Effects of Steroidal Na/K‐ATPase Inhibitor Marinobufagenin on Neurodegeneration, Neuroinflammation and Cognition in a Mouse Model of Alzheimer's Disease and Cardiovascular Amyloidosis

Background Na/K‐ATPase is a keystone enzyme in all living cells. Steroidal inhibitor of Na/K‐ATPase, marinobufagenin (MBG), participates in regulating cardiac function, vessel architecture, intracellular signaling transduction, and anti‐neuroinflammatory response. The aged double‐transgene APPswe/PS...

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Published in:The FASEB journal 2021-05, Vol.35 (S1), p.n/a, Article fasebj.2021.35.S1.05096
Main Authors: Zahariadis, Eleni, Juhasz, Ondrej, Wei, Wen, McDevitt, Ross, Zernetkina, Valentina, Grigorova, Yulia, Shearon, Jennifer, Cezayirli, Defne, Fenner, Rachel, Zheng, Lucy, Camandola, Simonetta, Mattson, Mark, Rapp, Peter, Lakatta, Edward, Fedorova, Olga
Format: Article
Language:English
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Summary:Background Na/K‐ATPase is a keystone enzyme in all living cells. Steroidal inhibitor of Na/K‐ATPase, marinobufagenin (MBG), participates in regulating cardiac function, vessel architecture, intracellular signaling transduction, and anti‐neuroinflammatory response. The aged double‐transgene APPswe/PS1dE9 mice, a model of Alzheimer's disease (AD), exhibit lower levels of urine MBG compared to wild‐type (WT) mice, impairments in cognitive function and amyloid β (Aβ) pathologies. Compromised blood supply to the brain may contribute to AD development and Aβ pathologies. Here we examined Aβ pathology in the cerebral and central vasculature of aged AD mice and whether MBG treatment affects neuroinflammation, neurodegeneration, and cognitive function. Methods To aged male AD (n=8; 15‐mo old) and age‐matched WT mice (n=4) MBG (100 µg/day/kg body weight) was administered via subcutaneous ALZET minipumps for 3‐mo. Age‐matched control mice received saline (AD‐C, n=8; WT‐C, n=4). Systolic blood pressure (SBP; by tail cuff plethysmography), cognitive flexibility (reversal learning in a water T‐maze), plasma (for MBG measurement), brain and tissue samples (for qPCR, 3D green light laser microscopy and immunohistochemistry analysis) were collected at 18‐mo. Data was analyzed by 2‐way ANOVA and presented as mean±SE. Results In aged AD mice, we observed granulated Aβ plaques and Aβ localization around small cerebral blood vessels (Fig 1B; white arrows). Aβ protein was also found in significantly larger abundance in aortae vessel wall of old AD mice vs. WT mice (Fig 2; blue stain). SBP was not affected by treatment and did not differ between AD and WT mice. Endogenous plasma MBG was lower in AD‐C vs. WT‐C (125±21 vs. 223±41 pmol/L; p
ISSN:0892-6638
1530-6860
DOI:10.1096/fasebj.2021.35.S1.05096