Ultraviolet radiation suppresses obesity and symptoms of metabolic syndrome independently of vitamin d in mice fed a high-fat diet.
Ultraviolet radiation suppresses obesity and symptoms of metabolic syndrome independently of vitamin d in mice fed a high-fat diet.
The role of vitamin D in curtailing the development of obesity and comorbidities such as the metabolic syndrome (MetS) and type 2 diabetes has received much attention recently. However, clinical trials have failed to conclusively demonstrate the benefits of vitamin D supplementation. In most studies, serum 25-hydroxyvitamin D [25(OH)D] decreases with increasing BMI above normal weight. These low 25(OH)D levels may also be a proxy for reduced exposure to sunlight-derived ultraviolet radiation (UVR). Here we investigate whether UVR and/or vitamin D supplementation modifies the development of obesity and type 2 diabetes in a murine model of obesity. Long-term suberythemal and erythemal UVR significantly suppressed weight gain, glucose intolerance, insulin resistance, nonalcoholic fatty liver disease measures; and serum levels of fasting insulin, glucose, and cholesterol in C57BL/6 male mice fed a high-fat diet. However, many of the benefits of UVR were not reproduced by vitamin D supplementation. In further mechanistic studies, skin induction of the UVR-induced mediator nitric oxide (NO) reproduced many of the effects of UVR. These studies suggest that UVR (sunlight exposure) may be an effective means of suppressing the development of obesity and MetS, through mechanisms that are independent of vitamin D but dependent on other UVR-induced mediators such as NO.
3759-3769
Geldenhuys, Sian
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Hart, Prue H.
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Endersby, Raelene
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Jacoby, Peter
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Feelisch, Martin
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Weller, Richard B.
6760c78a-63ae-484a-affa-b435f146e5a3
Matthews, Vance
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Gorman, Shelley
011f6b03-7b50-4c96-ab5e-9b0f6cc5c25d
November 2014
Geldenhuys, Sian
4dfa56a3-86c9-402c-b657-add282277771
Hart, Prue H.
30c350e2-ec01-48e9-8c5e-9ada39ab17ef
Endersby, Raelene
ea43e747-5bb8-4888-bfff-91e11131f30b
Jacoby, Peter
482b2b8c-81f4-4289-8f78-a453ad56b420
Feelisch, Martin
8c1b9965-8614-4e85-b2c6-458a2e17eafd
Weller, Richard B.
6760c78a-63ae-484a-affa-b435f146e5a3
Matthews, Vance
1c6c377d-081f-40c4-9c80-000553fd9e32
Gorman, Shelley
011f6b03-7b50-4c96-ab5e-9b0f6cc5c25d
Geldenhuys, Sian, Hart, Prue H., Endersby, Raelene, Jacoby, Peter, Feelisch, Martin, Weller, Richard B., Matthews, Vance and Gorman, Shelley
(2014)
Ultraviolet radiation suppresses obesity and symptoms of metabolic syndrome independently of vitamin d in mice fed a high-fat diet.
Diabetes, 63 (11), .
(doi:10.2337/db13-1675).
(PMID:25342734)
Abstract
The role of vitamin D in curtailing the development of obesity and comorbidities such as the metabolic syndrome (MetS) and type 2 diabetes has received much attention recently. However, clinical trials have failed to conclusively demonstrate the benefits of vitamin D supplementation. In most studies, serum 25-hydroxyvitamin D [25(OH)D] decreases with increasing BMI above normal weight. These low 25(OH)D levels may also be a proxy for reduced exposure to sunlight-derived ultraviolet radiation (UVR). Here we investigate whether UVR and/or vitamin D supplementation modifies the development of obesity and type 2 diabetes in a murine model of obesity. Long-term suberythemal and erythemal UVR significantly suppressed weight gain, glucose intolerance, insulin resistance, nonalcoholic fatty liver disease measures; and serum levels of fasting insulin, glucose, and cholesterol in C57BL/6 male mice fed a high-fat diet. However, many of the benefits of UVR were not reproduced by vitamin D supplementation. In further mechanistic studies, skin induction of the UVR-induced mediator nitric oxide (NO) reproduced many of the effects of UVR. These studies suggest that UVR (sunlight exposure) may be an effective means of suppressing the development of obesity and MetS, through mechanisms that are independent of vitamin D but dependent on other UVR-induced mediators such as NO.
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2014 Geldenhuys Diabetes for ePrints.pdf
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Published date: November 2014
Organisations:
Clinical & Experimental Sciences
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Local EPrints ID: 370461
URI: http://eprints.soton.ac.uk/id/eprint/370461
ISSN: 0012-1797
PURE UUID: f0fa2378-fd3d-4857-86d2-05c1e148a671
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Date deposited: 29 Oct 2014 13:22
Last modified: 15 Mar 2024 03:42
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Author:
Sian Geldenhuys
Author:
Prue H. Hart
Author:
Raelene Endersby
Author:
Peter Jacoby
Author:
Richard B. Weller
Author:
Vance Matthews
Author:
Shelley Gorman
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