Human Alzheimer's Disease ATN/ABC Staging Applied to Aging Rhesus Macaque Brains: Association With Cognition and MRI-Based Regional Gray Matter Volume

IF 2.1 4区 医学 Q3 NEUROSCIENCES Journal of Comparative Neurology Pub Date : 2024-09-24 DOI:10.1002/cne.25670
Carol A. Barnes, Michele R. Permenter, Julie A. Vogt, Kewei Chen, Thomas G. Beach
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Abstract

The brain changes of Alzheimer's disease (AD) include Abeta (Aβ) amyloid plaques (“A”), abnormally phosphorylated tau tangles (“T”), and neurodegeneration (“N”). These have been used to construct in vivo and postmortem diagnostic and staging classifications for evaluating the spectrum of AD in the “ATN” and “ABC” (“B” for Braak tau stage, “C” for Consortium to Establish a Registry for Alzheimer's Disease [CERAD] neuritic plaque density) systems. Another common AD feature involves cerebral amyloid angiopathy (CAA). We report the first experiment to examine relationships among cognition, brain distribution of amyloid plaques, CAA, tau/tangles, and magnetic resonance imaging (MRI)-determined volume changes (as a measure of “N”) in the same group of behaviorally characterized nonhuman primates. Both ATN and ABC systems were applied to a group of 32 rhesus macaques aged between 7 and 33 years. When an immunohistochemical method for “T” and “B” was used, some monkeys were “triple positive” on ATN, with a maximum ABC status of A1B2C3. With silver or thioflavin S methods, however, all monkeys were classified as T-negative and B0, indicating the absence of mature neurofibrillary tangles (NFTs) and hence neuropathologically defined AD. Although monkeys at extremes of the ATN and ABC classifications, or with frequent CAA, had significantly lower scores on some cognitive tests, the lack of fully mature NFTs or dementia-consistent cognitive impairment indicates that fully developed AD may not occur in rhesus macaques. There were sex differences noted in the types of histopathology present, and only CAA was significantly related to gray matter volume.

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将人类阿尔茨海默病 ATN/ABC 分期应用于老年猕猴大脑:与认知和基于核磁共振成像的区域灰质体积的关联。
阿尔茨海默病(AD)的脑部变化包括 Abeta(Aβ)淀粉样蛋白斑块("A")、异常磷酸化的 tau 结("T")和神经变性("N")。这些已被用于构建体内和死后诊断和分期分类,以评估 "ATN "和 "ABC"("B "表示 Braak tau 阶段,"C "表示建立阿尔茨海默病登记联盟[CERAD]神经窦斑块密度)系统中的阿氏症谱系。另一个常见的阿尔茨海默病特征是脑淀粉样血管病(CAA)。我们首次报道了在同一组具有行为特征的非人灵长类动物中研究认知能力、大脑淀粉样斑块分布、CAA、tau/tangles 和磁共振成像(MRI)确定的体积变化(作为 "N "的度量)之间关系的实验。ATN 和 ABC 系统都适用于一组 32 只年龄在 7 到 33 岁之间的猕猴。当使用 "T "和 "B "的免疫组化方法时,一些猴子的 ATN 呈 "三阳性",ABC 状态最高为 A1B2C3。然而,使用银法或硫黄素 S 法,所有猴子都被归类为 T 阴性和 B0,表明没有成熟的神经纤维缠结(NFT),因此神经病理学上定义为 AD。虽然处于ATN和ABC分类极端或经常出现CAA的猴子在某些认知测试中得分明显较低,但缺乏完全成熟的NFT或与痴呆症一致的认知障碍表明,猕猴可能不会出现完全成熟的注意力缺失症。在组织病理学类型方面存在性别差异,只有CAA与灰质体积有显著关系。
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来源期刊
CiteScore
5.80
自引率
8.00%
发文量
158
审稿时长
3-6 weeks
期刊介绍: Established in 1891, JCN is the oldest continually published basic neuroscience journal. Historically, as the name suggests, the journal focused on a comparison among species to uncover the intricacies of how the brain functions. In modern times, this research is called systems neuroscience where animal models are used to mimic core cognitive processes with the ultimate goal of understanding neural circuits and connections that give rise to behavioral patterns and different neural states. Research published in JCN covers all species from invertebrates to humans, and the reports inform the readers about the function and organization of nervous systems in species with an emphasis on the way that species adaptations inform about the function or organization of the nervous systems, rather than on their evolution per se. JCN publishes primary research articles and critical commentaries and review-type articles offering expert insight in to cutting edge research in the field of systems neuroscience; a complete list of contribution types is given in the Author Guidelines. For primary research contributions, only full-length investigative reports are desired; the journal does not accept short communications.
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