Voluntary Running Aids to Maintain High Body Temperature in Rats Bred for High Aerobic Capacity

Overview

Journal Front Physiol

Date 2016 Aug 10

PMID 27504097

Citations 7

Authors

Sira M Karvinen

Mika Silvennoinen

Hongqiang Ma

Timo Tormakangas

Timo Rantalainen

Rita Rinnankoski-Tuikka

Sanna Lensu

Lauren G Koch

Steven L Britton

Heikki Kainulainen

Affiliations

Soon will be listed here.

Abstract

The production of heat, i.e., thermogenesis, is a significant component of the metabolic rate, which in turn affects weight gain and health. Thermogenesis is linked to physical activity (PA) level. However, it is not known whether intrinsic exercise capacity, aging, and long-term voluntary running affect core body temperature. Here we use rat models selectively bred to differ in maximal treadmill endurance running capacity (Low capacity runners, LCR and High capacity Runners, HCR), that as adults are divergent for aerobic exercise capacity, aging, and metabolic disease risk to study the connection between PA and body temperature. Ten high capacity runner (HCR) and ten low capacity runner (LCR) female rats were studied between 9 and 21 months of age. Rectal body temperature of HCR and LCR rats was measured before and after 1-year voluntary running/control intervention to explore the effects of aging and PA. Also, we determined whether injected glucose and spontaneous activity affect the body temperature differently between LCR and HCR rats at 9 vs. 21 months of age. HCRs had on average 1.3°C higher body temperature than LCRs (p < 0.001). Aging decreased the body temperature level of HCRs to similar levels with LCRs. The opportunity to run voluntarily had a significant impact on the body temperature of HCRs (p < 0.001) allowing them to maintain body temperature at a similar level as when at younger age. Compared to LCRs, HCRs were spontaneously more active, had higher relative gastrocnemius muscle mass and higher UCP2, PGC-1α, cyt c, and OXPHOS levels in the skeletal muscle (p < 0.050). These results suggest that higher PA level together with greater relative muscle mass and higher mitochondrial content/function contribute to the accumulation of heat in the HCRs. Interestingly, neither aging nor voluntary training had a significant impact on core body temperature of LCRs. However, glucose injection resulted in a lowering of the body temperature of LCRs (p < 0.050), but not that of HCRs. In conclusion, rats born with high intrinsic capacity for aerobic exercise and better health have higher body temperature compared to rats born with low exercise capacity and disease risk. Voluntary running allowed HCRs to maintain high body temperature during aging, which suggests that high PA level was crucial in maintaining the high body temperature of HCRs.

Citing Articles

Intrinsic cardiorespiratory fitness modulates clinical and molecular response to caloric restriction.

Fleischman J, Qi N, Treutelaar M, Britton S, Koch L, Li J Mol Metab. 2023; 68:101668.

PMID: 36642218 PMC: 9938335. DOI: 10.1016/j.molmet.2023.101668.

Altered skeletal muscle sarco-endoplasmic reticulum Ca-ATPase calcium transport efficiency after a thermogenic stimulus.

Heemstra L, Koch L, Britton S, Novak C Am J Physiol Regul Integr Comp Physiol. 2022; 323(5):R628-R637.

PMID: 36094445 PMC: 9602703. DOI: 10.1152/ajpregu.00173.2022.

Interactive effects of aging and aerobic capacity on energy metabolism-related metabolites of serum, skeletal muscle, and white adipose tissue.

Zhuang H, Karvinen S, Tormakangas T, Zhang X, Ojanen X, Velagapudi V Geroscience. 2021; 43(6):2679-2691.

PMID: 34089174 PMC: 8602622. DOI: 10.1007/s11357-021-00387-1.

Enhanced weight and fat loss from long-term intermittent fasting in obesity-prone, low-fitness rats.

Smyers M, Koch L, Britton S, Wagner J, Novak C Physiol Behav. 2020; 230:113280.

PMID: 33285179 PMC: 7856160. DOI: 10.1016/j.physbeh.2020.113280.

Intrinsic High Aerobic Capacity in Male Rats Protects Against Diet-Induced Insulin Resistance.

Morris E, Meers G, Ruegsegger G, Wankhade U, Robinson T, Koch L Endocrinology. 2019; 160(5):1179-1192.

PMID: 31144719 PMC: 6482035. DOI: 10.1210/en.2019-00118.

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