corpus callosum

Callosum Corpus Callosum
  • 文章类型: Journal Article
    可以观察到各种疾病继发的RESLES(可逆性脾病变综合征),淀粉样蛋白内水肿可能在SCC(call体脾)的发病机理中起关键作用。一些研究表明,缺氧缺血性脑病可能是SCC病变的危险因素。然而,高海拔环境对SCC的潜在影响,尤其是在慢性暴露期间,保持模糊。
    我们的研究包括19名在高海拔地区符合RESLES诊断标准的患者。包括十名患有RESLES的低海拔患者作为对照。所有参与者都接受了两次MRI(磁共振成像)扫描。常规血液检查,肝脏,肾脏和甲状腺功能,凝血功能,在住院期间和出院前检测电解质和维生素.此外,患者于2023年5月获得随访.
    高海拔的低氧环境可能会增加RESLES的风险。两组均表现出不同的临床症状。高海拔患者的CRP水平明显高于低海拔患者。高海拔患者的病变大小与SaO2水平呈正相关。然而,低海拔的患者病变大小与几种炎症标志物呈正相关趋势(WBC,NEU和CRP)。所有患者的预后良好,可能不受醋酸泼尼松的影响。
    高海拔地区的低氧环境可能在RESLES的病因中起作用。此外,RESLES是一种可逆的疾病,糖皮质激素的给药对于其治疗可能是不必要的。
    UNASSIGNED: RESLES (Reversible splenial lesion syndrome) can be observed secondary to various diseases, and intramyelinic edema may play a crucial role in the pathogenesis of SCC (Splenium of the corpus callosum). Some studies have suggested that hypoxic-ischaemic encephalopathy may constitute a risk factor for SCC lesions. However, the potential impact of high-altitude environments on SCC, especially during chronic exposure, remain obscure.
    UNASSIGNED: Our study included 19 patients who satisfied the diagnostic criteria of RESLES at high altitudes. Ten low-altitude patients with RESLES were included as controls. All participants received MRI (Magnetic resonance imaging) scans twice. Routine blood tests, liver, kidney and thyroid function, coagulation function, electrolytes and vitamins were detected during hospitalization and before discharge. In addition, the patients were followed up in May 2023.
    UNASSIGNED: Hypoxic environments at high altitudes may increase the risk of RESLES. The two groups showed different clinical symptoms. High-altitude patients had significantly higher CRP levels than low-altitude patients. The lesion size in high-altitude patients showed a positive correlation with SaO2 levels. However, the patients at low altitudes had positive correlation trends between lesion size and several inflammatory markers (WBC, NEU and CRP). All patients had a benign prognosis that may not be affected by the use of prednisone acetate.
    UNASSIGNED: Hypoxic environments at high altitudes may play a role in the aetiology of RESLES. Additionally, RESLES is a reversible disease and the administration of glucocorticoids may be dispensable for its treatment.
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  • 文章类型: Journal Article
    多发性硬化症(MS)是一种使人衰弱的脱髓鞘疾病,其特征是由于少突胶质细胞前体细胞(OPCs)分化不足和异常星形胶质细胞增生而导致的髓鞘再生失败。临床标本的全面细胞图谱重新分析揭示了特定星形胶质细胞亚型中聚集蛋白(CLU)的表达与MS患者的活动性病变有关。我们的调查显示,患者组织的活跃病变和雌性鼠MS模型中星形胶质细胞CLU水平均升高。CLU给药刺激原发性星形胶质细胞增殖,同时阻碍星形胶质细胞介导的髓磷脂碎片清除。有趣的是,CLU过载直接阻碍OPC分化并诱导OPC和OLs凋亡。机械上,CLU通过极低密度脂蛋白受体抑制原发性OPCs中的PI3K-AKT信号传导.AKT的药理激活挽救了过量CLU对OPCs造成的损害,并改善了call体的脱髓鞘。此外,CLU的有条件敲除成为一种有希望的干预措施,在小鼠MS模型中展示了改善的髓鞘再生过程和降低的严重程度。
    Multiple sclerosis (MS) is a debilitating demyelinating disease characterized by remyelination failure attributed to inadequate oligodendrocyte precursor cells (OPCs) differentiation and aberrant astrogliosis. A comprehensive cell atlas reanalysis of clinical specimens brings to light heightened clusterin (CLU) expression in a specific astrocyte subtype links to active lesions in MS patients. Our investigation reveals elevated astrocytic CLU levels in both active lesions of patient tissues and female murine MS models. CLU administration stimulates primary astrocyte proliferation while concurrently impeding astrocyte-mediated clearance of myelin debris. Intriguingly, CLU overload directly impedes OPC differentiation and induces OPCs and OLs apoptosis. Mechanistically, CLU suppresses PI3K-AKT signaling in primary OPCs via very low-density lipoprotein receptor. Pharmacological activation of AKT rescues the damage inflicted by excess CLU on OPCs and ameliorates demyelination in the corpus callosum. Furthermore, conditional knockout of CLU emerges as a promising intervention, showcasing improved remyelination processes and reduced severity in murine MS models.
