Steady-state neuron-predominant LINE-1 encoded ORF1p protein and LINE-1 RNA increase with aging in the mouse and human brain

Author:

Bonnifet Tom1,Sinnassamy Sandra1,Massiani-Beaudoin Olivia1,Mailly Philippe2,Monnet Héloïse2,Loew Damarys3,Lombard Berangère3,Servant Nicolas4,Joshi Rajiv L1,Fuchs Julia1

Affiliation:

1. CIRB, Collège de France, Université PSL, INSERM, CNRS

2. Orion Technological Core, CIRB, Collège de France, Université PSL, INSERM, CNRS

3. Institut Curie, Université PSL, Centre de Recherche, CurieCoreTech Spectrométrie de Masse Protéomique

4. Institut Curie, INSERM U900, Mines Paris Tech, Université PSL

Abstract

Recent studies have established a reciprocal causal link between aging and the activation of transposable elements, characterized in particular by a de-repression of LINE-1 retrotransposons. These LINE-1 elements represent 21% of the human genome, but only a minority of these sequences retain the coding potential essential for their mobility. LINE-1 encoded proteins can induce cell toxicity implicated in aging and neurodegenerative diseases. However, our knowledge of the expression and localization of LINE-1-encoded proteins in the central nervous system is limited. Using a novel approach combining atlas-based brain mapping with deep-learning algorithms on large-scale pyramidal brain images, we unveil a heterogeneous, neuron-predominant and widespread ORF1p expression throughout the murine brain at steady-state. In aged mice, ORF1p expression increases significantly which is corroborated in human post-mortem dopaminergic neurons by an increase in young LINE-1 elements including those with open reading frames. Mass spectrometry analysis of endogenous mouse ORF1p revealed novel, neuron-specific protein interactors. These findings contribute to a comprehensive description of the dynamics of LINE-1 and ORF1p expression in the brain at steady-state and in aging and provide insights on ORF1p protein interactions in the brain.

Publisher

eLife Sciences Publications, Ltd

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