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Non-Genomic Hallmarks of Aging-The Review

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MDPI
DOI: 10.3390/ijms242015468

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aging; hallmarks; non-genomic; cancer

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Aging is a natural process that involves molecular, cellular, and tissue-level changes, which can increase the risk of diseases like cancer. The hallmarks of aging, including genomic and non-genomic changes, play a significant role in aging and cancer. Understanding the non-genomic hallmarks and their relationship with aging and cancer could help develop approaches to slow down aging and prevent cancer.
Aging is a natural, gradual, and inevitable process associated with a series of changes at the molecular, cellular, and tissue levels that can lead to an increased risk of many diseases, including cancer. The most significant changes at the genomic level (DNA damage, telomere shortening, epigenetic changes) and non-genomic changes are referred to as hallmarks of aging. The hallmarks of aging and cancer are intertwined. Many studies have focused on genomic hallmarks, but non-genomic hallmarks are also important and may additionally cause genomic damage and increase the expression of genomic hallmarks. Understanding the non-genomic hallmarks of aging and cancer, and how they are intertwined, may lead to the development of approaches that could influence these hallmarks and thus function not only to slow aging but also to prevent cancer. In this review, we focus on non-genomic changes. We discuss cell senescence, disruption of proteostasis, deregualation of nutrient sensing, dysregulation of immune system function, intercellular communication, mitochondrial dysfunction, stem cell exhaustion and dysbiosis.

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