Nobel Prize-winning research identified genes (Yamanaka factors) that revert specialized adult cells back into their embryonic, stem-cell state. This discovery proves cellular differentiation and aging are not irreversible, opening the door for regenerative therapies by "rebooting" cells to an earlier state.

The book posits that aging is a loss of epigenetic information, not an irreversible degradation of our DNA. Our cells' "software" forgets how to read the "hardware" (DNA) correctly. This suggests aging can be rebooted, much like restoring a computer's operating system.

When addressing hormone imbalances, start at the base of the "hormone pyramid." Optimizing foundational hormones like cortisol (stress) and insulin (blood sugar) is essential, as they directly impact thyroid function and sex hormones like estrogen and testosterone.

A 7-year study of healthy individuals over 85 found minimal genetic differences from their less healthy counterparts. The key to their extreme healthspan appears to be a robust immune system, which is significantly shaped by lifestyle choices, challenging the common narrative about being born with "good genes."

Dr. D'Agostino gives his aging, neutered dogs a Selective Androgen Receptor Modulator (SARM) to stimulate muscle protein synthesis and maintain vitality. This approach is analogous to Testosterone Replacement Therapy (TRT) in humans, aiming to counteract the loss of skeletal muscle mass associated with aging and hormonal changes.

Modern ethical boards make certain human studies, like extended fasting, nearly impossible to conduct. This creates an opportunity to revisit older, pre-regulatory research from places like the Soviet Union. While the proposed mechanisms may be outdated, the raw data could unlock valuable modern therapeutic approaches.

By auditing the "noise" or corruption in a cell's epigenetic settings, scientists can determine a biological age. This "epigenetic clock" is a better indicator of true health than birth date, revealing that a 40-year-old could have the biology of a 30-year-old.

The principle of hormesis shows that stressors like fasting and cold exposure trigger a self-preservation state in cells. This "hunker down" mode activates repair mechanisms like sirtuin proteins, which clean up cellular damage, making these seemingly negative activities profoundly healthy.

The common aversion to living to 120 stems from assuming extra years will be spent in poor health. The goal of longevity science is to extend *healthspan*—the period of healthy, mobile life—which reframes the debate from merely adding years to adding high-quality life.