Glucagon stimulates gluconeogenesis by INSP3R1-mediated hepatic lipolysis

Rachel J. Perry; Dongyan Zhang; Mateus T. Guerra; Allison L. Brill; Leigh Goedeke; Ali R. Nasiri; Aviva Rabin-Court; Yongliang Wang; Liang Peng; Sylvie Dufour; Ye Zhang; Xian Man Zhang; Gina M. Butrico; Keshia Toussaint; Yuichi Nozaki; Gary W. Cline; Kitt Falk Petersen; Michael H. Nathanson; Barbara E. Ehrlich; Gerald I. Shulman

doi:10.1038/s41586-020-2074-6

Glucagon stimulates gluconeogenesis by INSP3R1-mediated hepatic lipolysis

Rachel J. Perry, Dongyan Zhang, Mateus T. Guerra, Allison L. Brill, Leigh Goedeke, Ali R. Nasiri, Aviva Rabin-Court, Yongliang Wang, Liang Peng, Sylvie Dufour, Ye Zhang, Xian Man Zhang, Gina M. Butrico, Keshia Toussaint, Yuichi Nozaki, Gary W. Cline, Kitt Falk Petersen, Michael H. Nathanson, Barbara E. Ehrlich, Gerald I. Shulman

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133 Scopus citations

Abstract

Although it is well-established that reductions in the ratio of insulin to glucagon in the portal vein have a major role in the dysregulation of hepatic glucose metabolism in type-2 diabetes^1–3, the mechanisms by which glucagon affects hepatic glucose production and mitochondrial oxidation are poorly understood. Here we show that glucagon stimulates hepatic gluconeogenesis by increasing the activity of hepatic adipose triglyceride lipase, intrahepatic lipolysis, hepatic acetyl-CoA content and pyruvate carboxylase flux, while also increasing mitochondrial fat oxidation—all of which are mediated by stimulation of the inositol triphosphate receptor 1 (INSP3R1). In rats and mice, chronic physiological increases in plasma glucagon concentrations increased mitochondrial oxidation of fat in the liver and reversed diet-induced hepatic steatosis and insulin resistance. However, these effects of chronic glucagon treatment—reversing hepatic steatosis and glucose intolerance—were abrogated in Insp3r1 (also known as Itpr1)-knockout mice. These results provide insights into glucagon biology and suggest that INSP3R1 may represent a target for therapies that aim to reverse nonalcoholic fatty liver disease and type-2 diabetes.

Original language	English
Pages (from-to)	279-283
Number of pages	5
Journal	Nature
Volume	579
Issue number	7798
DOIs	https://doi.org/10.1038/s41586-020-2074-6
State	Published - 12 Mar 2020
Externally published	Yes

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Perry, R. J., Zhang, D., Guerra, M. T., Brill, A. L., Goedeke, L., Nasiri, A. R., Rabin-Court, A., Wang, Y., Peng, L., Dufour, S., Zhang, Y., Zhang, X. M., Butrico, G. M., Toussaint, K., Nozaki, Y., Cline, G. W., Petersen, K. F., Nathanson, M. H., Ehrlich, B. E., & Shulman, G. I. (2020). Glucagon stimulates gluconeogenesis by INSP3R1-mediated hepatic lipolysis. Nature, 579(7798), 279-283. https://doi.org/10.1038/s41586-020-2074-6

@article{d9a4c620c82a47c9824aff84472b4fe4,

title = "Glucagon stimulates gluconeogenesis by INSP3R1-mediated hepatic lipolysis",

abstract = "Although it is well-established that reductions in the ratio of insulin to glucagon in the portal vein have a major role in the dysregulation of hepatic glucose metabolism in type-2 diabetes1–3, the mechanisms by which glucagon affects hepatic glucose production and mitochondrial oxidation are poorly understood. Here we show that glucagon stimulates hepatic gluconeogenesis by increasing the activity of hepatic adipose triglyceride lipase, intrahepatic lipolysis, hepatic acetyl-CoA content and pyruvate carboxylase flux, while also increasing mitochondrial fat oxidation—all of which are mediated by stimulation of the inositol triphosphate receptor 1 (INSP3R1). In rats and mice, chronic physiological increases in plasma glucagon concentrations increased mitochondrial oxidation of fat in the liver and reversed diet-induced hepatic steatosis and insulin resistance. However, these effects of chronic glucagon treatment—reversing hepatic steatosis and glucose intolerance—were abrogated in Insp3r1 (also known as Itpr1)-knockout mice. These results provide insights into glucagon biology and suggest that INSP3R1 may represent a target for therapies that aim to reverse nonalcoholic fatty liver disease and type-2 diabetes.",

