Inhibiting tau-induced elevated nSMase2 activity and ceramides is therapeutic in murine Alzheimer's disease

Carolyn Tallon; Benjamin J Bell; Medhinee M Malvankar; Pragney Deme; Carlos Nogueras-Ortiz; Erden Eren; Ajit G Thomas; Kristen R Hollinger; Arindom Pal; Maja Mustapic; Meixiang Huang; Kaleem Coleman; Tawnjerae R Joe; Rana Rais; Norman J Haughey; Dimitrios Kapogiannis; Barbara S Slusher

doi:10.21203/rs.3.rs-3131295/v1

Inhibiting tau-induced elevated nSMase2 activity and ceramides is therapeutic in murine Alzheimer's disease

Res Sq [Preprint]. 2023 Jul 18:rs.3.rs-3131295. doi: 10.21203/rs.3.rs-3131295/v1.

Authors

Carolyn Tallon¹, Benjamin J Bell¹, Medhinee M Malvankar¹, Pragney Deme¹, Carlos Nogueras-Ortiz², Erden Eren², Ajit G Thomas¹, Kristen R Hollinger¹, Arindom Pal¹, Maja Mustapic², Meixiang Huang¹, Kaleem Coleman¹, Tawnjerae R Joe¹, Rana Rais¹, Norman J Haughey¹, Dimitrios Kapogiannis², Barbara S Slusher¹

Affiliations

¹ Johns Hopkins University.
² National Institute on Aging Laboratory of Clinical Investigation.

Abstract

Background: Cognitive decline in Alzheimer's disease (AD) is associated with prion-like tau propagation between neurons along synaptically connected networks, in part via extracellular vesicles (EV). EV biogenesis is triggered by ceramide enrichment at the plasma membrane from neutral sphingomyelinase2(nSMase2)-mediated cleavage of sphingomyelin. We report, for the first time, that tau expression triggers an elevation in brain ceramides and nSMase2 activity.

Methods: To determine the therapeutic benefit of inhibiting this elevation, we evaluated the efficacy of PDDC, the first potent, selective, orally bioavailable, and brain-penetrable nSMase2 inhibitor, in the PS19 tau transgenic AD murine model. Changes in brain ceramide and sphingomyelin levels, Tau content, histopathology, and nSMase2 target engagement were monitored, as well as changes in the number of brain-derived EVs in plasma and their Tau content. Additionally, we evaluated the ability of PDDC to impede tau propagation in a murine model where an adeno-associated virus(AAV) encoding for P301L/S320F double mutant human tau was stereotaxically-injected unilaterally into the hippocampus and the contralateral transfer to the dentate gyrus was monitored.

Results: Similar to human AD, PS19 mice exhibited increased brain ceramides and nSMase2 activity; both were completely normalized by PDDC treatment. PS19 mice exhibited elevated tau immunostaining, thinning of hippocampal neuronal cell layers, increased mossy fiber synaptophysin immunostaining, and glial activation, all pathologic features of human AD. PDDC treatment significantly attenuated these aberrant changes. Mouse plasma isolated from PDDC-treated PS19 mice exhibited reduced levels of neuron- and microglia-derived EVs, the former carrying lower phosphorylated Tau(pTau) levels, compared to untreated mice. In the AAV tau propagation model, PDDC normalized the tau-induced increase in brain ceramides and significantly decreased tau spreading to the contralateral side.

Conclusions: PDDC is a first-in-class therapeutic candidate that normalizes elevated brain ceramides and nSMase2 activity leading to the slowing of tau spread in AD mice.

Keywords: Alzheimer’s disease; ceramide; extracellular vesicles; neutral sphingomyelinase 2; tau.

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Preprint

Abstract

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