Deletion of the Homocysteine Thiolactone Detoxifying Enzyme Bleomycin Hydrolase, in Mice, Causes Memory and Neurological Deficits and Worsens Alzheimer's Disease-Related Behavioral and Biochemical Traits in the 5xFAD Model of Alzheimer's Disease

Łukasz Witucki; Kamila Borowczyk; Joanna Suszyńska-Zajczyk; Ewelina Warzych; Piotr Pawlak; Hieronim Jakubowski

doi:10.3233/JAD-230578

Deletion of the Homocysteine Thiolactone Detoxifying Enzyme Bleomycin Hydrolase, in Mice, Causes Memory and Neurological Deficits and Worsens Alzheimer's Disease-Related Behavioral and Biochemical Traits in the 5xFAD Model of Alzheimer's Disease

J Alzheimers Dis. 2023;95(4):1735-1755. doi: 10.3233/JAD-230578.

Authors

Łukasz Witucki^{1

2}, Kamila Borowczyk², Joanna Suszyńska-Zajczyk¹, Ewelina Warzych³, Piotr Pawlak³, Hieronim Jakubowski^{1

2}

Affiliations

¹ Department of Biochemistry and Biotechnology, Poznań University of Life Sciences, Poznań, Poland.
² Department of Microbiology, Biochemistry and Molecular Genetics, Rutgers University, New Jersey Medical School, International Center for Public Health, Newark, NJ, USA.
³ Department of Genetics and Animal Breeding, Poznań University of Life Sciences, Poznań, Poland.

Abstract

Background: Bleomycin hydrolase (BLMH), a homocysteine (Hcy)-thiolactone detoxifying enzyme, is attenuated in Alzheimer's disease (AD) brains. Blmh loss causes astrogliosis in mice while the loss of histone demethylase Phf8, which controls mTOR signaling, causes neuropathy in mice and humans.

Objective: To examine how Blmh gene deletion affects the Phf8/H4K20me1/mTOR/autophagy pathway, amyloid-β (Aβ) accumulation, and cognitive/neuromotor performance in mice.

Methods: We generated a new mouse model of AD, the Blmh-/-5xFAD mouse. Behavioral assessments were conducted by cognitive/neuromotor testing. Blmh and Phf8 genes were silenced in mouse neuroblastoma N2a-APPswe cells by RNA interference. mTOR- and autophagy-related proteins, and AβPP were quantified by western blotting and the corresponding mRNAs by RT-qPCR. Aβ was quantified by western blotting (brains) and by confocal microscopy (cells).

Results: Behavioral testing showed cognitive/neuromotor deficits in Blmh-/- and Blmh-/-5xFAD mice. Phf8 was transcriptionally downregulated in Blmh-/- and Blmh-/-5xFAD brains. H4K20me1, mTOR, phospho-mTOR, and AβPP were upregulated while autophagy markers Becn1, Atg5, and Atg7 were downregulated in Blmh-/- and Blmh-/-5xFAD brains. Aβ was elevated in Blmh-/-5xFAD brains. These biochemical changes were recapitulated in Blmh-silenced N2a-APPswe cells, which also showed increased H4K20me1-mTOR promoter binding and impaired autophagy flux (Lc3-I, Lc3-II, p62). Phf8-silencing or treatments with Hcy-thiolactone or N-Hcy-protein, metabolites elevated in Blmh-/- mice, induced biochemical changes in N2a-APPswe cells like those induced by the Blmh-silencing. However, Phf8-silencing elevated Aβ without affecting AβPP.

Conclusions: Our findings show that Blmh interacts with AβPP and the Phf8/H4K20me1/mTOR/autophagy pathway, and that disruption of those interactions causes Aβ accumulation and cognitive/neuromotor deficits.

Keywords: Alzheimer’s disease; Blmh-/-5xFAD mouse; H4K20me1; N2a-APPswe mouse neuroblastoma cells; Phf8; amyloid-β protein precursor; autophagy; bleomycin hydrolase; homocysteine thiolactone; mTOR.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Alzheimer Disease* / genetics
Alzheimer Disease* / metabolism
Amyloid beta-Peptides / metabolism
Amyloid beta-Protein Precursor / genetics
Animals
Aspartic Acid Endopeptidases / metabolism
Disease Models, Animal
Humans
Mice
Mice, Transgenic
TOR Serine-Threonine Kinases

Substances

bleomycin hydrolase
homocysteine thiolactone
Aspartic Acid Endopeptidases
Amyloid beta-Peptides
TOR Serine-Threonine Kinases
Amyloid beta-Protein Precursor