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MOŻE CI SIĘ SPODOBAĆ
The irreversible state of cell cycle arrest in which cells remain metabolically active but stop dividing, contributing to tissue aging and chronic inflammation.
Cellular senescence is a state of stable, irreversible cell cycle arrest in which cells remain metabolically active but permanently cease dividing. Senescence can be triggered by telomere shortening, DNA damage, oncogene activation, oxidative stress, or mitochondrial dysfunction. While senescence initially serves protective functions by preventing damaged cells from proliferating, the accumulation of senescent cells with age becomes pathological. Senescent cells secrete a complex mixture of pro-inflammatory cytokines, chemokines, and proteases known as the senescence-associated secretory phenotype (SASP), which drives chronic inflammation and tissue dysfunction. NAD+ decline promotes senescence by impairing sirtuin-mediated stress responses and DNA repair, while NAD+ supplementation research aims to delay senescence onset by maintaining cellular repair capacity.
SCIENCE
General research term
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Nicotinamide Adenine Dinucleotide, an essential coenzyme in every living cell that drives energy metabolism, DNA repair, and sirtuin-mediated longevity pathways.
Repetitive DNA sequences (TTAGGG) at chromosome ends that protect genetic information during cell division, progressively shortening with age.
An imbalance between reactive oxygen species production and antioxidant defences, leading to cellular and molecular damage associated with aging and disease.
A cellular self-cleaning process that degrades and recycles damaged organelles, misfolded proteins, and pathogens, crucial for longevity and cellular health.
Small signalling proteins secreted by immune and tissue cells that modulate inflammation, immune responses, and cell communication.
The physiological process of forming new blood vessels from pre-existing vasculature, essential for wound healing, tissue repair, and nutrient delivery.
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