Gain of PITRM1 peptidase in cortical neurons affords protection of mitochondrial and synaptic function in an advanced age mouse model of Alzheimer's disease

Fang Du; Qing Yu; Shijun Yan; Zhihua Zhang; Jhansi Rani Vangavaragu; Doris Chen; Shi Fang Yan; Shirley ShiDu Yan

doi:10.1111/acel.13368

Gain of PITRM1 peptidase in cortical neurons affords protection of mitochondrial and synaptic function in an advanced age mouse model of Alzheimer's disease

Aging Cell. 2021 May;20(5):e13368. doi: 10.1111/acel.13368. Epub 2021 May 5.

Authors

Fang Du¹, Qing Yu¹, Shijun Yan², Zhihua Zhang², Jhansi Rani Vangavaragu², Doris Chen², Shi Fang Yan¹, Shirley ShiDu Yan^{1

3}

Affiliations

¹ Department of Surgery, Columbia University, New York, NY, USA.
² Department of Pharmacology and Toxicology and Higuchi bioscience Center, University of Kansas, Lawrence, KS, USA.
³ Department of Molecular Pharmacology & Therapeutics, Columbia University, New York, NY, USA.

Abstract

Mitochondrial dysfunction is one of the early pathological features of Alzheimer's disease (AD). Accumulation of cerebral and mitochondrial Aβ links to mitochondrial and synaptic toxicity. We have previously demonstrated the mechanism by which presequence peptidase (PITRM1)-mediated clearance of mitochondrial Aβ contributes to mitochondrial and cerebral amyloid pathology and mitochondrial and synaptic stress in adult transgenic AD mice overexpressing Aβ up to 12 months old. Here, we investigate the effect of PITRM1 in an advanced age AD mouse model (up to 19-24 months) to address the fundamental unexplored question of whether restoration/gain of PITRM1 function protects against mitochondrial and synaptic dysfunction associated with Aβ accumulation and whether this protection is maintained even at later ages featuring profound amyloid pathology and synaptic failure. Using newly developed aged PITRM1/Aβ-producing AD mice, we first uncovered reduction in PITRM1 expression in AD-affected cortex of AD mice at 19-24 months of age. Increasing neuronal PITRM1 activity/expression re-established mitochondrial respiration, suppressed reactive oxygen species, improved synaptic function, and reduced loss of synapses even at advanced ages (up to 19-24 months). Notably, loss of PITRM1 proteolytic activity resulted in Aβ accumulation and failure to rescue mitochondrial and synaptic function, suggesting that PITRM1 activity is required for the degradation and clearance of mitochondrial Aβ and Aβ deposition. These data indicate that augmenting PITRM1 function results in persistent life-long protection against Aβ toxicity in an AD mouse model. Therefore, augmenting PITRM1 function may enhance Aβ clearance in mitochondria, thereby maintaining mitochondrial integrity and ultimately slowing the progression of AD.

Keywords: amyloid pathology; mitochondria-related proinflammation; mitochondrial Aβ clearance; mitochondrial proteolysis; synaptic rescue.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Aging
Alzheimer Disease / enzymology*
Alzheimer Disease / metabolism
Amyloid beta-Peptides / metabolism
Amyloid beta-Protein Precursor / genetics
Animals
Brain / metabolism
Cognition
Disease Models, Animal
Female
Inflammation
Male
Metalloendopeptidases / genetics
Metalloendopeptidases / metabolism*
Mice, Transgenic
Mitochondria / enzymology*
Mitochondria / metabolism
Neurons / enzymology*
Neurons / metabolism
Synapses / metabolism*
Synapses / physiology

Substances

Amyloid beta-Peptides
Amyloid beta-Protein Precursor
Metalloendopeptidases
PITRM1 protein, human

Abstract

Publication types

MeSH terms

Substances

Grants and funding