Emory University, Atlanta, GA, USA.
Sanders-Brown Center on Aging, University of Kentucky, Lexington, KY, USA.
Acta Neuropathol Commun. 2023 Jun 2;11(1):89. doi: 10.1186/s40478-023-01576-z.
In addition to the memory disorders and global cognitive impairment that accompany neurodegenerative diseases, behavioral and psychological symptoms of dementia (BPSD) commonly impair quality of life and complicate clinical management. To investigate clinical-pathological correlations of BPSD, we analyzed data from autopsied participants from the community-based University of Kentucky Alzheimer's Disease Research Center longitudinal cohort (n = 368 research volunteers met inclusion criteria, average age at death 85.4 years). Data assessing BPSD were obtained approximately annually, including parameters for agitation, anxiety, apathy, appetite problems, delusions, depression, disinhibition, hallucinations, motor disturbance, and irritability. Each BPSD was scored on a severity scale (0-3) via the Neuropsychiatric Inventory Questionnaire (NPI-Q). Further, Clinical Dementia Rating (CDR)-Global and -Language evaluations (also scored on 0-3 scales) were used to indicate the degree of global cognitive and language impairment. The NPI-Q and CDR ratings were correlated with neuropathology findings at autopsy: Alzheimer's disease neuropathological changes (ADNC), neocortical and amygdala-only Lewy bodies (LBs), limbic predominant age-related TDP-43 encephalopathy neuropathologic changes (LATE-NC), primary age-related tauopathy (PART), hippocampal sclerosis, and cerebrovascular pathologies. Combinations of pathologies included the quadruple misfolding proteinopathy (QMP) phenotype with co-occurring ADNC, neocortical LBs, and LATE-NC. Statistical models were used to estimate the associations between BPSD subtypes and pathologic patterns. Individuals with severe ADNC (particularly those with Braak NFT stage VI) had more BPSD, and the QMP phenotype was associated with the highest mean number of BPSD symptoms: > 8 different BPSD subtypes per individual. Disinhibition and language problems were common in persons with severe ADNC but were not specific to any pathology. "Pure" LATE-NC was associated with global cognitive impairment, apathy, and motor disturbance, but again, these were not specific associations. In summary, Braak NFT stage VI ADNC was strongly associated with BPSD, but no tested BPSD subtype was a robust indicator of any particular "pure" or mixed pathological combination.
除了伴随神经退行性疾病出现的记忆障碍和整体认知障碍外,痴呆的行为和心理症状(BPSD)通常也会降低生活质量,并使临床管理复杂化。为了研究 BPSD 的临床病理相关性,我们分析了来自基于社区的肯塔基大学阿尔茨海默病研究中心纵向队列(368 名符合研究条件的研究志愿者,平均死亡年龄为 85.4 岁)的尸检参与者的数据。每年大约都会评估一次 BPSD,包括激越、焦虑、淡漠、食欲问题、妄想、抑郁、抑制障碍、幻觉、运动障碍和易怒的参数。通过神经精神问卷(NPI-Q),对每个 BPSD 进行严重程度评分(0-3 分)。此外,临床痴呆评定量表(CDR)-整体和语言评估(也采用 0-3 分的评分)用于表示整体认知和语言障碍的程度。NPI-Q 和 CDR 评分与尸检时的神经病理学发现相关:阿尔茨海默病神经病理改变(ADNC)、皮质和杏仁核路易体(LBs)、边缘为主的年龄相关 TDP-43 脑炎神经病理改变(LATE-NC)、原发性年龄相关性 tau 病(PART)、海马硬化和脑血管病理学。病理学包括四重错误折叠蛋白病(QMP)表型与 ADNC、皮质 LBs 和 LATE-NC 同时发生。统计模型用于估计 BPSD 亚型与病理模式之间的关联。严重 ADNC(特别是 Braak NFT 阶段 VI)患者的 BPSD 更多,而 QMP 表型与平均出现的 BPSD 症状数量最多有关:每人超过 8 种不同的 BPSD 亚型。抑制障碍和语言问题在严重 ADNC 患者中很常见,但与任何一种病理学都没有特异性。“纯”LATE-NC 与整体认知障碍、淡漠和运动障碍相关,但这些都不是特定的关联。总之,Braak NFT 阶段 VI ADNC 与 BPSD 强烈相关,但没有一种经过测试的 BPSD 亚型是任何特定“纯”或混合病理组合的可靠指标。
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