Department of Neurodegenerative Disease, Dementia Research Centre, UCL Institute of Neurology, London, UK.
Department of Neurology, Erasmus Medical Centre, Rotterdam, Netherlands.
Appl Neuropsychol Adult. 2022 Jan-Feb;29(1):112-119. doi: 10.1080/23279095.2020.1716357. Epub 2020 Feb 5.
Impaired semantic knowledge is a characteristic feature of some forms of frontotemporal dementia (FTD), particularly the sporadic disorder semantic dementia. Less is known about semantic cognition in the genetic forms of FTD caused by mutations in the genes , , and . We developed a modified version of the Camel and Cactus Test (mCCT) to investigate the presence of semantic difficulties in a large genetic FTD cohort from the Genetic FTD Initiative (GENFI) study. Six-hundred-forty-four participants were tested with the mCCT including 67 mutation carriers (15 symptomatic, and 52 in the presymptomatic period), 165 mutation carriers (33 symptomatic, 132 presymptomatic), and 164 mutation carriers (56 symptomatic, 108 presymptomatic) and 248 mutation-negative members of FTD families who acted as a control group. The presymptomatic mutation carriers were further split into those early and late in the presymptomatic period (more than vs. within 10 years of expected symptom onset). Groups were compared using a linear regression model, adjusting for age and education, with bootstrapping. Performance on the mCCT had a weak negative correlation with age (rho = -0.20) and a weak positive correlation with education (rho = 0.13), with an overall abnormal score (below the 5th percentile of the control population) being below 27 out of a total of 32. All three of the symptomatic mutation groups scored significantly lower than controls: mean 22.3 (standard deviation 8.0), 24.4 (7.2), 23.6 (6.5) and controls 30.2 (1.6). However, in the presymptomatic groups, only the late and late mutation groups scored lower than controls (28.8 (2.2) and 28.9 (2.5) respectively). Performance on the mCCT correlated strongly with temporal lobe volume in the symptomatic mutation group (rho > 0.80). In the group, mCCT score correlated with both bilateral temporal lobe volume (rho > 0.31) and bilateral frontal lobe volume (rho > 0.29), whilst in the group mCCT score correlated only with left frontal lobe volume (rho = 0.48). This study provides evidence for presymptomatic impaired semantic knowledge in genetic FTD. The different neuroanatomical associations of the mCCT score may represent distinct cognitive processes causing deficits in different groups: loss of core semantic knowledge associated with temporal lobe atrophy (particularly in the group), and impaired executive control of semantic information associated with frontal lobe atrophy. Further studies will be helpful to address the longitudinal change in mCCT performance and the exact time at which presymptomatic impairment occurs.
语义知识受损是某些形式额颞叶痴呆(FTD)的特征,特别是散发性语义痴呆。对于由基因 、 和 突变引起的 FTD 的遗传形式的语义认知知之甚少。我们开发了一种改良的骆驼和仙人掌测试(mCCT),以调查来自遗传 FTD 倡议(GENFI)研究的大型遗传 FTD 队列中是否存在语义困难。共有 644 名参与者接受了 mCCT 测试,包括 67 个 突变携带者(15 名症状性,52 名处于无症状期),165 个 突变携带者(33 名症状性,132 名无症状期),和 164 个 突变携带者(56 名症状性,108 名无症状期)以及 248 名 FTD 家族的突变阴性成员作为对照组。无症状突变携带者进一步分为早期和晚期无症状期(超过 vs. 预计症状发作前 10 年)。使用线性回归模型进行比较,调整年龄和教育,使用引导。mCCT 的表现与年龄呈弱负相关(rho=-0.20),与教育呈弱正相关(rho=0.13),总分共 32 分,总异常分数(低于对照组人群第 5 百分位数)低于 27。所有三个症状性突变组的得分均明显低于对照组: 平均 22.3(标准差 8.0), 24.4(7.2), 23.6(6.5)和对照组 30.2(1.6)。然而,在无症状组中,只有晚期 和晚期 突变组的得分低于对照组(分别为 28.8(2.2)和 28.9(2.5))。mCCT 在症状性 突变组中的表现与颞叶体积强烈相关(rho>0.80)。在 组中,mCCT 评分与双侧颞叶体积(rho>0.31)和双侧额叶体积(rho>0.29)相关,而在 组中,mCCT 评分仅与左侧额叶体积(rho=0.48)相关。这项研究为遗传 FTD 的无症状期语义知识受损提供了证据。mCCT 评分的不同神经解剖学关联可能代表不同的认知过程,导致不同组的缺陷:与颞叶萎缩相关的核心语义知识丧失(特别是在 组中),以及与额叶萎缩相关的语义信息执行控制受损。进一步的研究将有助于解决 mCCT 表现的纵向变化以及无症状期损伤发生的确切时间。
