We know senescent cells contribute to body dysfunction (ageing). We know telomere shortening is a recognized cause of cellular senescence. Several conditions associated with normal ageing are precipitated by accelerated telomere dysfunction.
#BagOfBeans
ncbi.nlm.nih.gov/pmc/articles/P…

When you are reading papers or studies about cancer, inflammation, cellular senescence, stem cell exhaustion, mitochondrial dysfunction, genomic instability, telomere dysfunction and cellular aging - it is important to look for references AFTER 2009.

Prior to 2009, the dominant theory was free radicals coming from mitochondria processing of oxygen (ROS) created a feedforward loop linking telomere dysfunction, mitochondrial dysfunction and more oxidative stress pathways, resulting in ageing. Not all theories are right.

That theory only partially explains the age-related increase in the inflammatory response seen in the aged population. It doesn't explain the cooperation between cell-intrinsic telomere dysfunction-driven molecular pathways and the microbiome in driving the inflammatory response.

After 2009, we understood how human chromosomes can be copied in a complete way during cell divisions while they are protected against degradation using Nonsense-mediated mRNA decay (NMD).
en.wikipedia.org/wiki/Nonsense-…

We solved a major problem in biology: the cure against aging is found in the ends of the chromosomes – the telomeres – and in an enzyme that forms them – telomerase. The process of detecting aberrant transcripts occurs during the translation of the mRNA.

nobelprize.org/prizes/medicin…

That discovery of such a fundamental mechanism in the cell has stimulated the development of gut biome therapeutic strategies but it's also enabled us to characterize the causation of certain metabolic diseases.

en.wikipedia.org/wiki/Metabolic…