Abstract
The protection mediated by the bioactive sphingolipid sphingosine-1-phosphate (S1P) declines during Alzheimer's disease (AD) progression, especially in patients carrying the apolipoprotein E ε4 (APOE4) isoform. The drug FTY720 mimics S1P bioactivity, but its efficacy in treating AD is unclear. Two doses of FTY720 (0.1 mg / kg and 0.5 mg / kg daily) were given by oral gavage for 15 weeks to transgenic mouse models of familial AD carrying human apolipoprotein E (APOE) APOE3 (E3FAD) or APOE4 (E4FAD). After 12 weeks of treatment, animals were subjected to behavioral tests for memory, locomotion, and anxiety. Blood was withdrawn at different time points and brains were collected for sphingolipids analysis by mass spectrometry, gene expression by RT-PCR and Aβ quantification by ELISA. We discovered that low levels of S1P in the plasma is associated with a higher probability of failing the memory test and that FTY720 prevents memory impairments in E4FAD. The beneficial effect of FTY720 was induced by a shift of the sphingolipid metabolism in the brain towards a lower production of toxic metabolites, like ceramide d18:1/16:0 and d18:1/22:0, and reduction of amyloid-β burden and inflammation. In conclusion, we provide further evidence of the druggability of the sphingolipid system in AD.
Original language | English |
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Article number | 113240 |
Journal | Biomedicine and Pharmacotherapy |
Volume | 152 |
DOIs | |
State | Published - Aug 2022 |
Bibliographical note
Publisher Copyright:© 2022
Funding
This work was supported by grants to MTM, JW, AR, PMM, and HEV from the ZonMw Memorabel Program (project nr: 733050105 ), the Alzheimer Nederland (projectnr: 14545 , The Netherlands) to PMM, the Interreg VA EMR program (EURLIPIDS, EMR23 , The Netherlands) to EW and PM. Aspects of this work were supported by grants to QL (the China Scholarship Council 201706220095 , China), EB ( National Institutes of Health : R01AG034389 , R01NS095215 , R01AG064234 ; U.S. Department of Veterans Affairs : I01BX003643 , USA) and to SMC ( BrightFocus Grant Submission Number: A20201464F ; National Institute On Aging of the National Institutes of Health under Award Number P30AG028383 , USA). Acknowledgment is made to the donors of ADR, a program of BrightFocus Foundation . We acknowledge Christian Beerli for analyzing FTY720/-P levels and to Novartis Pharma AG for supplying the FTY720. This work was supported by grants to MTM, JW, AR, PMM, and HEV from the ZonMw Memorabel Program (project nr: 733050105), the Alzheimer Nederland (projectnr: 14545, The Netherlands) to PMM, the Interreg VA EMR program (EURLIPIDS, EMR23, The Netherlands) to EW and PM. Aspects of this work were supported by grants to QL (the China Scholarship Council 201706220095, China), EB (National Institutes of Health: R01AG034389, R01NS095215, R01AG064234; U.S. Department of Veterans Affairs: I01BX003643, USA) and to SMC (BrightFocus Grant Submission Number: A20201464F; National Institute On Aging of the National Institutes of Health under Award Number P30AG028383, USA). Acknowledgment is made to the donors of ADR, a program of BrightFocus Foundation. We acknowledge Christian Beerli for analyzing FTY720/-P levels and to Novartis Pharma AG for supplying the FTY720.
Funders | Funder number |
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Interreg | EMR23 |
ZonMw Memorabel program | 733050105 |
National Institutes of Health (NIH) | R01NS095215, R01AG034389, R01AG064234 |
National Institutes of Health (NIH) | |
U.S. Department of Veterans Affairs | P30AG028383, A20201464F, I01BX003643 |
U.S. Department of Veterans Affairs | |
BrightFocus Foundation | FTY720 |
BrightFocus Foundation | |
Netherlands Organisation for Health Research and Development/Alzheimer Nederland | 14545 |
Netherlands Organisation for Health Research and Development/Alzheimer Nederland |
Keywords
- 5xFAD
- APOE3
- APOE4
- Anxiety
- Ceramide
- FTY720
- Memory
- S1P
- Sphingomyelin
ASJC Scopus subject areas
- Pharmacology