚未进行正式研究。关于脆性X综合征相关行为治疗的精神药理学研究非常少。这些对脆性X综合征患者使用精神药物的有限研究和调查表明,兴奋剂对多动有帮助,α₂肾上腺素能受体激动剂和β肾上腺素能受体拮抗剂有助于控制过度易激惹、冲动和攻击性,选择性5-羟色胺再摄取抑制剂(SSRIs)可控制焦虑、冲动和易怒,减轻抑郁症状并减少攻击和自伤行为。典型和非典型抗精神病药物与其他精神药物联合使用可用于控制精神障碍和严重攻击行为。当存在或不存在攻击行为的情况下出现情绪失调或情绪障碍时,发现情绪稳定剂有用。尚未发现叶酸和L-乙酰肉碱(左卡尼汀)能改善缺陷或行为。由于没有针对脆性X综合征相关任何缺陷或行为的特异性精神药物,建议临床医生诊断存在的任何精神综合征或障碍,并用适当的精神药物进行治疗。如果无法诊断出精神障碍,且患者具有挑战性的行为无法通过环境操纵或行为矫正技术控制,则应使用最温和的精神药物。抗精神病药物应保留用于精神障碍、冲动控制障碍(与其他精神药物联合使用),或当具有挑战性的行为构成紧急情况时。未来,针对参与调节焦虑、恐惧和恐惧反应的分子的新型药物将有助于治疗脆性X综合征患者表现出的社交焦虑和过度易激惹。

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