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  • 文章类型: Journal Article
    研究表明,肌萎缩侧索硬化症(ALS)损害了白质纤维束的完整性,主要影响电机纤维。然而,尚不确定这些纤维的完整性是否会影响ALS的风险。我们进行了双向双样本孟德尔随机化(MR)和多变量MR分析,以评估纤维束(包括皮质脊髓束(CST)和call体(CC))的完整性与ALS风险之间的关联关系。从已发表的全基因组关联研究(GWAS)获得了特定纤维束的遗传工具变量,包括来自五个扩散磁共振成像(dMRI)数据集的33,292名欧洲个体。ALS的汇总水平GWAS数据来自27,205名ALS患者和110,881名对照。MR结果表明,CC(GCC)类型中分数各向异性(FA)的第一主成分(PC1)的增加与ALS的风险增加相关(PFDR=0.001,比值比=1.363,95%置信区间1.178-1.577)。尽管其他神经影像学表型[CST中的平均扩散率,CST中的径向扩散率(RD),海湾合作委员会中的FA,CC(BCC)正文中的PC1,CST中的PC1,和RD在GCC]没有通过修正,他们也被认为与ALS的风险有暗示性关联.没有证据表明ALS引起纤维束完整性的变化。总之,这项研究的结果为特定纤维束的完整性与ALS风险之间的潜在关联提供了遗传支持.GCC和BCC中更高的纤维完整性可能是ALS的风险因素,而CST中更大的纤维完整性可能对ALS具有保护作用。这项研究提供了对ALS发展的见解。
    Studies suggest that amyotrophic lateral sclerosis (ALS) compromises the integrity of white matter fiber tracts, primarily affecting motor fibers. However, it remains uncertain whether the integrity of these fibers influences the risk of ALS. We performed bidirectional two-sample Mendelian randomization (MR) and multivariable MR analyses to evaluate the associative relationships between the integrity of fiber tracts [including the corticospinal tract (CST) and corpus callosum (CC)] and the risk of ALS. Genetic instrumental variables for specific fiber tracts were obtained from published genome-wide association studies (GWASs), including 33,292 European individuals from five diffusion magnetic resonance imaging (dMRI) datasets. Summary-level GWAS data for ALS were derived from 27,205 ALS patients and 110,881 controls. The MR results suggested that an increase in the first principal component (PC1) of fractional anisotropy (FA) in the genu of the CC (GCC) was correlated with an increased risk of ALS (PFDR = 0.001, odds ratio = 1.363, 95% confidence interval 1.178-1.577). Although other neuroimaging phenotypes [mean diffusivity in the CST, radial diffusivity (RD) in the CST, FA in the GCC, PC1 in the body of the CC (BCC), PC1 in the CST, and RD in the GCC] did not pass correction, they were also considered to have suggestive associations with the risk of ALS. No evidence revealed that ALS caused changes in the integrity of fiber tracts. In summary, the results of this study provide genetic support for the potential association between the integrity of specific fiber tracts and the risk of ALS. Greater fiber integrity in the GCC and BCC may be a risk factor for ALS, while greater fiber integrity in the CST may have a protective effect on ALS. This study provides insights into ALS development.
