The Power of the Heterogeneous Stock Rat Founder Strains in Modeling Metabolic Disease

Author:

Wagner Valerie A1ORCID,Holl Katie L1,Clark Karen C23ORCID,Reho John J14ORCID,Lehmler Hans-Joachim5ORCID,Wang Kai6,Grobe Justin L1247,Dwinell Melinda R12ORCID,Raff Hershel1238ORCID,Kwitek Anne E1279ORCID

Affiliation:

1. Department of Physiology, Medical College of Wisconsin , Milwaukee, WI 53226 , USA

2. Cardiovascular Center, Medical College of Wisconsin , Milwaukee, WI 53226 , USA

3. Department of Medicine, Medical College of Wisconsin , Milwaukee, WI 53226 , USA

4. Comprehensive Rodent Metabolic Phenotyping Core, Medical College of Wisconsin , Milwaukee, WI 53226 , USA

5. Department of Occupational and Environmental Health, University of Iowa , Iowa City, IA 52242 , USA

6. Department of Biostatistics, University of Iowa , Iowa City, IA 52242 , USA

7. Department of Biomedical Engineering, Medical College of Wisconsin , Milwaukee, WI 53226 , USA

8. Endocrine Research Laboratory, Aurora St. Luke's Medical Center, Advocate Aurora Research Institute , Milwaukee, WI 53233 , USA

9. Rat Genome Database, Medical College of Wisconsin , Milwaukee, WI 53226 , USA

Abstract

Abstract Metabolic diseases are a host of complex conditions, including obesity, diabetes mellitus, and metabolic syndrome. Endocrine control systems (eg, adrenals, thyroid, gonads) are causally linked to metabolic health outcomes. N/NIH Heterogeneous Stock (HS) rats are a genetically heterogeneous outbred population developed for genetic studies of complex traits. Genetic mapping studies in adult HS rats identified loci associated with cardiometabolic risks, such as glucose intolerance, insulin resistance, and increased body mass index. This study determined underappreciated metabolic health traits and the associated endocrine glands within available substrains of the HS rat founders. We hypothesize that the genetic diversity of the HS rat founder strains causes a range of endocrine health conditions contributing to the diversity of cardiometabolic disease risks. ACI/EurMcwi, BN/NHsdMcwi, BUF/MnaMcwi, F344/StmMcwi, M520/NRrrcMcwi, and WKY/NCrl rats of both sexes were studied from birth until 13 weeks of age. Birth weight was recorded, body weight was measured weekly, metabolic characteristics were assessed, and blood and tissues were collected. Our data show wide variation in endocrine traits and metabolic health states in ACI, BN, BUF, F344, M520, and WKY rat strains. This is the first report to compare birth weight, resting metabolic rate, endocrine gland weight, hypothalamic–pituitary–thyroid axis hormones, and brown adipose tissue weight in these rat strains. Importantly, this work unveils new potential for the HS rat population to model early life adversity and adrenal and thyroid pathophysiology. The HS population likely inherited risk alleles for these strain-specific traits, making the HS rat a powerful model to investigate interventions on endocrine and metabolic health.

Funder

University of Iowa Environmental Health Sciences Research Center

National Institutes of Health Predoctoral Training

National Institutes of Health

Hybrid Rat Diversity Panel

Advocate Aurora Research Institute

Medical College of Wisconsin

Publisher

The Endocrine Society

Subject

Endocrinology

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