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1. Lifespan effects in male UM-HET3 mice treated with sodium thiosulfate, 16-hydroxyestriol, and late-start canagliflozin.

2. Differential mitochondrial bioenergetics and cellular resilience in astrocytes, hepatocytes, and fibroblasts from aging baboons.

3. The common marmoset as a translational model of age-related osteoarthritis.

4. Changes in oral health during aging in a novel non-human primate model.

5. Age‐related changes in hematological biomarkers in common marmosets.

6. Sensory innervation of masseter, temporal and lateral pterygoid muscles in common marmosets.

7. Pan-primate studies of age and sex.

8. Sexually dimorphic effects of methionine sulfoxide reductase A (MsrA) on murine longevity and health span during methionine restriction.

9. Testing the evidence that lifespan-extending compound interventions are conserved across laboratory animal model species.

10. Canagliflozin retards age-related lesions in heart, kidney, liver, and adrenal gland in genetically heterogenous male mice.

11. Determination of dexamethasone dose for cortisol suppression in adult common marmosets (Callithrix jacchus).

12. Short term treatment with a cocktail of rapamycin, acarbose and phenylbutyrate delays aging phenotypes in mice.

13. Metabolic benefits of methionine restriction in adult mice do not require functional methionine sulfoxide reductase A (MsrA).

14. DNA methylation age analysis of rapamycin in common marmosets.

15. San Antonio Nathan Shock Center: your one-stop shop for aging research.

16. Age and sex modify cellular proliferation responses to oxidative stress and glucocorticoid challenges in baboon cells.

17. Chloride channel accessory 1 integrates chloride channel activity and mTORC1 in aging‐related kidney injury.

18. Beta-guanidinopropionic acid has age-specific effects on markers of health and function in mice.

19. Primary neuron and astrocyte cultures from postnatal Callithrix jacchus: a non-human primate in vitro model for research in neuroscience, nervous system aging, and neurological diseases of aging.

20. Rapamycin‐mediated mouse lifespan extension: Late‐life dosage regimes with sex‐specific effects.

21. Is Rapamycin a Dietary Restriction Mimetic?

22. Aging research using the common marmoset: Focus on aging interventions.

23. Maternal nutrient restriction in baboon programs later-life cellular growth and respiration of cultured skin fibroblasts: a potential model for the study of aging-programming interactions.

25. Pharmaceutical inhibition of mTOR in the common marmoset: effect of rapamycin on regulators of proteostasis in a non-human primate.

26. MsrA Overexpression Targeted to the Mitochondria, but Not Cytosol, Preserves Insulin Sensitivity in Diet-Induced Obese Mice.

27. Rapamycin and Dietary Restriction Induce Metabolically Distinctive Changes in Mouse Liver.

28. Altered metabolism and resistance to obesity in long-lived mice producing reduced levels of IGF-I.

31. Rapamycin-mediated lifespan increase in mice is dose and sex dependent and metabolically distinct from dietary restriction.

32. Mice Producing Reduced Levels of Insulin-Like Growth Factor Type 1 Display an Increase in Maximum, but not Mean, Life Span.

33. Mice Fed Rapamycin Have an Increase in Lifespan Associated with Major Changes in the Liver Transcriptome.

34. Genetic Disruption of SOD1 Gene Causes Glucose Intolerance and Impairs β-Cell Function.

35. Short-Term Treatment With Rapamycin and Dietary Restriction Have Overlapping and Distinctive Effects in Young Mice.

36. Reduction of glucose intolerance with high fat feeding is associated with anti-inflammatory effects of thioredoxin 1 overexpression in mice.

37. Increased superoxide in vivo accelerates age-associated muscle atrophy through mitochondrial dysfunction and neuromuscular junction degeneration.

38. Overexpression of Mn Superoxide Dismutase Does Not Increase Life Span in Mice.

39. Insulin resistance is a cellular antioxidant defense mechanism.

40. Lack of methionine sulfoxide reductase A in mice increases sensitivity to oxidative stress but does not diminish life span.

41. The long lifespan of two bat species is correlated with resistance to protein oxidation and enhanced protein homeostasis.

43. Protein stability and resistance to oxidative stress are determinants of longevity in the longest-living rodent, the naked mole-rat.

44. Reduction of mitochondrial H2O2 by overexpressing peroxiredoxin 3 improves glucose tolerance in mice.

45. Cells From Long-Lived Mutant Mice Exhibit Enhanced Repair of Ultraviolet Lesions.

46. Fibroblasts From Naked Mole-Rats Are Resistant to Multiple Forms of Cell Injury, But Sensitive to Peroxide, Ultraviolet Light, and Endoplasmic Reticulum Stress.

47. Skin-derived fibroblasts from long-lived species are resistant to some, but not all, lethal stresses and to the mitochondrial inhibitor rotenone.

48. Fibroblast cell lines from young adult mice of long-lived mutant strains are resistant to multiple forms of stress.

49. A COST OF REPRODUCTION IN DROSOPHILA MELANOGASTER: STRESS SUSCEPTIBILITY.

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