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  • 文章类型: Journal Article
    该研究旨在研究HEK293-XPack-Olig2细胞衍生的外泌体对铜宗诱导的脱髓鞘疾病模型中call体髓鞘再生的治疗影响。使用XPack技术构建表达Olig2的慢病毒载体。通过离心分离高度丰富的Olig2外泌体(ExoO)用于后续实验。蛋白质印迹,纳米粒子跟踪分析(NTA),和电子显微镜显示Exos和ExoOs之间的颗粒尺寸和形态没有显着差异,在Exoos中可以检测到高水平的Olig2表达,表明XPack技术的外泌体修饰是成功的。黑金/氟髓磷脂染色分析表明,与PBS和Exos组相比,ExoOs组明显减少了call体的脱髓鞘区域。此外,脱髓鞘区的PDGFRa/APC染色显示,ExoOs组中APC+少突胶质细胞增加,PDGFRa+少突胶质祖细胞(OPCs)减少。此外,在Exoos治疗后,脱髓鞘区域有明显的髓鞘再生,与其他治疗组相比,具有更好的g比和更高的完整髓鞘数量。与PBS和Exos组相比,ExoOs组的脑组织中的SoxlO表达水平更高。XPack修饰的外泌体可以显著减缓脱髓鞘过程,促进了OPCs的差异化,病理条件下髓磷脂再生加速。推测该过程是通过在外来体转运Olig2富集到少突胶质细胞祖细胞中后改变细胞内分化相关基因的表达水平来实现的。
    The research aims to study the therapeutic impact of HEK293-XPack-Olig2 cell-derived exosomes on remyelination of the corpus callosum in a cuprizone-induced demyelinating disease model. A lentiviral vector expressing Olig2 was constructed using XPack technology. The highly abundant Olig2 exosomes (ExoOs) were isolated by centrifugation for subsequent experiments. Western blot, nanoparticle tracking analysis (NTA), and electron microscopy showed no significant difference in particle size and morphology between Exos and ExoOs, and a high level of Olig2 expression could be detected in ExoOs, indicating that exosome modification by XPack technology was successful. The Black Gold/Fluromyelin staining analysis showed that the ExoOs group significantly reduced the demyelination area in the corpus callosum compared to the PBS and Exos groups. Additionally, the PDGFRα/APC staining of the demyelinating region revealed an increase in APC+ oligodendrocytes and a decrease in PDGFRα+ oligodendrocyte progenitor cells (OPCs) in the ExoOs group. Furthermore, there was evident myelin regeneration in the demyelinated areas after ExoOs treatment, with better g-ratio and a higher number of intact myelin compared to the other treatment groups. The level of Sox10 expression in the brain tissue of the ExoOs group were higher compared to those of the PBS and Exos groups. The demyelination process can be significantly slowed down by the XPack-modified exosomes, the differentiation of OPCs promoted, and myelin regeneration accelerated under pathological conditions. This process is presumed to be achieved by changing the expression level of intracellular differentiation-related genes after exosomes transport Olig2 enriched into oligodendrocyte progenitors.
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  • 文章类型: Meta-Analysis
    背景:重度抑郁障碍(MDD)是一种普遍且致残的情绪障碍,被认为与脑白质(WM)改变有关。先前的扩散张量成像(DTI)研究报告了MDD患者不同大脑区域的分数各向异性(FA)变化不一致。然而,这些研究均未使用原始t图数据进行MDD的WM荟萃分析。我们的研究旨在通过使用基于种子的d映射通过受试者图像排列(SDM-PSI)对MDD中的FA进行基于全脑的荟萃分析来解决这一差距,结合报告的峰坐标和原始统计参数图。
    目标:遵循PRISMA指南,我们进行了系统检索和荟萃分析,以比较MDD患者与健康对照(HC)的FA.我们的目标是识别MDD中的WM异常,使用SDM,这可以揭示这种疾病的发病机理。
    结果:荟萃分析包括39项研究,3696名参与者(2094名MDD,1602HC)。它揭示了MDD患者,与HC相比,在call体(CC)和前丘脑投射(ATP)中具有较低的FA。亚组分析表明,CC是MDD中更稳定的致病因子。荟萃回归分析显示,平均年龄之间没有线性相关,女性患者的百分比,抑郁症的持续时间,和FA异常。这表明半球间连接和前丘脑皮质回路的WM损伤在MDD的发病机理中很重要。
    BACKGROUND: Major depressive disorder (MDD) is a prevalent and disabling mood disorder, thought to be linked with brain white matter (WM) alterations. Prior diffusion tensor imaging (DTI) studies have reported inconsistent changes in fractional anisotropy (FA) across different brain regions in MDD patients. However, none of these studies utilized raw t-map data for WM meta-analysis in MDD. Our study aims to address this gap by conducting a whole-brain-based meta-analysis of FA in MDD using Seed-based d mapping via permutation of subject images (SDM-PSI), combining reported peak coordinates and raw statistical parametric maps.
    OBJECTIVE: Following PRISMA guidelines, we performed a systematic search and meta-analysis to compare FA in MDD patients with healthy controls (HC). Our goal was to identify WM abnormalities in MDD, using SDM, which could shed light on the disorder\'s pathogenesis.
