Department of Medicine, University of Washington, Seattle.
Department of Rehabilitation Medicine, Mt Sinai School of Medicine, New York, New York.
JAMA Neurol. 2016 Sep 1;73(9):1062-9. doi: 10.1001/jamaneurol.2016.1948.
The late effects of traumatic brain injury (TBI) are of great interest, but studies characterizing these effects are limited.
To determine whether TBI with loss of consciousness (LOC) is associated with an increased risk for clinical and neuropathologic findings of Alzheimer disease (AD), Parkinson disease (PD), and other dementias.
DESIGN, SETTING, AND PARTICIPANTS: This study analyzed data from the Religious Orders Study (ROS), Memory and Aging Project (MAP), and Adult Changes in Thought study (ACT). All ROS and MAP participants and a subset of ACT participants consent to autopsy. Studies performed annual (ROS and MAP) or biennial (ACT) cognitive and clinical testing to identify incident cases of dementia and AD. The 7130 participants included members of a Seattle-area health care delivery system (ACT), priests and nuns living in orders across the United States (ROS), and Chicago-area adults in retirement communities (MAP). Of these, 1589 underwent autopsy. Primary hypothesis was that TBI with LOC would be associated with increased risk for AD and neurofibrillary tangles. Data were accrued from 1994 to April 1, 2014.
Self-reported TBI when the participant was free of dementia, categorized as no more than 1 vs more than 1 hour of LOC.
Clinical outcomes included incident all-cause dementia, AD, and PD in all studies and incident mild cognitive impairment and progression of parkinsonian signs in ROS and MAP. Neuropathologic outcomes included neurofibrillary tangles, neuritic plaques, microinfarcts, cystic infarcts, Lewy bodies, and hippocampal sclerosis in all studies.
Of 7130 participants (2879 [40.4%] men; overall mean [SD] age, 79.9 [6.9] years), 865 reported a history of TBI with LOC. In 45 190 person-years of follow-up, 1537 incident cases of dementia and 117 of PD were identified. No association was found between TBI with LOC and incident dementia (ACT: HR for TBI with LOC ≤1 hour, 1.03; 95% CI, 0.83-1.27; HR for TBI with LOC >1 hour, 1.18; 95% CI, 0.77-1.78; ROS and MAP: HR for TBI with LOC ≤1 hour, 0.87; 95% CI, 0.58-1.29; HR for TBI with LOC >1 hour, 0.84; 95% CI, 0.44-1.57) or AD (findings similar to those for dementia). Associations were found for TBI with LOC and incident PD in ACT (HR for TBI with LOC >1 hour, 3.56; 95% CI, 1.52-8.28) and progression of parkinsonian signs in ROS and MAP (odds ratio [OR] for TBI with LOC ≤1 hour, 1.65; 95% CI, 1.23-2.21; OR for TBI with LOC >1 hour, 2.23; 95% CI, 1.16-4.29). Traumatic brain injury with LOC was associated with Lewy bodies (any Lewy body in ACT: RR for TBI with LOC >1 hour, 2.64; 95% CI, 1.40-4.99; Lewy bodies in substantia nigra and/or locus ceruleus in ACT: RR for TBI with LOC >1 hour, 3.30; 95% CI, 1.71-6.38; Lewy bodies in frontal or temporal cortex in ACT: RR for TBI with LOC >1 hour, 5.73; 95% CI, 2.18-15.0; ROS and MAP: RR for TBI with LOC ≤1 hour, 1.64; 95% CI, 1.00-2.70; pooled RR for TBI with LOC ≤1 hour, 1.59; 95% CI, 1.06-2.39) and microinfarcts (any cortical microinfarct in ROS and MAP: RR for TBI with LOC >1 hour, 2.12; 95% CI, 1.12-4.01; pooled RR for TBI with LOC >1 hour, 1.58; 95% CI, 1.06-2.35).
Pooled clinical and neuropathologic data from 3 prospective cohort studies indicate that TBI with LOC is associated with risk for Lewy body accumulation, progression of parkinsonism, and PD, but not dementia, AD, neuritic plaques, or neurofibrillary tangles.