author = "Perry, {Rachel J.} and Dongyan Zhang and Guerra, {Mateus T.} and Brill, {Allison L.} and Leigh Goedeke and Nasiri, {Ali R.} and Aviva Rabin-Court and Yongliang Wang and Liang Peng and Sylvie Dufour and Ye Zhang and Zhang, {Xian Man} and Butrico, {Gina M.} and Keshia Toussaint and Yuichi Nozaki and Cline, {Gary W.} and Petersen, {Kitt Falk} and Nathanson, {Michael H.} and Ehrlich, {Barbara E.} and Shulman, {Gerald I.}",

note = "Publisher Copyright: {\textcopyright} 2020, The Author(s), under exclusive licence to Springer Nature Limited.",

year = "2020",

month = mar,

day = "12",

doi = "10.1038/s41586-020-2074-6",

language = "English",

volume = "579",

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Perry, RJ, Zhang, D, Guerra, MT, Brill, AL, Goedeke, L, Nasiri, AR, Rabin-Court, A, Wang, Y, Peng, L, Dufour, S, Zhang, Y, Zhang, XM, Butrico, GM, Toussaint, K, Nozaki, Y, Cline, GW, Petersen, KF, Nathanson, MH, Ehrlich, BE & Shulman, GI 2020, 'Glucagon stimulates gluconeogenesis by INSP3R1-mediated hepatic lipolysis', Nature, vol. 579, no. 7798, pp. 279-283. https://doi.org/10.1038/s41586-020-2074-6

TY - JOUR

T1 - Glucagon stimulates gluconeogenesis by INSP3R1-mediated hepatic lipolysis

AU - Perry, Rachel J.

AU - Zhang, Dongyan

AU - Guerra, Mateus T.

AU - Brill, Allison L.

AU - Goedeke, Leigh

AU - Nasiri, Ali R.

AU - Rabin-Court, Aviva

AU - Wang, Yongliang

AU - Peng, Liang

AU - Dufour, Sylvie

AU - Zhang, Ye

AU - Zhang, Xian Man

AU - Butrico, Gina M.

AU - Toussaint, Keshia

AU - Nozaki, Yuichi

AU - Cline, Gary W.

AU - Petersen, Kitt Falk

AU - Nathanson, Michael H.

AU - Ehrlich, Barbara E.

AU - Shulman, Gerald I.

PY - 2020/3/12

Y1 - 2020/3/12

N2 - Although it is well-established that reductions in the ratio of insulin to glucagon in the portal vein have a major role in the dysregulation of hepatic glucose metabolism in type-2 diabetes1–3, the mechanisms by which glucagon affects hepatic glucose production and mitochondrial oxidation are poorly understood. Here we show that glucagon stimulates hepatic gluconeogenesis by increasing the activity of hepatic adipose triglyceride lipase, intrahepatic lipolysis, hepatic acetyl-CoA content and pyruvate carboxylase flux, while also increasing mitochondrial fat oxidation—all of which are mediated by stimulation of the inositol triphosphate receptor 1 (INSP3R1). In rats and mice, chronic physiological increases in plasma glucagon concentrations increased mitochondrial oxidation of fat in the liver and reversed diet-induced hepatic steatosis and insulin resistance. However, these effects of chronic glucagon treatment—reversing hepatic steatosis and glucose intolerance—were abrogated in Insp3r1 (also known as Itpr1)-knockout mice. These results provide insights into glucagon biology and suggest that INSP3R1 may represent a target for therapies that aim to reverse nonalcoholic fatty liver disease and type-2 diabetes.

AB - Although it is well-established that reductions in the ratio of insulin to glucagon in the portal vein have a major role in the dysregulation of hepatic glucose metabolism in type-2 diabetes1–3, the mechanisms by which glucagon affects hepatic glucose production and mitochondrial oxidation are poorly understood. Here we show that glucagon stimulates hepatic gluconeogenesis by increasing the activity of hepatic adipose triglyceride lipase, intrahepatic lipolysis, hepatic acetyl-CoA content and pyruvate carboxylase flux, while also increasing mitochondrial fat oxidation—all of which are mediated by stimulation of the inositol triphosphate receptor 1 (INSP3R1). In rats and mice, chronic physiological increases in plasma glucagon concentrations increased mitochondrial oxidation of fat in the liver and reversed diet-induced hepatic steatosis and insulin resistance. However, these effects of chronic glucagon treatment—reversing hepatic steatosis and glucose intolerance—were abrogated in Insp3r1 (also known as Itpr1)-knockout mice. These results provide insights into glucagon biology and suggest that INSP3R1 may represent a target for therapies that aim to reverse nonalcoholic fatty liver disease and type-2 diabetes.

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DO - 10.1038/s41586-020-2074-6

M3 - Article

C2 - 32132708

AN - SCOPUS:85081039349

SN - 0028-0836

VL - 579

SP - 279

EP - 283

JO - Nature

JF - Nature

IS - 7798

ER -

Glucagon stimulates gluconeogenesis by INSP3R1-mediated hepatic lipolysis

Abstract

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