L-type calcium channels in Alzheimer’s disease pathophysiology

Abstract The calcium hypothesis of Alzheimer’s disease (AD) links calcium dysregulation and the amyloidogenic pathway to cognitive dysfunction and tau pathology in AD. Calcium dysregulation occurs in many cell types during Alzheimer’s disease. One potential source of dysregulated calcium during AD is L-type calcium channels

(LTCCs). We have found that LTCC antagonists can reduce endo-lysosomal dysfunction around amyloid plaques during Alzheimer’s disease and can ameliorate microglia dysregulation during chronic neuroinflammation. There is significant crosstalk between these two pathways, suggesting that LTCC antagonists can target both microglia and neurons, mediating complementary and age-dependent

neuroprotection during AD pathology. Notably, the non-brain-penetrant LTCC antagonist amlodipine is associated with reduced risk for AD neuropathology and cognitive deficits, suggesting a role for brain-periphery crosstalk contributing to LTCC antagonist mediated neuroprotection during AD pathology. The overall goal of

our proposed research is to determine how LTCC antagonists may mediate their neuroprotective effects in the context of amyloid pathology. In Aim 1, we will evaluate the contribution of neuronal Cav1.2 and Cav1.3 LTCCs to endo-lysosomal dysfunction during amyloid pathology using conditional neuron-specific knockout mice. In Aim

2, we will evaluate the contributions of microglial Cav1.2 and Cav1.3 LTCCs to endo-lysosomal dysfunction during amyloid pathology using microglia-specific conditional knockout mice. In Aim 3, we will evaluate the peripheral contribution of LTCC antagonists to neuroprotection during AD pathology using brain-penetrant and

non-brain-penetrant LTCC antagonists. Overall, these studies will enhance our current understanding of LTCCs as mediators of calcium dysregulation during AD pathology and the beneficial role of LTCC antagonists on different neural cells and peripheral contributions. In turn, understanding which LTCC subunits to target and how

to best target lays the groundwork for future clinical trials repurposing LTCC antagonists for AD and other neurodegenerative disorders.