创伤性脑损伤 (TBI) 的迟发性效应备受关注,但描述这些效应的研究有限。
确定有无意识丧失 (LOC) 的 TBI 是否与阿尔茨海默病 (AD)、帕金森病 (PD) 和其他痴呆症的临床和神经病理学发现的风险增加相关。
设计、地点和参与者:本研究分析了宗教秩序研究 (ROS)、记忆与衰老项目 (MAP) 和成人思想变化研究 (ACT) 的数据。所有 ROS 和 MAP 参与者以及 ACT 参与者的一个子集同意接受尸检。研究每年 (ROS 和 MAP) 或每两年 (ACT) 进行认知和临床测试,以确定痴呆症和 AD 的发病病例。7130 名参与者包括西雅图地区医疗保健系统的成员 (ACT)、居住在美国各地的神职人员和修女 (ROS) 以及芝加哥地区退休社区的成年人 (MAP)。其中 1589 人接受了尸检。主要假设是 LOC 伴 TBI 与 AD 和神经纤维缠结的风险增加有关。数据于 1994 年至 2014 年 4 月 1 日累积。
参与者无痴呆时报告的 TBI,分为 LOC 不超过 1 小时和超过 1 小时。
临床结果包括所有研究中的全因痴呆、AD 和 PD 发病,以及 ROS 和 MAP 中的轻度认知障碍和帕金森病体征进展。神经病理学结果包括所有研究中的神经纤维缠结、神经原纤维缠结、微梗死、囊性梗死、路易体和海马硬化。
在 7130 名参与者(2879 名男性[40.4%];总体平均[SD]年龄,79.9[6.9]岁)中,865 名报告了有 LOC 伴 TBI 的病史。在 45190 人年的随访中,发现 1537 例痴呆和 117 例 PD 发病。LOC 伴 TBI 与痴呆发病无关联(ACT:LOC 伴 TBI 持续时间不超过 1 小时的 HR,1.03;95%CI,0.83-1.27;LOC 伴 TBI 持续时间超过 1 小时的 HR,1.18;95%CI,0.77-1.78;ROS 和 MAP:LOC 伴 TBI 持续时间不超过 1 小时的 HR,0.87;95%CI,0.58-1.29;LOC 伴 TBI 持续时间超过 1 小时的 HR,0.84;95%CI,0.44-1.57)或 AD(与痴呆的发现相似)。ACT 中发现 LOC 伴 TBI 与 PD 发病相关(LOC 伴 TBI 持续时间超过 1 小时的 HR,3.56;95%CI,1.52-8.28),ROS 和 MAP 中发现 LOC 伴 TBI 与帕金森病体征进展相关(LOC 伴 TBI 持续时间不超过 1 小时的 OR,1.65;95%CI,1.23-2.21;LOC 伴 TBI 持续时间超过 1 小时的 OR,2.23;95%CI,1.16-4.29)。LOC 伴 TBI 与路易体有关(ACT 中任何路易体的 RR,LOC 伴 TBI 持续时间超过 1 小时的 RR,2.64;95%CI,1.40-4.99;LOC 伴 TBI 持续时间超过 1 小时的 RR,3.30;95%CI,1.71-6.38;LOC 伴 TBI 持续时间超过 1 小时的 RR,5.73;95%CI,2.18-15.0;ROS 和 MAP:LOC 伴 TBI 持续时间不超过 1 小时的 RR,1.64;95%CI,1.00-2.70;LOC 伴 TBI 持续时间不超过 1 小时的合并 RR,1.59;95%CI,1.06-2.39)和微梗死(ROS 和 MAP 中任何皮质微梗死的 RR,LOC 伴 TBI 持续时间超过 1 小时的 RR,2.12;95%CI,1.12-4.01;LOC 伴 TBI 持续时间超过 1 小时的 RR,1.58;95%CI,1.06-2.35)。
3 项前瞻性队列研究的汇总临床和神经病理学数据表明,LOC 伴 TBI 与路易体堆积、帕金森病进展和 PD 相关,但与痴呆症、AD、神经原纤维缠结无关。