    RESULTS: The meta-analysis included 39 studies with 3696 participants (2094 with MDD, 1602HC). It revealed that MDD patients, in comparison to HC, have lower FA in the corpus callosum (CC) and anterior thalamic projections (ATP). Subgroup analyses indicated that the CC is a more stable pathogenic factor in MDD. Meta-regression analyses showed no linear correlation between the mean age, percentage of female patients, duration of depression, and FA abnormalities. This suggests that WM impairments in interhemispheric connections and anterior thalamocortical circuits are significant in the pathogenesis of MDD.
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  • 文章类型: Case Reports
    胼胝体损伤是中风后发生的一种罕见类型的损伤,可导致下肢功能障碍和日常生活能力活动下降。此外,目前还没有研究集中在由胼胝体梗死引起的下肢功能障碍的康复进展和有效的治疗方案。我们旨在介绍两名中风后call体梗死引起的下肢功能障碍患者的报告和步行训练方法。
    我们实施了一种步行训练方法,该方法优先考虑双侧对称性,并在患者建立坐/站平衡之前增加侧向摇摆。该计划是改善call体梗死引起的步行功能障碍的快速有效方法。
    在突发call体梗死后,两名患者的下肢运动功能评分均显著降低,并表现出明显的步态障碍.量表评估证实,对于call体梗死后下肢运动功能障碍的患者,基于对称和增加的横向摇摆的步行训练可导致症状显着改善。
    我们报告了2例call体梗死患者的突发性运动功能障碍。对称和增加的基于横向摇摆的步行训练导致症状的实质性改善。经比额表评估确认。
    UNASSIGNED: Corpus callosum injury is a rare type of injury that occurs after a stroke and can cause lower limb dysfunction and a decrease in activities of daily living ability. Furthermore, there are no studies that focus on the progress in rehabilitation of the lower limb dysfunction caused by infarction in the corpus callosum and the effective treatment plans for this condition. We aimed to present a report of two patients with lower limb dysfunction caused by corpus callosum infarction after a stroke and a walking training method.
    UNASSIGNED: We implemented a walking training method that prioritizes bilateral symmetry and increases lateral swaying before the patients established sitting/standing balance. The plan is a rapid and effective method for improving walking dysfunction caused by corpus callosum infarction.
    UNASSIGNED: Following sudden corpus callosum infarction, both patients experienced a significant reduction in lower limb motor function scores and exhibited evident gait disorders. Scale evaluations confirmed that walking training based on symmetrical and increased lateral sway for patients with lower limb motor dysfunction after corpus callosum infarction led to significant symptom improvement.
    UNASSIGNED: We report two cases of sudden motor dysfunction in patients with corpus callosum infarction. Symmetrical and increased lateral sway-based walking training resulted in substantial symptom improvement, as confirmed by scale assessments.
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  • 文章类型: Journal Article
    背景:据报道,成人发病的甲状腺功能减退症患者的call体(CC)中存在磁共振成像(MRI)脑异常。然而,尚无研究直接比较亚临床甲状腺功能减退症(SCH)中CC特异性形态学或功能改变,明显的甲状腺功能减退症(OH),和健康对照(HC)。此外,CC改变与认知和情绪的关系尚不清楚。
    方法:人口统计数据,临床变量,神经心理学评分,和152名参与者的MRI数据(60SCH,37OH,和55HC)被收集。这项研究调查了临床表现,三组CC亚区的形态和功能变化。此外,我们进行了相关分析,以探索这些因素之间的潜在关系.
    结果:与HC相比,SCH和OH组表现出较低的认知评分和较高的抑郁/焦虑评分。值得注意的是,SCH组CC的柱体和柱体体积较大。头端体之间的功能连接,SCH组的前中体和右中央和背外侧额上回增加。相比之下,SCH和OH基团在脾和右角回之间的功能连通性下降。在SCH组中,讲台体积与蒙特利尔认知评估和视觉空间/执行分数呈负相关,同时显示与24项汉密尔顿抑郁量表评分呈正相关。在OH基团中,头端体体积与血清促甲状腺激素水平呈负相关,而与血清总甲状腺素和游离甲状腺素水平呈正相关。
    结论:本研究提示不同阶段的成人发病甲状腺功能减退患者可能表现出不同的CC异常模式。这些发现为甲状腺功能减退症的神经病理生理机制提供了新的见解。
    BACKGROUND: Magnetic resonance imaging (MRI) brain abnormalities have been reported in the corpus callosum (CC) of patients with adult-onset hypothyroidism. However, no study has directly compared CC-specific morphological or functional alterations among subclinical hypothyroidism (SCH), overt hypothyroidism (OH), and healthy controls (HC). Moreover, the association of CC alterations with cognition and emotion is not well understood.
