Genome-wide RNA polymerase stalling shapes the transcriptome during aging

Gyenis, Ákos; Chang, Jiang; Demmers, Joris J. P. G.; Bruens, Serena T.; Barnhoorn, Sander; Brandt, Renata M. C.; Baar, Marjolein P.; Rašeta, Marko; Derks, Kasper; Hoeijmakers, Jan H.J.; Pothof, Joris

doi:10.1038/s41588-022-01279-6

Cited by 77 publications

(72 citation statements)

References 79 publications

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“…Recent research, including my own, has revealed that as an organism ages, its transcriptome changes in a manner that is informed by the lengths of transcript molecules. This relationship between transcript length and aging has been first observed by the lab of Jan Hoeijmakers 8 , and since then been described for C. elegans 9 , fruit flies 10 , killifish 11 , mice 8,9,[11][12][13] , rats 11 , and humans 8,11,14 . In most cases, the correlation between transcript length and age-dependent change is negative, although some tissues and cell types exhibit a positive correlation 11 .…”

Section: Introductionmentioning

confidence: 72%

“…There are many reviews on organismal 63,64 and molecular damage 39,[65][66][67][68][69] , but it is challenging to find a well-cited review on the various types of transcript damage that occur during biological aging. These damages extend beyond premature termination 9 and include intron retention 27,28 , oxidative damage 70 , and lost synchronization toward the circadian rhythm 71 . It is surprising how few reviews discuss transcript damages 22,39,72,73 , given that research by Lorena Harries and colleagues 74 found that out of 1,065 considered biological and metabolic pathways, six of the seven pathways significantly associated with age in human peripheral blood leukocytes are related to RNA metabolism.…”

Section: Discussionmentioning

confidence: 99%

“…This figure, adapted from Cohen et al 6 (licensed under CC BY 4.0), illustrates the inputs and outputs connected to length-correlated changes of the transcriptome. References for the specific inputs and outputs are provided 8,9,11,13,21,55 . Note that this figure includes references to the preprint version 55 of a recent manuscript of mine, as I had removed some material following reviewer feedback to enhance focus.…”

Section: Reanalysis Of Lincs1000mentioning

confidence: 99%

“…In most cases, the correlation between transcript length and age-dependent change is negative, although some tissues and cell types exhibit a positive correlation 11 . The strength of these correlations can be influenced by various factors, such as UV radiation exposure 9 or smoking 13 or caloric restriction 8 .…”

Section: Introductionmentioning

confidence: 99%

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The Road Less Traveled: Uncovering the Convergence Toward Specific Pleiotropic Phenotypes in Aging

Stoeger

2023

Preprint

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Aging is a complex process influenced by a wide range of environmental and molecular factors. Despite this complexity, individuals tend to age in highly similar ways, leading to the question of what drives this convergence. Recent research, including my own discoveries, suggests that the length of transcript molecules plays a crucial role in age-dependent changes to the transcriptome. Drawing inspiration from the road trip analogy of cellular transcription, I propose that a non-linear scaling law drives convergence towards specific pleiotropic phenotypes in biological aging. This scaling law is based on the notion that molecular changes observed during aging may reflect unspecific damage to cellular physiology. By validating this hypothesis, I can improve our understanding of biological aging and identify new candidate compounds for anti-aging interventions, as well as re-identify one known intervention. This work has actionable implications for improving human health and extending lifespans.

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Section: Introductionmentioning

confidence: 72%

Section: Discussionmentioning

confidence: 99%

Section: Reanalysis Of Lincs1000mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The Road Less Traveled: Uncovering the Convergence Toward Specific Pleiotropic Phenotypes in Aging

Stoeger

2023

Preprint

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“…It will be interesting to investigate if a similar reduction of TC-NER capacity can be measured in aging tissues of e.g. mouse models of aging, as accumulating DNA damage leading to transcription stress is considered one of the driving forces of the aging process (22, 64).…”

Section: Resultsmentioning

confidence: 99%

Recovery of protein synthesis to measure transcription-coupled DNA repair in living cells and tissues

Woude

Davó-Martínez

Thijssen

et al. 2023

Preprint

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Transcription-coupled nucleotide excision repair (TC-NER) is an important DNA repair mechanism that protects against the negative effects of transcription-blocking DNA lesions. Hereditary TC-NER deficiency causes pleiotropic and often severe neurodegenerative and progeroid symptoms. Multiple assays have been developed for the clinic and for research to measure TC-NER activity, which is hampered by the relatively low abundance of repair events taking place in transcribed DNA. "Recovery of RNA Synthesis" is widely used as indirect TC-NER assay based on the notion that lesion-blocked transcription only resumes after successful TC-NER. Here, we show that measuring novel synthesis of a protein that has been degraded prior to DNA damage induction is an equally effective but more versatile manner to indirectly monitor TC-NER. This "Recovery of Protein Synthesis" (RPS) assay is readily adaptable for use with different degradable proteins and readouts, including fluorescence imaging and immunoblot. Moreover, with the RPS assay TC-NER activity can be measured in real-time, in various living cells types and even in differentiated tissues of living organisms. As example, we show that TC-NER capacity declines in aging muscle tissue of C. elegans. Therefore, the RPS assay constitutes an important novel clinical and research tool to investigate transcription-coupled DNA repair.

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Nurturing longevity through natural compounds: Where do we stand, and where do we go?

Todorova,

Savova,

Mihaylova

et al. 2024

Food Frontiers

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The revolution in aging research through the past decade has driven the progress in interventions that promote longevity. Dissection of the “old” hallmarks of aging has provided solid data for the definition of at least three “new” ones, opening avenues for the development of novel hallmark‐targeted pro‐longevity approaches. The quest for geroprotectors is of enormous interest with the ultimate goal of finding the alchemical stone that induces healthy aging and increases lifespan, pushing the limits of human longevity or even uncovering the absence of such limits. Several of the well‐appreciated geroprotectors that are recognized as longevity promoters are of natural origin such as metformin, resveratrol, aspirin, and spermidine. As the search for pharmacological modulators of healthspan and lifespan continues, numerous studies are focusing on the potential of plant secondary metabolites. The current review attempts to critically assess the available interventions and the breakthrough discoveries in the field of longevity research over the past decade. Correspondingly, novel approaches targeting the hallmarks of aging have been outlined, and the future goals in longevity research have been enlightened. Special emphasis has been placed on the potential of plant‐derived compounds as pro‐longevity agents.

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Genome-wide RNA polymerase stalling shapes the transcriptome during aging

Cited by 77 publications

References 79 publications

The Road Less Traveled: Uncovering the Convergence Toward Specific Pleiotropic Phenotypes in Aging

The Road Less Traveled: Uncovering the Convergence Toward Specific Pleiotropic Phenotypes in Aging

Recovery of protein synthesis to measure transcription-coupled DNA repair in living cells and tissues

Nurturing longevity through natural compounds: Where do we stand, and where do we go?

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