Differential effect of an evolving amyloid and tau pathology on brain phospholipids and bioactive lipid mediators in rat models of Alzheimer-like pathology

Authors

Sonia Do Carmo, McGill Faculty of Medicine and Health Sciences
Marie Audrey I. Kautzmann, LSU Health Sciences Center - New OrleansFollow
Surjyadipta Bhattacharjee, LSU Health Sciences Center - New OrleansFollow
Bokkyoo Jun, LSU Health Sciences Center - New Orleans
Carolyn Steinberg, McGill Faculty of Medicine and Health Sciences
Joshua T. Emmerson, McGill Faculty of Medicine and Health Sciences
Janice C. Malcolm, Université McGill
Quentin Bonomo, Université McGill
Nicolas G. Bazan, LSU Health Sciences Center - New OrleansFollow
A. Claudio Cuello, McGill Faculty of Medicine and Health Sciences

Document Type

Article

Publication Date

7-30-2024

Publication Title

Journal of Neuroinflammation

Abstract

Background: Brain inflammation contributes significantly to the pathophysiology of Alzheimer’s disease, and it is manifested by glial cell activation, increased production of cytokines/chemokines, and a shift in lipid mediators from a pro-homeostatic to a pro-inflammatory profile. However, whether the production of bioactive lipid mediators is affected at earlier stages, prior to the deposition of Aβ plaques and tau hyperphosphorylation, is unknown. The differential contribution of an evolving amyloid and tau pathology on the composition and abundance of membrane phospholipids and bioactive lipid mediators also remains unresolved. Methods: In this study, we examined the cortical levels of DHA- and AA-derived bioactive lipid mediators and of membrane phospholipids by liquid chromatography with tandem mass spectrometry in transgenic rat models of the Alzheimer’s-like amyloid and tau pathologies at early and advanced pathological stages. Results: Our findings revealed a complex balance between pro-inflammatory and pro-resolving processes in which tau pathology has a more pronounced effect compared to amyloid pathology. At stages preceding tau misfolding and aggregation, there was an increase in pro-resolving lipid mediators (RVD6 and NPD1), DHA-containing phospholipids and IFN-γ levels. However, in advanced tau pathology displaying NFT-like inclusions, neuronal death, glial activation and cognitive deficits, there was an increase in cytokine and PGD2, PGE2, and PGF2α generation accompanied by a drop in IFN-γ levels. This pathology also resulted in a marked increase in AA-containing phospholipids. In comparison, pre-plaque amyloid pathology already presented high levels of cytokines and AA-containing phospholipids together with elevated RVD6 and NPD1 levels. Finally, Aβ plaque deposition was accompanied by a modest increase in prostaglandins, increased AA-containing phospholipids and reduced DHA-containing phospholipids. Conclusions: Our findings suggest a dynamic trajectory of inflammatory and lipid mediators in the evolving amyloid and tau pathologies and support their differing roles on membrane properties and, consequentially, on signal transduction.

PubMed ID

39080670

Volume

21

Issue

1

Creative Commons License

This work is licensed under a Creative Commons Attribution-NonCommercial-No Derivative Works 4.0 International License.

Recommended Citation

Do Carmo, Sonia; Kautzmann, Marie Audrey I.; Bhattacharjee, Surjyadipta; Jun, Bokkyoo; Steinberg, Carolyn; Emmerson, Joshua T.; Malcolm, Janice C.; Bonomo, Quentin; Bazan, Nicolas G.; and Cuello, A. Claudio, "Differential effect of an evolving amyloid and tau pathology on brain phospholipids and bioactive lipid mediators in rat models of Alzheimer-like pathology" (2024). School of Graduate Studies Faculty Publications. 304.
https://digitalscholar.lsuhsc.edu/sogs_facpubs/304
10.1186/s12974-024-03184-7