    METHODS: Demographic data, clinical variables, neuropsychological scores, and MRI data of 152 participants (60 SCH, 37 OH, and 55 HC) were collected. This study investigated the clinical performance, morphological and functional changes of CC subregions across three groups. Moreover, a correlation analysis was performed to explore potential relationships between these factors.
    RESULTS: Compared to HC, SCH and OH groups exhibited lower cognitive scores and higher depressive/anxious scores. Notably, rostrum and rostral body volume of CC was larger in the SCH group. Functional connectivity between rostral body, anterior midbody and the right precentral and dorsolateral superior frontal gyrus were increased in the SCH group. In contrast, the SCH and OH groups exhibited a decline in functional connectivity between splenium and the right angular gyrus. Within the SCH group, rostrum volume demonstrated a negative correlation with Montreal Cognitive Assessment and visuospatial/executive scores, while displaying a positive correlation with 24-item Hamilton Depression Rating Scale scores. In the OH group, rostral body volume exhibited a negative correlation with serum thyroid stimulating hormone levels, while a positive correlation with serum total thyroxine and free thyroxine levels.
    CONCLUSIONS: This study suggests that patients with different stages of adult-onset hypothyroidism may exhibit different patterns of CC abnormalities. These findings offer new insights into the neuropathophysiological mechanisms in hypothyroidism.
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  • 文章类型: Case Reports
    在这里,我们描述了一名18岁的妇女,她最初在精神病院被误诊为精神疾病。她因为意识受损被转移到我们的神经病房。神经元抗体检测证实了抗N-甲基-D-天冬氨酸受体(NMDAR)脑炎的诊断。脑磁共振成像(MRI)显示伴随疾病,称为可逆性脾病变综合征(RESLES)。联合免疫治疗后,患者出院后3个月完全康复.据我们所知,仅在两名畸胎瘤患者中描述了RESLES和抗NMDAR脑炎的同时发生,我们提供了另一例无畸胎瘤的病例.我们强调抗NMDAR抗体可以添加到RESLES的多种原因中。因此,临床医生必须检测RESLES患者的抗神经元抗体,以避免漏诊。
    Here we described an 18-year-old woman who were initially misdiagnosed as psychiatric disorders in a psychiatric institution. She was transferred to our neurological ward because of impaired consciousness. Neuronal antibody testing confirmed the diagnosis of anti-N-methyl-D-aspartate receptor (NMDAR) encephalitis. Cerebral magnetic resonance imaging (MRI) revealed a concomitant disorder named reversible splenial lesion syndrome (RESLES). After administration of combined immunotherapy, the patient recovered completely 3 months after discharge. To our knowledge, co-occurrence of RESLES and anti-NMDAR encephalitis was only described in two patients with teratoma and we provide another case without teratoma. We highlight that anti-NMDAR antibodies can be added to the multiple causes of RESLES. It is therefore imperative for clinicians to detect anti-neuronal antibodies in patients with RESLES to avoid missed diagnosis.
