Litcius/Paper detail

Chronic BMAA exposure combined with TDP-43 mutation elicits motor neuron dysfunction phenotypes in mice

Frederick J. Arnold, M. Burns, Yu‐Chun Chiu, Joana Carvalho, Ashlie Nguyen, P.C. Ralph, Albert R. La Spada, Craig L. Bennett

2023Neurobiology of Aging12 citationsDOIOpen Access PDF

Abstract

Amyotrophic lateral sclerosis (ALS) is a neurodegenerative disease with an average age-of-onset of ∼60 years and is usually fatal within 2-5 years of diagnosis. Mouse models based upon single gene mutations do not recapitulate all ALS pathological features. Environmental insults may also contribute to ALS, and β-N-methylamino-L-alanine (BMAA) is an environmental toxin linked with an increased risk of developing ALS. BMAA, along with cycasin, are hypothesized to be the cause of the Guam-ALS epicenter of the 1950s. We developed a multihit model based on low expression of a dominant familial ALS TDP-43 mutation (Q331K) and chronic low-dose BMAA exposure. Our two-hit mouse model displayed a motor phenotype absent from either lesion alone. By LC/MS analysis, free BMAA was confirmed at trace levels in brain, and were as high as 405 ng/mL (free) and 208 ng/mL (protein-bound) in liver. Elevated BMAA levels in liver were associated with dysregulation of the unfolded protein response (UPR) pathway. Our data represent initial steps towards an ALS mouse model resulting from combined genetic and environmental insult.

Topics & Concepts

Amyotrophic lateral sclerosisPhenotypeNeurodegenerationMutationBiologyDiseaseUnfolded protein responseGeneMedicineNeuroscienceGeneticsPathologyAmyotrophic Lateral Sclerosis ResearchFibromyalgia and Chronic Fatigue Syndrome ResearchCholinesterase and Neurodegenerative Diseases