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Hypomania and saccadic changes in Parkinson’s disease: influence of D2 and D3 dopaminergic signalling

机译:帕金森病的轩轩和扫视变化:D2和D3多巴胺能信号的影响

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In order to understand the influence of two dopaminergic signalling pathways, TaqIA rs1800497 (influencing striatal D2 receptor density) and Ser9Gly rs6280 (influencing the striatal D3 dopamine-binding affinity), on saccade generation and psychiatric comorbidities in Parkinson’s disease, this study aimed to investigate the association of saccadic performance in hypomanic or impulsive behaviour in parkinsonian patients; besides we questioned whether variants of D2 (A1+/A1?) and D3 (B1+/B1?) receptor polymorphism influence saccadic parameters differently, and if clinical parameters or brain connectivity changes modulate this association in the nigro-caudatal and nigro-collicular tract. Initially, patients and controls were compared regarding saccadic performance and differed in the parameter duration in memory-guided saccades (MGS) and visually guided saccades (VGS) trials (p??0.0001) and in the MGS trial (p??0.03). We were able to find associations between hypomanic behaviour (HPS) and saccade parameters (duration, latency, gain and amplitude) for both conditions [MGS (p?=?0.036); VGS (p?=?0.033)], but not for impulsive behaviour. For the A1 variant duration was significantly associated with HPS [VGS (p?=?0.024); MGS (p?=?0.033)]. In patients with the B1 variant, HPS scores were more consistently associated with duration [VGS (p?=?0.005); MGS (p?=?0.015), latency [VGS (p?=?0.022)]] and amplitude [MGS (p?=?0.006); VGS (p?=?0.005)]. The mediation analysis only revealed a significant indirect effect for amplitude in the MGS modality for the variable UPDRS-ON (p??0.05). All other clinical scales and brain connectivity parameters were not associated with behavioural traits. Collectively, our findings stress the role of striatal D2 and D3 signalling mechanisms in saccade generation and suggest that saccadic performance is associated with the clinical psychiatric state in Parkinson’s disease.
机译:为了了解两种多巴胺能信号传导途径的影响,Taqia RS1800497(影响纹状体D2受体密度)和Ser9GLY RS6280(影响纹状体D3多巴胺结合亲和力),在帕金森病中的扫视生成和精神病患者中,这项研究旨在调查帕金森患者的奇数或冲动行为的扫视性能协会;此外,我们质疑D2(A1 + / A1〜)和D3(B1 + / B1α)的变体是否不同地影响扫视参数,并且如果临床参数或脑连接性改变调节尼氏尾菌和尼硫核细胞的该关联。最初,将患者和对照与扫视性能进行比较,并且在记忆引导扫描囊(MGS)中的参数持续时间(MGS)和视觉引导(VGS)试验(P?<?0.0001)和MGS试验中的参数持续时间(P?<?0.03 )。我们能够在奇皮式行为(HPS)和Saccade参数(持续时间,延迟,增益和幅度)之间找到关联[MGS(P?= 0.036); VGS(p?= 0.033)],但不是脉冲行为。对于A1变体持续时间与HPS [VGS(p≤X.024)显着相关; mgs(p?= 0.033)]。在B1变体的患者中,HPS分数与持续时间持续相关[VGS(P?= 0.005); mgs(p?= 0.015),等待时间[Vgs(p?=Δ022)]和幅度[mgs(p?= 0.006); VGS(p?= 0.005)]。中介分析仅显示了MGS模态的振幅的显着间接效果,用于变量UPDRS-ON(P?<?0.05)。所有其他临床尺度和脑连接参数与行为性状无关。统称,我们的研究结果强调了骨垂D2和D3信号传导机制在扫视生成中的作用,并表明扫视性能与帕金森病的临床精神状态有关。

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