# Project 1: Developmental Programming and Aging Interactions in Primate Brain  and Glucocorticoid Function.

> **NIH NIH U19** · UNIVERSITY OF WYOMING · 2021 · $272,983

## Abstract

Project 1: Developmental Programming and Aging Interactions in Primate Brain and Glucocorticoid
Function
Lead PI: Peter Nathanielsz; Multiple PIs: Cun Li, Peter Fox
ABSTRACT
Controlled translational animal studies are needed to determine how developmental programming-aging
interactions by glucocorticoid (GC- cortisol) and other mechanisms, e.g. blood flow and metabolism, influence
brain aging and cognitive decline. Evidence supports early blood GC changes and activity and other
antecedents of aging. The Barker programming hypothesis states responses to specific challenges in critical
developmental time windows alter the developmental trajectory with persistent effects on phenotype.
Preliminary data. We 1) confirmed a linear baboon plasma cortisol fall starting at 6y age (human ~15y) and
showed a fall in paraventricular nuclear (PVN) vasopressin and increased GC receptor (GR), potential
mechanisms for the fall (increased feedback and decreased PVN drive); 2) peripheral cortisol production; and
3) GR and blood flow changes with aging.
Premises. 1. Aging antecedents are present early in the hippocampal-hypothalamo-pituitary (HHPA) axis,
brain function, and behavior. 2a. Moderate perinatal global nutrient reduction-induced IUGR alters HHPA, brain
structure and function, and behavior, evident in changes in IUGR offspring (F1) aging biomarkers compared to
controls who received normal perinatal nutrition. 2b. Maternal obesity (MO) in the perinatal period alters HHPA,
brain structure and function, and behavior, evident in changes in aging biomarkers in MO F1 vs. controls who
received normal perinatal nutrition. 2c. Cortisol replacement from 13y to maintain cortisol at 5y levels increases
the HHPA, brain, and behavior rate of aging, evident in changes in HHPA and brain-related aging biomarkers
vs. controls. 3. Comparing normative, life course observational control data with data from interventions that
alter the aging trajectory provides insights into key mechanisms in systems and cellular aging pathways. Data
will provide information for translation to humans to anticipate age-related mechanisms that both increase and
decrease health span, enabling development of markers and interventions in human aging
Approach. We study 96 baboons over 24-68% of the life course, equal males and females. Groups: 1. Normal
life course; 2. IUGR (F1) of 30% globally food reduced mothers; 3. F1 of over-nourished, obese mothers; 4.
Cortisol Replacement Intervention beginning at 13y to maintain baboons' cortisol at 5y old levels for 5 years to
address cortisol regulated mechanisms. We conduct awake, tether studies, 24h rhythms, HHPA suppression
and stimulation, MRI, brain histology, and cognitive tests to relate phenotype to cellular pathways. No baboons
are euthanized. We integrate our fetal and adult tissue archives with in vivo studies. Innovation. We propose a
new framework to understand aging based on programming-aging interactions. Environment. With our funds,
we built ...

## Key facts

- **NIH application ID:** 10201487
- **Project number:** 5U19AG057758-04
- **Recipient organization:** UNIVERSITY OF WYOMING
- **Principal Investigator:** PETER W. NATHANIELSZ
- **Activity code:** U19 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2021
- **Award amount:** $272,983
- **Award type:** 5
- **Project period:** 2018-09-30 → 2023-05-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10201487

## Citation

> US National Institutes of Health, RePORTER application 10201487, Project 1: Developmental Programming and Aging Interactions in Primate Brain  and Glucocorticoid Function. (5U19AG057758-04). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/10201487. Licensed CC0.

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