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首页> 外文期刊>Biological psychiatry >Converging pharmacological and genetic evidence indicates a role for steroid sulfatase in attention.
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Converging pharmacological and genetic evidence indicates a role for steroid sulfatase in attention.

机译:越来越多的药理和遗传证据表明,甾体硫酸酯酶在人们的关注中发挥了作用。

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摘要

BACKGROUND: Attention-deficit/hyperactivity disorder (ADHD) is a complex neurodevelopmental disorder characterized by deficits in attention, increased motor impulsivity, and hyperactivity. Preliminary work in mice and humans has suggested the X-linked gene STS (which encodes the enzyme steroid sulfatase) as a mediator of attentional functioning and as a candidate gene for ADHD. METHODS: The effects of modulating the murine steroid sulfatase axis pharmacologically (through administration of the substrate dehydroepiandrosterone sulfate [DHEAS], 0-40 mg/kg, or acute inhibition of the enzyme by COUMATE, 10mg/kg) or genetically (through loss of the gene in 39,X(Y)*O mice) were assayed using the 5-choice serial reaction time task (5-CSRTT) a test of visuospatial attention and response control, and a locomotor activity paradigm. RESULTS: DHEAS administration improved 5-CSRTT performance under attentionally demanding conditions, whereas steroid sulfatase inhibition impaired accuracy under the same conditions. Loss of Sts expression constitutively throughout development in 39,X(Y)*O mice resulted in deficits in 5-CSRTT performance at short stimulus durations and reduced anticipatory responding. Neither the pharmacologic nor the genetic manipulations affected basic locomotor activity. CONCLUSIONS: These data provide converging evidence indicating a role for steroid sulfatase in discrete aspects of attentional functioning and are suggestive of a role in motor impulsivity. The findings provide novel insights into the neurobiology of attention and strengthen the notion of STS as a candidate gene for the attentional component of ADHD.
机译:背景:注意缺陷多动障碍(ADHD)是一种复杂的神经发育障碍,其特征是注意力不足,运动冲动增加和活动亢进。在小鼠和人类中的初步工作表明,X连锁基因STS(编码类固醇硫酸酯酶)可作为注意力功能的介体和ADHD的候选基因。方法:通过药理作用(通过施用底物硫酸脱氢表雄酮硫酸盐[DHEAS],0-40 mg / kg,或通过COUMATE急性抑制酶,剂量为10mg / kg)或通过基因调控(通过丢失)来调节鼠类固醇硫酸酯酶轴的作用。使用5选择连续反应时间任务(5-CSRTT),视觉空间注意力和反应控制测试以及运动活动范式对39,X(Y)* O小鼠的基因进行了分析。结果:DHEAS给药改善了5-CSRTT在苛刻要求的条件下的性能,而类固醇硫酸酯酶抑制作用在相同条件下会降低准确性。在39,X(Y)* O小鼠的整个发育过程中,Sts表达的组成性丧失导致5-CSRTT性能的下降,刺激时间较短,预期反应减少。药理学和遗传学操作均不影响基本运动能力。结论:这些数据提供了越来越多的证据,表明类固醇硫酸酯酶在注意功能的离散方面起作用,并暗示了在运动冲动中的作用。这些发现为注意力神经生物学提供了新颖的见解,并加强了STS作为ADHD注意力成分候选基因的观念。

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