Obesity-associated improvements in metabolic profile through expansion of adipose tissue

Ja Young Kim; Esther Van De Wall; Mathieu Laplante; Anthony Azzara; Maria E. Trujillo; Susanna M. Hofmann; Todd Schraw; Jorge L. Durand; Hua Li; Guangyu Li; Linda A. Jelicks; Mark F. Mehler; David Y. Hui; Yves Deshaies; Gerald I. Shulman; Gary J. Schwartz; Philipp E. Scherer

doi:10.1172/JCI31021

Obesity-associated improvements in metabolic profile through expansion of adipose tissue

Ja Young Kim, Esther Van De Wall, Mathieu Laplante, Anthony Azzara, Maria E. Trujillo, Susanna M. Hofmann, Todd Schraw, Jorge L. Durand, Hua Li, Guangyu Li, Linda A. Jelicks, Mark F. Mehler, David Y. Hui, Yves Deshaies, Gerald I. Shulman, Gary J. Schwartz, Philipp E. Scherer

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1066 Scopus citations

Abstract

Excess caloric intake can lead to insulin resistance. The underlying reasons are complex but likely related to ectopic lipid deposition in nonadipose tissue. We hypothesized that the inability to appropriately expand subcutaneous adipose tissue may be an underlying reason for insulin resistance and β cell failure. Mice lacking leptin while overexpressing adiponectin showed normalized glucose and insulin levels and dramatically improved glucose as well as positively affected serum triglyceride levels. Therefore, modestly increasing the levels of circulating full-length adiponectin completely rescued the diabetic phenotype in ob/ob mice. They displayed increased expression of PPARγ target genes and a reduction in macrophage infiltration in adipose tissue and systemic inflammation. As a result, the transgenic mice were morbidly obese, with significantly higher levels of adipose tissue than their ob/ob littermates, leading to an interesting dichotomy of increased fat mass associated with improvement in insulin sensitivity. Based on these data, we propose that adiponectin acts as a peripheral "starvation" signal promoting the storage of triglycerides preferentially in adipose tissue. As a consequence, reduced triglyceride levels in the liver and muscle convey improved systemic insulin sensitivity. These mice therefore represent what we believe is a novel model of morbid obesity associated with an improved metabolic profile.

Original language	English (US)
Pages (from-to)	2621-2637
Number of pages	17
Journal	Journal of Clinical Investigation
Volume	117
Issue number	9
DOIs	https://doi.org/10.1172/JCI31021
State	Published - Sep 4 2007

ASJC Scopus subject areas

General Medicine

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1172/JCI31021

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Kim, J. Y., Van De Wall, E., Laplante, M., Azzara, A., Trujillo, M. E., Hofmann, S. M., Schraw, T., Durand, J. L., Li, H., Li, G., Jelicks, L. A., Mehler, M. F., Hui, D. Y., Deshaies, Y., Shulman, G. I., Schwartz, G. J., & Scherer, P. E. (2007). Obesity-associated improvements in metabolic profile through expansion of adipose tissue. Journal of Clinical Investigation, 117(9), 2621-2637. https://doi.org/10.1172/JCI31021

Kim, JY, Van De Wall, E, Laplante, M, Azzara, A, Trujillo, ME, Hofmann, SM, Schraw, T, Durand, JL, Li, H, Li, G, Jelicks, LA, Mehler, MF, Hui, DY, Deshaies, Y, Shulman, GI, Schwartz, GJ & Scherer, PE 2007, 'Obesity-associated improvements in metabolic profile through expansion of adipose tissue', Journal of Clinical Investigation, vol. 117, no. 9, pp. 2621-2637. https://doi.org/10.1172/JCI31021

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abstract = "Excess caloric intake can lead to insulin resistance. The underlying reasons are complex but likely related to ectopic lipid deposition in nonadipose tissue. We hypothesized that the inability to appropriately expand subcutaneous adipose tissue may be an underlying reason for insulin resistance and β cell failure. Mice lacking leptin while overexpressing adiponectin showed normalized glucose and insulin levels and dramatically improved glucose as well as positively affected serum triglyceride levels. Therefore, modestly increasing the levels of circulating full-length adiponectin completely rescued the diabetic phenotype in ob/ob mice. They displayed increased expression of PPARγ target genes and a reduction in macrophage infiltration in adipose tissue and systemic inflammation. As a result, the transgenic mice were morbidly obese, with significantly higher levels of adipose tissue than their ob/ob littermates, leading to an interesting dichotomy of increased fat mass associated with improvement in insulin sensitivity. Based on these data, we propose that adiponectin acts as a peripheral {"}starvation{"} signal promoting the storage of triglycerides preferentially in adipose tissue. As a consequence, reduced triglyceride levels in the liver and muscle convey improved systemic insulin sensitivity. These mice therefore represent what we believe is a novel model of morbid obesity associated with an improved metabolic profile.",

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AU - Schraw, Todd

AU - Durand, Jorge L.

AU - Li, Hua

AU - Li, Guangyu

AU - Jelicks, Linda A.

AU - Mehler, Mark F.

AU - Hui, David Y.

AU - Deshaies, Yves

AU - Shulman, Gerald I.

AU - Schwartz, Gary J.

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AB - Excess caloric intake can lead to insulin resistance. The underlying reasons are complex but likely related to ectopic lipid deposition in nonadipose tissue. We hypothesized that the inability to appropriately expand subcutaneous adipose tissue may be an underlying reason for insulin resistance and β cell failure. Mice lacking leptin while overexpressing adiponectin showed normalized glucose and insulin levels and dramatically improved glucose as well as positively affected serum triglyceride levels. Therefore, modestly increasing the levels of circulating full-length adiponectin completely rescued the diabetic phenotype in ob/ob mice. They displayed increased expression of PPARγ target genes and a reduction in macrophage infiltration in adipose tissue and systemic inflammation. As a result, the transgenic mice were morbidly obese, with significantly higher levels of adipose tissue than their ob/ob littermates, leading to an interesting dichotomy of increased fat mass associated with improvement in insulin sensitivity. Based on these data, we propose that adiponectin acts as a peripheral "starvation" signal promoting the storage of triglycerides preferentially in adipose tissue. As a consequence, reduced triglyceride levels in the liver and muscle convey improved systemic insulin sensitivity. These mice therefore represent what we believe is a novel model of morbid obesity associated with an improved metabolic profile.

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Obesity-associated improvements in metabolic profile through expansion of adipose tissue

Abstract

ASJC Scopus subject areas

UN SDGs

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