Evaluation of [125I]α-Bungarotoxin Binding to α7 Nicotinic Acetylcholinergic Receptors in Hippocampus-Subiculum of Postmortem Human Alzheimer's Disease Brain.

Receptors (Basel, Switzerland) Pub Date : 2025-03-01 Epub Date: 2025-03-20 DOI:10.3390/receptors4010007
Allyson Ngo, Fariha Karim, Oshini V Keerthisinghe, Tram B Danh, Christopher Liang, Jogeshwar Mukherjee
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Abstract

Background/objectives: Alzheimer's disease (AD) severely hinders cognitive function in the hippocampus (HP) and subiculum (SUB), impacting the expression of nicotinic acetylcholine receptors (nAChRs) such as the α7-subtype. To investigate α7 nAChRs as a potential PET imaging biomarker, we report the quantitative binding of [125I]α-Bungarotoxin ([125I]α-Bgtx) for binding to postmortem human AD (n = 29; 13 males, 16 females) HP compared to cognitively normal (CN) (n = 28; 13 male, 15 female) HP.

Methods: For comparisons with common AD biomarkers, adjacent slices were anti-Aβ and anti-Tau immunostained for analysis using QuPath.

Results: The [125I]α-Bgtx average SUB/HP ratio was 0.5 among the CN subjects, suggesting higher [125I]α-Bgtx binding in the HP gray matter regions. The AD subjects showed overall less binding than the CN subjects, with no statistical significance. A positive correlation was found in the [125I]α-Bgtx binding in the AD subjects as the age increased. The Braak stage comparisons of [125I]α-Bgtx were made with [18F]flotaza binding to Aβ plaques and [125I]IPPI binding to Tau. A positive correlation was found between [125I]α-Bgtx and [18F]flotaza and there was a negative correlation between [125I]α-Bgtx and [125I]IPPI, implicating intricate relationships between the different AD biomarkers.

Conclusions: [125I]α-Bgtx shows complimentary potential as a α7 nAChR imaging agent but needs more preclinical assessments to confirm effectiveness for translational PET studies using α7 nAChR radioligands.

[125I]α-虫毒与阿尔茨海默病死后脑海马-下丘α7烟碱胆碱能受体结合的研究
背景/目的:阿尔茨海默病(AD)严重阻碍海马(HP)和下托(SUB)的认知功能,影响烟碱乙酰胆碱受体(nachr)的表达,如α7亚型。为了研究α7 nAChRs作为潜在的PET成像生物标志物,我们报道了[125I]α-Bungarotoxin ([125I]α-Bgtx)与死后AD的定量结合(n = 29;男性13例,女性16例)HP与认知正常(CN) (n = 28;13名男性,15名女性)HP。方法:与常见AD生物标志物进行比较,相邻切片进行抗a β和抗tau免疫染色,使用QuPath进行分析。结果:CN组[125I]α-Bgtx平均SUB/HP比值为0.5,表明[125I]α-Bgtx在HP灰质区结合较高。AD组与CN组的结合程度总体较低,差异无统计学意义。AD患者的[125I]α-Bgtx结合随着年龄的增长呈正相关。将[125I]α-Bgtx与[18F]flotaza结合Aβ斑块和[125I]IPPI结合Tau进行Braak期比较。[125I]α-Bgtx与[18F]flotaza呈正相关,[125I]α-Bgtx与[125I]IPPI呈负相关,提示不同AD生物标志物之间存在复杂的关系。结论:[125I]α-Bgtx作为α7 nAChR显像剂具有互补的潜力,但需要更多的临床前评估来确认α7 nAChR放射配体在翻译PET研究中的有效性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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