A new longevity stem cell therapy in monkeys showed an estimated 3โ5 yrs of biological age reversal, across 54% of tissues. Scaled cautiously to humans, could correspond to ~9โ15 years of rejuvenation.
If this replicates, it's a big deal. ๐งต

What researchers did: engineered human embryonic stem cells (hESCs) with a modified FOXO3 gene (FOXO3SA2/SA2) to resist degradation.
These hESCs were then differentiated into senescence-resistant mesenchymal progenitor cells (SRCs). When injected into cynomolgus monkeys (2 million cells/kg) across various age groups, SRCs demonstrated significant rejuvenation, reversing brain atrophy, blood senescence, inflammation, and oxidative stress.
Transcriptomic and epigenetic analyses confirmed biological age reversal in organs like skin, aorta, lungs, and the digestive system.
FOXO3-enhanced senescence resistant MPCs (SRCs) consistently outperformed wild-type MPCs, producing systemic rejuvenation across brain, blood, and organs.
On average, this corresponded to estimated 3โ5 years of biological age reversal, across 54% of tissues (vs 31% with WTCs). Scaled cautiously to humans, this may approximate ~9โ15 years of rejuvenation.
These hESCs were then differentiated into senescence-resistant mesenchymal progenitor cells (SRCs). When injected into cynomolgus monkeys (2 million cells/kg) across various age groups, SRCs demonstrated significant rejuvenation, reversing brain atrophy, blood senescence, inflammation, and oxidative stress.
Transcriptomic and epigenetic analyses confirmed biological age reversal in organs like skin, aorta, lungs, and the digestive system.
FOXO3-enhanced senescence resistant MPCs (SRCs) consistently outperformed wild-type MPCs, producing systemic rejuvenation across brain, blood, and organs.
On average, this corresponded to estimated 3โ5 years of biological age reversal, across 54% of tissues (vs 31% with WTCs). Scaled cautiously to humans, this may approximate ~9โ15 years of rejuvenation.
Here are some of the effects in more detail.
SRCs = are special stem cells engineered with a FOXO3 tweak that makes them resistant to aging
WTCs = are the normal โwild-typeโ cells without that upgrade
Brain
+ Cortical thickness and volume restored toward youthful levels: SRC up to ~50โ70% vs WTC ~10โ20% (inferred from imaging and figure analysis; not direct author statistics).
+ Hippocampus sn-transcriptAge: SRC โ2.5 years (WTC not reported).
+ Cognition: significant improvement with SRC; modest effect with WTC.
Blood / Immune
+ Age-related gene programs reversed: SRC 39% (upregulated) / 30% (downregulated); WTC reversed fewer (Fig. 2CโD, no exact percentages reported).
+ Equivalent immune rejuvenation: SRC 3 years vs WTC 1.5 years (observational estimate, not author statistic).
Organs (transcriptomic & epigenomic)
+ Average transcriptomic rejuvenation: SRC โ3.34 years (54% of tissues) vs WTC โ2.80 years (31% of tissues).
+ Standout tissues:
โข Skin: SRC โ5.6 years vs WTC โ4.4 years
โข Lung: SRC โ4.1 years vs WTC โ3.3 years
โข Skeletal muscle: SRC โ4.9 / โ3.5 years vs WTC โ3.2 / โ2.4 years
โข Spleen: SRC โ2.6 years vs WTC โ1.9 years
โข Hippocampus: SRC โ2.0 years vs WTC โ1.5 years
+ Reproductive system: Ovaries SRC โ4.5 years vs WTC โ3.1 years; granulosa cells showed >6 years reversal with SRC.
+ DNAmAge: Brain โ5 years, skeletal muscle โ4 years, spleen โ2 years with SRC; WTC changes negligible.
Safety
+ Dose: 2 million cells/kg IV biweekly for 44 weeks.
+ No fevers, immune rejection, or metabolic issues in either group.
+ No tumors at the primate dose of 2 million cells/kg, or even at 10ร higher dose (20 million cells/kg) in nude mice.
SRCs = are special stem cells engineered with a FOXO3 tweak that makes them resistant to aging
WTCs = are the normal โwild-typeโ cells without that upgrade
Brain
+ Cortical thickness and volume restored toward youthful levels: SRC up to ~50โ70% vs WTC ~10โ20% (inferred from imaging and figure analysis; not direct author statistics).
+ Hippocampus sn-transcriptAge: SRC โ2.5 years (WTC not reported).
+ Cognition: significant improvement with SRC; modest effect with WTC.
Blood / Immune
+ Age-related gene programs reversed: SRC 39% (upregulated) / 30% (downregulated); WTC reversed fewer (Fig. 2CโD, no exact percentages reported).
+ Equivalent immune rejuvenation: SRC 3 years vs WTC 1.5 years (observational estimate, not author statistic).
Organs (transcriptomic & epigenomic)
+ Average transcriptomic rejuvenation: SRC โ3.34 years (54% of tissues) vs WTC โ2.80 years (31% of tissues).
+ Standout tissues:
โข Skin: SRC โ5.6 years vs WTC โ4.4 years
โข Lung: SRC โ4.1 years vs WTC โ3.3 years
โข Skeletal muscle: SRC โ4.9 / โ3.5 years vs WTC โ3.2 / โ2.4 years
โข Spleen: SRC โ2.6 years vs WTC โ1.9 years
โข Hippocampus: SRC โ2.0 years vs WTC โ1.5 years
+ Reproductive system: Ovaries SRC โ4.5 years vs WTC โ3.1 years; granulosa cells showed >6 years reversal with SRC.
+ DNAmAge: Brain โ5 years, skeletal muscle โ4 years, spleen โ2 years with SRC; WTC changes negligible.
Safety
+ Dose: 2 million cells/kg IV biweekly for 44 weeks.
+ No fevers, immune rejection, or metabolic issues in either group.
+ No tumors at the primate dose of 2 million cells/kg, or even at 10ร higher dose (20 million cells/kg) in nude mice.

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