Mechanisms and consequences of aneuploidy and chromosome instability in the aging brain

Andriani, Grasiella; Vijg, Jan; Montagna, Cristina

doi:10.1016/j.mad.2016.03.007

Cited by 41 publications

(38 citation statements)

References 240 publications

(321 reference statements)

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“…However, compared with healthy subjects, patients with both familial/early‐onset and sporadic late‐onset AD show widespread aneuploidy in their brains and in peripheral blood cells (Bajic, Spremo‐Potparevic, Zivkovic, Isenovic, & Arendt, ; Hou, Song, Croteau, Akbari, & Bohr, ; Iourov et al, ; Lee, Thomas, & Fenech, ; Zivković et al, ). This AD‐associated aneuploidy is thought to be due to genomic instability (Andriani, Vijg, & Montagna, ; Shepherd, Yang, & Halliday, ). This observation suggests the existence of a cell population that has newly entered a flawed cell cycle in patients with AD.…”

Section: The “Amyloid‐beta Accumulation Cycle”mentioning

confidence: 99%

“Amyloid‐beta accumulation cycle” as a prevention and/or therapy target for Alzheimer's disease

et al. 2020

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The cell cycle and its regulators are validated targets for cancer drugs. Reagents that target cells in a specific cell cycle phase (e.g., antimitotics or DNA synthesis inhibitors/replication stress inducers) have demonstrated success as broad‐spectrum anticancer drugs. Cyclin‐dependent kinases (CDKs) are drivers of cell cycle transitions. A CDK inhibitor, flavopiridol/alvocidib, is an FDA‐approved drug for acute myeloid leukemia. Alzheimer's disease (AD) is another serious issue in contemporary medicine. The cause of AD remains elusive, although a critical role of latent amyloid‐beta accumulation has emerged. Existing AD drug research and development targets include amyloid, amyloid metabolism/catabolism, tau, inflammation, cholesterol, the cholinergic system, and other neurotransmitters. However, none have been validated as therapeutically effective targets. Recent reports from AD‐omics and preclinical animal models provided data supporting the long‐standing notion that cell cycle progression and/or mitosis may be a valid target for AD prevention and/or therapy. This review will summarize the recent developments in AD research: (a) Mitotic re‐entry, leading to the “amyloid‐beta accumulation cycle,” may be a prerequisite for amyloid‐beta accumulation and AD pathology development; (b) AD‐associated pathogens can cause cell cycle errors; (c) thirteen among 37 human AD genetic risk genes may be functionally involved in the cell cycle and/or mitosis; and (d) preclinical AD mouse models treated with CDK inhibitor showed improvements in cognitive/behavioral symptoms. If the “amyloid‐beta accumulation cycle is an AD drug target” concept is proven, repurposing of cancer drugs may emerge as a new, fast‐track approach for AD management in the clinic setting.

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Section: The “Amyloid‐beta Accumulation Cycle”mentioning

confidence: 99%

“Amyloid‐beta accumulation cycle” as a prevention and/or therapy target for Alzheimer's disease

et al. 2020

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“…Moreover, mutations in the gene encoding for Senataxin (SETX), a protein involved in resolving collisions between transcription and replication and, therefore, preventing R-loop formation, lead to various neurodegenerative diseases, such as amyotrophic lateral sclerosis 4 and ataxia-ocular apraxia 2 106,286 . The molecular link between neurologic diseases and replication stress may lie in the fact that many of the genes involved in brain development are long and are therefore more susceptible to collisions between transcription and replication, 127 transcription-associated DNA damage, or replication stress-induced segregation defects and aneuploidy 287 …”

Section: The Role Of Mitotic Replication Stress In Human Diseasementioning

confidence: 99%

Rescue from replication stress during mitosis

Fragkos

Naim

2017

Cell Cycle

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Genomic instability is a hallmark of cancer and a common feature of human disorders, characterized by growth defects, neurodegeneration, cancer predisposition, and aging. Recent evidence has shown that DNA replication stress is a major driver of genomic instability and tumorigenesis. Cells can undergo mitosis with under-replicated DNA or unresolved DNA structures, and specific pathways are dedicated to resolving these structures during mitosis, suggesting that mitotic rescue from replication stress (MRRS) is a key process influencing genome stability and cellular homeostasis. Deregulation of MRRS following oncogene activation or loss-of-function of caretaker genes may be the cause of chromosomal aberrations that promote cancer initiation and progression. In this review, we discuss the causes and consequences of replication stress, focusing on its persistence in mitosis as well as the mechanisms and factors involved in its resolution, and the potential impact of incomplete replication or aberrant MRRS on tumorigenesis, aging and disease.

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“…Numerical whole chromosome instability ( W-CIN ) is a cellular state with a high propensity for chromosome mis-segregation generated by defects in the mitotic machinery and in cellular pathways controlling chromosome segregation, such as the Spindle Assembly Checkpoint ( SAC ) and sister chromatid cohesion 3 4 . Accordingly, deficient expression of components from either pathway results in W-CIN in vitro and in vivo 5 6 7 8 .…”

mentioning

confidence: 99%

“…Several mammalian tissues undergo changes in ploidy during normative aging, such as the brain 9 , liver 10 , lymphocytes 11 , oocytes 12 , lungs, kidney and heart 13 . Interestingly, decreased levels of SAC, cohesin and kinetochore proteins are observed in tissues that undergo age-related aneuploidization 3 14 15 , which could be causative of W-CIN generation at older age.…”

mentioning

confidence: 99%

Whole Chromosome Instability induces senescence and promotes SASP

Andriani

Almeida

Faggioli

et al. 2016

Sci Rep

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122

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Age-related accumulation of ploidy changes is associated with decreased expression of genes controlling chromosome segregation and cohesin functions. To determine the consequences of whole chromosome instability (W-CIN) we down-regulated the spindle assembly checkpoint component BUB1 and the mitotic cohesin SMC1A, and used four-color-interphase-FISH coupled with BrdU incorporation and analyses of senescence features to reveal the fate of W-CIN cells. We observed significant correlations between levels of not-diploid cells and senescence-associated features (SAFs). W-CIN induced DNA double strand breaks and elevated oxidative stress, but caused low apoptosis. SAFs of W-CIN cells were remarkably similar to those induced by replicative senescence but occurred in only 13 days versus 4 months. Cultures enriched with not-diploid cells acquired a senescence-associated secretory phenotype (SASP) characterized by IL1B, CXCL8, CCL2, TNF, CCL27 and other pro-inflammatory factors including a novel SASP component CLEC11A. These findings suggest that W-CIN triggers premature senescence, presumably to prevent the propagation of cells with an abnormal DNA content. Cells deviating from diploidy have the ability to communicate with their microenvironment by secretion of an array of signaling factors. Our results suggest that aneuploid cells that accumulate during aging in some mammalian tissues potentially contribute to age-related pathologies and inflammation through SASP secretion.

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Mechanisms and consequences of aneuploidy and chromosome instability in the aging brain

Cited by 41 publications

References 240 publications

“Amyloid‐beta accumulation cycle” as a prevention and/or therapy target for Alzheimer's disease

“Amyloid‐beta accumulation cycle” as a prevention and/or therapy target for Alzheimer's disease

Rescue from replication stress during mitosis

Whole Chromosome Instability induces senescence and promotes SASP

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