Abstract (Easy to Understand Article)
Imagine if a simple injection of “young DNA” could help older animals—and potentially people—turn back the clock. Scientists now suspect that tiny genetic signals, whether from exosomes (little bubbles with microRNAs) or purified DNA fragments, might push aging cells to act younger. One striking example is Dr. Harold Katcher’s “E5” therapy, which used factors from young pig blood to reverse biological age markers in rats by over 60%. Researchers also note that normal cell turnover (apoptosis) might naturally release small DNA pieces that keep tissues “in sync” with a body’s overall age, suggesting there’s already a built-in system for coordinating youth signals. By carefully harnessing these DNA or RNA-based messengers—and ensuring they don’t trigger harmful immune responses—we could be looking at a new and surprisingly straightforward route to rejuvenation. This paper highlights how epigenetics, exosomes, and possibly even raw DNA injections are coming together in the quest to make cells feel (and function) younger.
Before we get started let me just whet your appetite about what is contained in the rest of this article. The results of the most important study on aging EVER, that will be the most important study of aging for all time- have just been released! Steve Horvath’s :
Universal DNA methylation age across mammalian tissues
The study proves conclusively that aging is selected for by evolution and is programmed. A result that contradicts all major mainstream theories of aging that have been proposed since the early 1900’s. It turns out August Weisman got the right answer in 1882 but with the wrong reasoning.
The new study also reveals the true cause of aging at the cellular level- the programmed loss of cellular differentiation.
UPDATE- Everything in this article has been proven to be most likely correct with Steve Horvath’s new study in mammals…
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