Identification of microRNAs dysregulated in cellular senescence driven by endogenous genotoxic stress

Nidadavolu, Lolita S.; Niedernhofer, Laura J.; Khan, Saleem Ayaz

doi:10.18632/aging.100571

Cited by 40 publications

(32 citation statements)

References 57 publications

(66 reference statements)

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“…miR‐22‐3p and miR‐128‐3p were positively correlated with age at onset in iPD, but not SNCA A53T or GBA PD. miR‐22‐3p targets GBA mRNA, whereas miR‐128‐3p is a marker of mild cognitive impairment and cellular senescence . Moreover, miR‐128‐3p has been shown to govern motor activity by suppressing the expression of various ion channels and mitogen‐activated protein kinase 1 (ERK2) signaling components and its overexpression attenuates motor abnormalities associated with Parkinson's‐like disease and seizures in mice .…”

Section: Discussionmentioning

confidence: 99%

Circulating Brain‐Enriched MicroRNAs for Detection and Discrimination of Idiopathic and Genetic Parkinson's Disease

et al. 2019

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Background A minimally invasive test for early detection and monitoring of Parkinson's disease (PD) is a highly unmet need for drug development and planning of patient care. Blood plasma represents an attractive source of biomarkers. MicroRNAs (miRNAs) are conserved noncoding RNA molecules that serve as posttranscriptional regulators of gene expression. As opposed to ubiquitously expressed miRNAs that control house‐keeping processes, brain‐enriched miRNAs regulate diverse aspects of neuron development and function. These include neuron‐subtype specification, axonal growth, dendritic morphogenesis, and spine density. Backed by a large number of studies, we now know that the differential expression of neuron‐enriched miRNAs leads to brain dysfunction. Objectives The aim was to identify subsets of brain‐enriched miRNAs with diagnostic potential for familial and idiopathic PD as well as specify the molecular pathways deregulated in PD. Methods Initially, brain‐enriched miRNAs were selected based on literature review and validation studies in human tissues. Subsequently, real‐time reverse transcription polymerase chain reaction was performed in the plasma of 100 healthy controls and 99 idiopathic and 53 genetic (26 alpha‐synucleinA53T and 27 glucocerebrosidase) patients. Statistical and bioinformatics analyses were carried out to pinpoint the diagnostic biomarkers and deregulated pathways, respectively. Results An explicit molecular fingerprint for each of the 3 PD cohorts was generated. Although the idiopathic PD fingerprint was different from that of genetic PD, the molecular pathways deregulated converged between all PD subtypes. Conclusions The study provides a group of brain‐enriched miRNAs that may be used for the detection and differentiation of PD subtypes. It has also identified the molecular pathways deregulated in PD. © 2019 International Parkinson and Movement Disorder Society

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Section: Discussionmentioning

confidence: 99%

Circulating Brain‐Enriched MicroRNAs for Detection and Discrimination of Idiopathic and Genetic Parkinson's Disease

et al. 2019

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“…Cells that experience oxidative stress may undergo senescence. In embryonic fibroblasts from a mouse model that rapidly accumulates DNA damage from oxidative stress, miR-449a, miR-455, and miR-128 were found to be significantly downregulated (Nidadavolu et al, 2013). These results mirrored expression found in kidneys of elderly mice.…”

Section: Mirna Synthesis/actionmentioning

confidence: 99%

Are microRNAs true sensors of ageing and cellular senescence?

Williams

Smith

Kumar

et al. 2017

Ageing Research Reviews

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All living beings are programmed to death due to aging and age-related processes. Aging is a normal process of every living species. While all cells are inevitably progressing towards death, many disease processes accelerate the aging process, leading to senescence. Pathologies such as Alzheimer’s disease, Parkinson’s disease, multiple sclerosis, amyotrophic lateral sclerosis, Huntington’s disease, cardiovascular disease, cancer, and skin diseases have been associated with deregulated aging. Healthy aging can delay onset of all age-related diseases. Genetics and epigenetics are reported to play large roles in accelerating and/or delaying the onset of age-related diseases. Cellular mechanisms of aging and age-related diseases are not completely understood. However, recent molecular biology discoveries have revealed that microRNAs (miRNAs) are potential sensors of aging and cellular senescence. Due to miRNAs capability to bind to the 3’ untranslated region (UTR) of mRNA of specific genes, miRNAs can prevent the translation of specific genes. The purpose of our article is to highlight recent advancements in miRNAs and their involvement in cellular changes in aging and senescence. Our article discusses the current understanding of cellular senescence, its interplay with miRNAs regulation, and how they both contribute to disease processes.

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“…In nematodes, miRNA‐binding proteins Argonaute‐like 1 (alg‐1), Dicer, Drosha, and DGCR8/Pasha regulate aging and control life span (Kato et al , ; Lehrbach et al , ; Mori et al , ). The activity of at least one of these miRNA‐binding proteins, Dicer, decreases also in aging mammals; Dicer was found to be globally down‐regulated in old mouse tissues in comparison with their younger adult counterparts (Nidadavolu et al , ).…”

Section: Mirna Activity and Stress Signaling In Human Diseasementioning

confidence: 99%

mi RNA s at the interface of cellular stress and disease

Emde

Hornstein

2014

EMBO J

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microRNAs (miRNAs) are a family of small, non-coding RNAs, which provides broad silencing activity of mRNA targets in a sequencedependent fashion. This review explores the hypothesis that the miRNA machinery is intimately linked with the cellular stress pathway and apparatus. Stress signaling potentially alters the function of the miRNA-bioprocessing core components and decompensates regulation. In addition, dysregulation of miRNA activity renders the cell more prone to stress and emerges as a new pathway for agerelated insults and diseases, such as neurodegeneration.

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Identification of microRNAs dysregulated in cellular senescence driven by endogenous genotoxic stress

Cited by 40 publications

References 57 publications

Circulating Brain‐Enriched MicroRNAs for Detection and Discrimination of Idiopathic and Genetic Parkinson's Disease

Circulating Brain‐Enriched MicroRNAs for Detection and Discrimination of Idiopathic and Genetic Parkinson's Disease

Are microRNAs true sensors of ageing and cellular senescence?

mi RNA s at the interface of cellular stress and disease

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