Retrotransposons as a Source of DNA Damage in Neurodegeneration

Peze‐Heidsieck, Eugenie; Bonnifet, Tom; Znaidi, Rania; Ravel-Godreuil, Camille; Massiani‐Beaudoin, Olivia; Joshi, Rajiv L.; Fuchs, Julia

doi:10.3389/fnagi.2021.786897

Cited by 24 publications

(22 citation statements)

References 229 publications

(302 reference statements)

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“…To date, multiple authors have provided evidence that TE activity may be involved in pathogenesis of Alzheimer’s disease, autism, schizophrenia, Rett syndrome, ataxia-telangiectasia, amyotrophic lateral sclerosis, macular degeneration and some other neuropathologies [ 39 , 56 , 112 , 113 , 350 , 466 ]. Physiological conditions such as stress and aging are not formally considered disorders, but since they are associated with some detrimental effects as well as with TE derepression [ 384 , 467 , 468 , 469 ], we discuss these conditions as well.…”

Section: The Role Of Neuronal Tes In Pathologymentioning

confidence: 99%

“…Aging is a result of gradual accumulation of damage in cells and tissues [ 469 ]. A phylogenetically conserved feature of aging is induction of stress response pathways that was confirmed in all systems studied, including whole organism analysis of invertebrates and analysis of the brain of different mammalian species [ 480 ].…”

Section: The Role Of Neuronal Tes In Pathologymentioning

confidence: 99%

“…Moreover, even normal aging in healthy people includes decrements in learning and memory, attention, decision-making speed, sensory perception and motor coordination, and even reduction in brain size [ 476 ]. Many pathological features of neurodegeneration are aggravated hallmarks of normal brain aging (including genomic instability and epigenetic alterations), suggesting that neurodegeneration may be actually seen as accelerated aging [ 468 , 469 ]. One of the most important mechanisms in neuronal aging and age-associated cognitive impairment is oxidative damage [ 482 ].…”

Section: The Role Of Neuronal Tes In Pathologymentioning

confidence: 99%

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The Role of Transposable Elements of the Human Genome in Neuronal Function and Pathology

Чеснокова

Beletskiy

Kolosov

2022

IJMS

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Transposable elements (TEs) have been extensively studied for decades. In recent years, the introduction of whole-genome and whole-transcriptome approaches, as well as single-cell resolution techniques, provided a breakthrough that uncovered TE involvement in host gene expression regulation underlying multiple normal and pathological processes. Of particular interest is increased TE activity in neuronal tissue, and specifically in the hippocampus, that was repeatedly demonstrated in multiple experiments. On the other hand, numerous neuropathologies are associated with TE dysregulation. Here, we provide a comprehensive review of literature about the role of TEs in neurons published over the last three decades. The first chapter of the present review describes known mechanisms of TE interaction with host genomes in general, with the focus on mammalian and human TEs; the second chapter provides examples of TE exaptation in normal neuronal tissue, including TE involvement in neuronal differentiation and plasticity; and the last chapter lists TE-related neuropathologies. We sought to provide specific molecular mechanisms of TE involvement in neuron-specific processes whenever possible; however, in many cases, only phenomenological reports were available. This underscores the importance of further studies in this area.

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Section: The Role Of Neuronal Tes In Pathologymentioning

confidence: 99%

Section: The Role Of Neuronal Tes In Pathologymentioning

confidence: 99%

Section: The Role Of Neuronal Tes In Pathologymentioning

confidence: 99%

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The Role of Transposable Elements of the Human Genome in Neuronal Function and Pathology

Чеснокова

Beletskiy

Kolosov

2022

IJMS

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“…For example, endogenous retroelements are getting considerable attention as a potential class of alternative tumor-specific antigens ( Smith et al., 2019 ). Interestingly, dysregulated increase of endogenous retroelements has also been associated with NDs ( Peze-Heidsieck et al., 2021 ; Ravel-Godreuil et al., 2021 ): high levels of expression and reactivation of retrotransposable element, LINE-1 (Long interspersed nuclear element 1, L1), in postmortem brain samples of ALS and FTD ALS in TDP-43 (TAR DNA-binding protein of 43 kDa)-dependent manner ( Liu et al., 2019 ; Tam et al., 2019 ). Thus, aberrant expression of endogenous retroelement under chronic inflammation could provide the currently unknown antigen(s) that may prime Th cell in the CNS.…”

Section: Introductionmentioning

confidence: 99%

“…Meanwhile, dysregulated L1 insertion potentially compromises developing and mature neurons and so may cause neurodevelopmental diseases and neurodegenerative diseases ( Nicole et al., 2017 ). Interestingly, L1 activation has been frequently highlighted as a comorbidity in NDs ( Peze-Heidsieck et al., 2021 ; Ravel-Godreuil et al., 2021 ). However, comprehensive analysis of the mode of L1 activation and its relevance to neuronal cell death remains to be investigated.…”

Section: Introductionmentioning

confidence: 99%

Immune-mediated neurodegenerative trait provoked by multimodal derepression of long-interspersed nuclear element-1

et al. 2022

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From the genome's perspective: Bearing somatic retrotransposition to leverage the regulatory potential of L1 RNAs

Mangoni,

Mazzetti,

Ansaloni

et al. 2024

BioEssays

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Transposable elements (TEs) are mobile genomic elements constituting a big fraction of eukaryotic genomes. They ignite an evolutionary arms race with host genomes, which in turn evolve strategies to restrict their activity. Despite being tightly repressed, TEs display precisely regulated expression patterns during specific stages of mammalian development, suggesting potential benefits for the host. Among TEs, the long interspersed nuclear element (LINE‐1 or L1) has been found to be active in neurons. This activity prompted extensive research into its possible role in cognition. So far, no specific cause‐effect relationship between L1 retrotransposition and brain functions has been conclusively identified. Nevertheless, accumulating evidence suggests that interactions between L1 RNAs and RNA/DNA binding proteins encode specific messages that cells utilize to activate or repress entire transcriptional programs. We summarize recent findings highlighting the activity of L1 RNAs at the non‐coding level during early embryonic and brain development. We propose a hypothesis suggesting a mutualistic relationship between L1 mRNAs and the host cell. In this scenario, cells tolerate a certain rate of retrotransposition to leverage the regulatory effects of L1s as non‐coding RNAs on potentiating their mitotic potential. In turn, L1s benefit from the cell's proliferative state to increase their chance to mobilize.

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Retrotransposons as a Source of DNA Damage in Neurodegeneration

Cited by 24 publications

References 229 publications

The Role of Transposable Elements of the Human Genome in Neuronal Function and Pathology

The Role of Transposable Elements of the Human Genome in Neuronal Function and Pathology

Immune-mediated neurodegenerative trait provoked by multimodal derepression of long-interspersed nuclear element-1

From the genome's perspective: Bearing somatic retrotransposition to leverage the regulatory potential of L1 RNAs

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