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Single photon emission computed tomography (SPECT) of anxiety disorders before and after treatment with citalopram

机译:西酞普兰治疗前后焦虑症的单光子发射计算机断层扫描(SPECT)

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Background Several studies have now examined the effects of selective serotonin reuptake inhibitor (SSRI) treatment on brain function in a variety of anxiety disorders including obsessive-compulsive disorder (OCD), posttraumatic stress disorder (PTSD), and social anxiety disorder (social phobia) (SAD). Regional changes in cerebral perfusion following SSRI treatment have been shown for all three disorders. The orbitofrontal cortex (OFC) (OCD), caudate (OCD), medial pre-frontal/cingulate (OCD, SAD, PTSD), temporal (OCD, SAD, PTSD) and, thalamic regions (OCD, SAD) are some of those implicated. Some data also suggests that higher perfusion pre-treatment in the anterior cingulate (PTSD), OFC, caudate (OCD) and antero-lateral temporal region (SAD) predicts subsequent treatment response. This paper further examines the notion of overlap in the neurocircuitry of treatment and indeed treatment response across anxiety disorders with SSRI treatment. Methods Single photon emission computed tomography (SPECT) using Tc-99 m HMPAO to assess brain perfusion was performed on subjects with OCD, PTSD, and SAD before and after 8 weeks (SAD) and 12 weeks (OCD and PTSD) treatment with the SSRI citalopram. Statistical parametric mapping (SPM) was used to compare scans (pre- vs post-medication, and responders vs non-responders) in the combined group of subjects. Results Citalopram treatment resulted in significant deactivation (p = 0.001) for the entire group in the superior (t = 4.78) and anterior (t = 4.04) cingulate, right thalamus (t = 4.66) and left hippocampus (t = 3.96). Deactivation (p = 0.001) within the left precentral (t = 4.26), right mid-frontal (t = 4.03), right inferior frontal (t = 3.99), left prefrontal (3.81) and right precuneus (t= 3.85) was more marked in treatment responders. No pattern of baseline activation distinguished responders from non-responders to subsequent pharmacotherapy. Conclusions Although each of the anxiety disorders may be mediated by different neurocircuits, there is some overlap in the functional neuro-anatomy of their response to SSRI treatment. The current data are consistent with previous work demonstrating the importance of limbic circuits in this spectrum of disorders. These play a crucial role in cognitive-affective processing, are innervated by serotonergic neurons, and changes in their activity during serotonergic pharmacotherapy seem crucial.
机译:背景技术现在有几项研究研究了选择性5-羟色胺再摄取抑制剂(SSRI)治疗对多种焦虑症(包括强迫症(OCD),创伤后应激障碍(PTSD)和社交焦虑症(社交恐惧症))的脑功能的影响。 (伤心)。在所有三种疾病中,SSRI治疗后脑灌注的区域变化均已显示。眶额皮质(OFC)(OCD),尾状(OCD),内侧前额叶/扣带状(OCD,SAD,PTSD),颞部(OCD,SAD,PTSD)和丘脑区(OCD,SAD)就是其中一些牵连。一些数据还表明,在前扣带回(PTSD),OFC,尾状(OCD)和前外侧颞区(SAD)中进行更高的灌注预处理可预测随后的治疗反应。本文进一步研究了神经回路治疗中重叠的概念,以及SSRI治疗跨焦虑症的实际治疗反应。方法在8周(SAD)和12周(OCD)前后,对患有OCD,PTSD和SAD的受试者进行Tc- 99 m HMPAO单光子发射计算机断层扫描(SPECT)以评估脑灌注和PTSD)用SSRI西酞普兰治疗。统计参数映射(SPM)用于比较组合对象组中的扫描结果(用药前和用药后,应答者与非应答者)。结果西酞普兰治疗导致整个组的上扣齿(t = 4.78)和前扣齿(t = 4.04),右丘脑(t = 4.66)和左海马(t = 3.96)均明显失活(p = 0.001)。左前中央(t = 4.26),右中额叶(t = 4.03),右下额叶(t = 3.99),左前额叶(t = 3.85)和右前突(t = 3.85)内的失活(p = 0.001)更多在治疗反应者中标记。没有基线激活模式可将反应者与未反应者区分开来进行后续药物治疗。结论尽管每种焦虑症可能是由不同的神经回路介导的,但在功能性神经解剖学上,它们对SSRI治疗的反应存在一些重叠。目前的数据与先前的研究结果相符,证明了在这种疾病中边缘循环的重要性。这些在认知情感加工中起关键作用,受血清素神经元神经支配,在血清素神经药物治疗期间其活性的改变似乎至关重要。

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