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  • 文章类型: Journal Article
    扩散张量成像(DTI)已成为一种有前途的神经成像工具,用于检测爆炸引起的轻度创伤性脑损伤(bmTBI)。然而,缺乏精细的急性期监测和可靠的影像学生物标志物,阻碍了其在早期诊断bmTBI的临床应用,导致患者潜在的长期残疾。这里,我们在暴露于单个侧向冲击波(151.16和349.75kPa,持续47.48ms)在密闭生物休克管(BST-I)中释放,以研究受伤后1、3、7天bmTBI急性期的全脑DTI变化。免疫组织化学分析的联合评估,透射电子显微镜(TEM)和行为读数允许将DTI变化与同步细胞损伤联系起来,并确定稳定的成像生物标志物。call体(CC)和脑干被确定为主要受影响区域,其中早在受伤后的第一天就检测到降低的分数各向异性(FA),最大下降发生在受伤后3天,然后在7天恢复到接近正常水平。损伤后3天,CC和脑干内的轴向扩散率(AD)值也显着降低。相比之下,CC中的径向扩散率(RD)显示为急性升高,在受伤后3天达到峰值,然后在7天时间点恢复正常。对神经纤维的损伤,包括脱髓鞘和轴突变性,随着DTI参数的变化而进展,支持DTI对微观神经元纤维损伤的实时宏观反射。最敏感的生物标志物被确定为FA降低,受伤后第三天,AD和CC内RD增加,支持DTI在急性期bmTBI病例中的诊断实用性。
    Diffusion tensor imaging (DTI) has emerged as a promising neuroimaging tool for detecting blast-induced mild traumatic brain injury (bmTBI). However, lack of refined acute-phase monitoring and reliable imaging biomarkers hindered its clinical application in early diagnosis of bmTBI, leading to potential long-term disability of patients. In this study, we used DTI in a rat model of bmTBI generated by exposing to single lateral blast waves (151.16 and 349.75 kPa, lasting 47.48 ms) released in a confined bioshock tube, to investigate whole-brain DTI changes at 1, 3, and 7 days after injury. Combined assessment of immunohistochemical analysis, transmission electron microscopy, and behavioral readouts allowed for linking DTI changes to synchronous cellular damages and identifying stable imaging biomarkers. The corpus callosum (CC) and brainstem were identified as predominantly affected regions, in which reduced fractional anisotropy (FA) was detected as early as the first day after injury, with a maximum decline occurring at 3 days post-injury before returning to near normal levels by 7 days. Axial diffusivity (AD) values within the CC and brainstem also significantly reduced at 3 days post-injury. In contrast, the radial diffusivity (RD) in the CC showed acute elevation, peaking at 3 days after injury before normalizing by the 7-day time point. Damages to nerve fibers, including demyelination and axonal degeneration, progressed in lines with changes in DTI parameters, supporting a real-time macroscopic reflection of microscopic neuronal fiber injury by DTI. The most sensitive biomarker was identified as a decrease in FA, AD, and an increase in RD within the CC on the third day after injury, supporting the diagnostic utility of DTI in cases of bmTBI in the acute phase.
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  • 文章类型: Journal Article
    目的:Tourette综合征(TS)是一种神经发育障碍,可引起突然不受控制的快速和重复的声音或称为抽动的运动。在这里,采用扩散磁共振成像(dMRI)连接测量技术评估TS患者的白质连接差异.
    方法:本研究共纳入63名TS和77名典型发育(TD)个体。基于定量各向异性(QA),使用dMRI连接测量法识别TS患者白质束连接模式的差异。比较了TS和TD患者之间的QA,并与严重程度评分相关,例如耶鲁全球抽动严重程度量表(YGTSS)和抽动先兆急迫量表(PUTS)。
    结果:相对于TD,TS中call体和双侧扣带的白质连通性较高,皮质丘脑和皮质纹状体通路的连通性较低。基线YGTSS电机,YGTSS总计,和PUTS与皮质纹状体通路呈负相关,皮质丘脑途径,和双侧扣带完整性,分别。行为治疗后,抽动严重程度评分的变化也与这些大脑区域白质完整性的改变呈正相关。
    结论:TS患者的白质微结构有几种异常,特别是在皮质-纹状体-丘脑-皮质(CSTC)回路中,与疾病的严重程度有关。此外,行为治疗后这些区域白质完整性的变化被证明是反应预测因子.
    OBJECTIVE: Tourette syndrome (TS) is a neurodevelopmental disorder that cause sudden uncontrolled rapid and repeated vocal sounds or movements called tics. Herein, diffusion magnetic resonance imaging (dMRI) connectometry was implemented to evaluate the white matter connectivity differences among TS patients.
    METHODS: A total of 63 TS and 77 typically developed (TD) individuals were enrolled in the present study. dMRI connectometry was utilized to identify differences in connectivity patterns of white matter tracts in TS patients based on quantitative anisotropy (QA). QA was compared between TS and TD patients and correlated with severity scores such as Yale Global Tic Severity Scale (YGTSS) and Premonitory Urge for Tics Scale (PUTS).
    RESULTS: Higher white matter connectivity of corpus callosum and bilateral cingulum as well as lower connectivity of corticothalamic and corticostriatal pathways were evident in TS relative to TD. The baseline YGTSS motor, YGTSS total, and PUTS were negatively correlated with corticostriatal pathway, corticothalamic pathway, and bilateral cingulum integrity, respectively. The changes in tic severity scores were also positively correlated with alterations in the white matter integrity of these brain regions following behavioral therapy.
    CONCLUSIONS: Patients with TS have several abnormalities in their white matter microstructure particularly in the cortico-striato-thalamo-cortical (CSTC) circuit, correlated with the severity of the disease. Besides, the post-behavioral therapy changes in the white matter integrity of these regions are demonstrated as response predictors.
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