Thermoneutral Housing Accelerates Metabolic Inflammation to Potentiate Atherosclerosis but Not Insulin Resistance

Tian, Xiaoyu; Ganeshan, Kirthana; Hong, Cynthia; Nguyen, Khoa D.; Qiu, Yifu; Kim, Jason; Tangirala, Rajendra K.; Tontonoz, Peter; Chawla, Ajay

doi:10.1016/j.cmet.2015.10.003

Cited by 120 publications

(116 citation statements)

References 68 publications

Supporting

Mentioning

104

Contrasting

Order By: Relevance

“…Tnfa expression did not increase in mice at 4 or 10 weeks of a HFD (Supplemental Figure 5D). These findings are consistent with previous reports showing that mice develop adipose and systemic insulin resistance within several days to 4 weeks of a HFD (44,45), whereas the number of M1 macrophages in WAT increases only within 8 to 10 weeks of a HFD (10,15,45,46). The finding that HFD-induced insulin resistance precedes the accumulation of M1 macrophages is consistent with our above conclusion that insulin resistance leads to inflammation.…”

Section: Resultssupporting

confidence: 83%

“…However, it has been demonstrated that immunocompromised mice are not protected from systemic insulin resistance induced by a short-term high-fat diet (HFD) (14). Furthermore, Tian et al have shown that adipose tissue inflammation is dispensable for local and systemic insulin resistance (15). Another study has shown that inhibition of adipose tissue inflammation results in glucose intolerance, suggesting that inflammation may even be a mechanism to counter insulin resistance (16).…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Insulin resistance causes inflammation in adipose tissue

Shimobayashi

Albert

Woelnerhanssen³

et al. 2018

Journal of Clinical Investigation

353

232

View full text Add to dashboard Cite

Section: Resultssupporting

confidence: 83%

Section: Introductionmentioning

confidence: 99%

Insulin resistance causes inflammation in adipose tissue

Shimobayashi

Albert

Woelnerhanssen³

et al. 2018

Journal of Clinical Investigation

353

232

View full text Add to dashboard Cite

“…In agreement with our findings and those of others 53 , Tian et al reported improved glucose clearance in mice housed at 30°C. However, they also reported worsened atherosclerosis along with modestly elevated cholesterol, albeit with minimal disease effects at the aortic arch and the most dramatic effects in the descending aorta 22 . Aortic sinus disease, which we quantified in the present study along with aortic disease at multiple time points, was not examined by Tian et al Giles et al failed to find a major shift in plasma cholesterol but nonetheless reported that enhanced atherosclerosis was worsened in Apoe −/− mice fed a high fat diet, but there was no disease change in Apoe −/− mice fed a chow diet.…”

Section: Discussionmentioning

confidence: 98%

“…Yet, some reports indicate that cold temperature, a powerful stimulus for brown and beige fat and UCP1 activation, enhances atherosclerosis 21 . However, other studies suggest that thermoneutral housing at the warm temperature of 30°C—the temperature at which energy expenditure is not needed to maintain body temperature—enhances atherosclerosis 22 . The impact of housing temperature on blood monocyte counts has scarcely been discussed, despite reported connections of sympathetic activation to both beige fat activation and monocytosis, as discussed above.…”

Section: Introductionmentioning

confidence: 99%

Thermoneutrality but Not UCP1 Deficiency Suppresses Monocyte Mobilization Into Blood

Williams

Elvington

Ivanov

et al. 2017

Circulation Research

View full text Add to dashboard Cite

Rationale Ambient temperature is a risk factor for cardiovascular disease. Cold weather increases cardiovascular events, but paradoxically, cold exposure is metabolically protective due to UCP1-dependent thermogenesis. Objective We sought to determine the differential effects of ambient environmental temperature challenge and UCP1 activation in relation to cardiovascular disease progression. Methods and Results Using mouse models of atherosclerosis housed at three different ambient temperatures, we observed that cold temperature enhanced while thermoneutral housing temperature inhibited atherosclerotic plaque growth, as did deficiency in UCP1. However, while UCP1 deficiency promoted poor glucose tolerance, thermoneutral housing enhanced glucose tolerance, and this effect held even in the context of UCP1 deficiency. In conditions of thermoneutrality, but not UCP1 deficiency, circulating monocyte counts were reduced, likely accounting for fewer monocytes entering plaques. Reductions in circulating blood monocytes were also found in a large human cohort in correlation with environmental temperature. By contrast, reduced plaque growth in mice lacking UCP1 was linked to lower cholesterol. Through application of a positron emission tomography (PET) tracer to track CCR2+ cell localization and intravital 2-photon imaging of bone marrow, we associated thermoneutrality with an increased monocyte retention in bone marrow. Pharmacological activation of β3 adrenergic receptors applied to mice housed at thermoneutrality induced UCP1 in beige fat pads but failed to promote monocyte egress from the marrow. Conclusions Warm ambient temperature is, like UCP1 deficiency, atheroprotective, but the mechanisms of action differ. Thermoneutrality associates with reduced monocyte egress from the bone marrow in a UCP-1 dependent manner in mice and likewise may also suppress blood monocyte counts in man.

show abstract

“…116 An emerging consideration is the temperature of the vivarium, which has been demonstrated to alter the development of mouse atherosclerosis. 171,172 Mice are usually housed in rooms that are ~20°C, whereas their thermoneutrality is ~30°C. Although maintaining mice under thermoneutral conditions is not usually practical, these recent publications highlight the need to monitor room temperatures throughout the course of the study.…”

Section: Vivarium Conditionsmentioning

confidence: 99%

Recommendation on Design, Execution, and Reporting of Animal Atherosclerosis Studies: A Scientific Statement From the American Heart Association

Daugherty¹,

Tall²,

Daemen³

et al. 2017

ATVB

288

215

View full text Add to dashboard Cite

Abstract-Animal studies are a foundation for defining mechanisms of atherosclerosis and potential targets of drugs to prevent lesion development or reverse the disease. In the current literature, it is common to see contradictions of outcomes in animal studies from different research groups, leading to the paucity of extrapolations of experimental findings into understanding the human disease. The purpose of this statement is to provide guidelines for development and execution of experimental design and interpretation in animal studies. Recommendations include the following: (1) animal model selection, with commentary on the fidelity of mimicking facets of the human disease; (2) experimental design and its impact on the interpretation of data; and (3) standard methods to enhance accuracy of measurements and characterization of atherosclerotic lesions. (Arterioscler Thromb Vasc Biol. 2017;37:e131-e157.

show abstract

Thermoneutral Housing Accelerates Metabolic Inflammation to Potentiate Atherosclerosis but Not Insulin Resistance

Cited by 120 publications

References 68 publications

Insulin resistance causes inflammation in adipose tissue

Insulin resistance causes inflammation in adipose tissue

Thermoneutrality but Not UCP1 Deficiency Suppresses Monocyte Mobilization Into Blood

Recommendation on Design, Execution, and Reporting of Animal Atherosclerosis Studies: A Scientific Statement From the American Heart Association

Contact Info

Product

Resources

About