The Transient Receptor Potential Melastatin 2 (TRPM2) Channel Contributes to β-Amyloid
      Oligomer-Related Neurotoxicity and Memory Impairment

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Abstract

In Alzheimer's disease, accumulation of soluble oligomers of β-amyloid peptide is known to be highly toxic, causing disturbances in synaptic activity and neuronal death. Multiple studies relate these effects to increased oxidative stress and aberrant activity of calcium-permeable cation channels leading to calcium imbalance. The transient receptor potential melastatin 2 (TRPM2) channel, a Ca ²⁺-permeable nonselective cation channel activated by oxidative stress, has been implicated in neurodegenerative diseases, and more recently in amyloid-induced toxicity. Here we show that the function of TRPM2 is augmented by treatment of cultured neurons with β-amyloid oligomers. Aged APP/PS1 Alzheimer's mouse model showed increased levels of endoplasmic reticulum stress markers, protein disulfide isomerase and phosphorylated eukaryotic initiation factor 2α, as well as decreased levels of the presynaptic marker synaptophysin. Elimination of TRPM2 in APP/PS1 mice corrected these abnormal responses without affecting plaque burden. These effects of TRPM2 seem to be selective for β-amyloid toxicity, as ER stress responses to thapsigargin or tunicamycin in TRPM2 ^−/− neurons was identical to that of wild-type neurons. Moreover, reduced microglial activation was observed in TRPM2 ^−/−/APP/PS1 hippocampus compared with APP/PS1 mice. In addition, age-dependent spatial memory deficits in APP/PS1 mice were reversed in TRPM2 ^−/−/APP/PS1 mice. These results reveal the importance of TRPM2 for β-amyloid neuronal toxicity, suggesting that TRPM2 activity could be potentially targeted to improve outcomes in Alzheimer's disease.

SIGNIFICANCE STATEMENT Transient receptor potential melastatin 2 (TRPM2) is an oxidative stress sensing calcium-permeable channel that is thought to contribute to calcium dysregulation associated with neurodegenerative diseases, including Alzheimer's disease. Here we show that oligomeric β-amyloid, the toxic peptide in Alzheimer's disease, facilitates TRPM2 channel activation. In mice designed to model Alzheimer's disease, genetic elimination of TRPM2 normalized deficits in synaptic markers in aged mice. Moreover, the absence of TRPM2 improved age-dependent spatial memory deficits observed in Alzheimer's mice. Our results reveal the importance of TRPM2 for neuronal toxicity and memory impairments in an Alzheimer's mouse model and suggest that TRPM2 could be targeted for the development of therapeutic agents effective in the treatment of dementia.

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Author and article information

Journal

Journal ID (nlm-ta): J Neurosci

Journal ID (iso-abbrev): J. Neurosci

Journal ID (hwp): jneuro

Journal ID (pmc): jneurosci

Journal ID (publisher-id): J. Neurosci

Title: The Journal of Neuroscience

Publisher: Society for Neuroscience

ISSN (Print): 0270-6474

ISSN (Electronic): 1529-2401

Publication date (Print): 11 November 2015

Volume: 35

Issue: 45

Pages: 15157-15169

Affiliations

[1] ¹Molecular Medicine, Robarts Research Institute,

[2] ²Department of Physiology and Pharmacology, Schulich School of Medicine, and

[3] ³Department of Anatomy and Cell Biology, Schulich School of Medicine, University of Western Ontario, London, Ontario N6A 5B7, Canada,

[4] ⁴Department of Pharmacology and Therapeutics, College of Medicine, University of Manitoba, Winnipeg, Manitoba R3E 0T6, Canada,

[5] ⁵Neuroscience Research Group, Kleysen Institute for Advanced Medicine, University of Manitoba, Winnipeg, Manitoba R3E 3J7, Canada, and

[6] ⁶Laboratory of Molecular Biology, Department of Synthetic Chemistry and Biological Chemistry, Graduate School of Engineering, Kyoto University, Kyoto 615-8510, Japan

Author notes

Correspondence should be addressed to Dr. Marco A.M. Prado, Robarts Research Institute, University of Western Ontario, 1151 Richmond Street N, London, ON N6A 5B7, Canada, mprado@ 123456robarts.ca ; Dr. Vania F. Prado, Robarts Research Institute, University of Western Ontario, 1151 Richmond Street N, London, ON N6A 5B7, Canada, vprado@ 123456robarts.ca ; or Dr. Michael F. Jackson, Neuroscience Research Program SR426, University of Manitoba, 710 William Avenue, Winnipeg, MB R3E 0Z3, Canada, michael.jackson@ 123456umanitoba.ca

Author contributions: V.G.O., M.S.G., F.H.B., J.F.M., V.F.P., M.A.M.P., and M.F.J. designed research; V.G.O., M.C., M.S.G., Y.-F.X., N.L., J.F., F.H.B., A.C.M., and J.C.B. performed research; Y.M. contributed unpublished reagents/analytic tools; V.G.O., M.C., M.S.G., Y.-F.X., N.L., J.F., F.H.B., A.C.M., J.C.B., J.F.M., V.F.P., M.A.M.P., and M.F.J. analyzed data; V.G.O., F.H.B., V.F.P., M.A.M.P., and M.F.J. wrote the paper.

*V.G.O. and M.C. contributed equally to this work.

†Deceased, April 22, 2014.

M. F. Jackson's present address: Kleysen Institute for Advanced Medicine, University of Manitoba, Winnipeg, MB R3E 3J7, Canada.