Glycogen shortage during fasting triggers liver-brain-adipose neurocircuitry to facilitate fat utilization

Yoshihiko Izumida; Naoya Yahagi; Yoshinori Takeuchi; Makiko Nishi; Akito Shikama; Ayako Takarada; Yukari Masuda; Midori Kubota; Takashi Matsuzaka; Yoshimi Nakagawa; Yoko Iizuka; Keiji Itaka; Kazunori Kataoka; Seiji Shioda; Akira Niijima; Tetsuya Yamada; Hideki Katagiri; Ryozo Nagai; Nobuhiro Yamada; Takashi Kadowaki; Hitoshi Shimano

doi:10.1038/ncomms3316

Glycogen shortage during fasting triggers liver-brain-adipose neurocircuitry to facilitate fat utilization

Yoshihiko Izumida, Naoya Yahagi, Yoshinori Takeuchi, Makiko Nishi, Akito Shikama, Ayako Takarada, Yukari Masuda, Midori Kubota, Takashi Matsuzaka, Yoshimi Nakagawa, Yoko Iizuka, Keiji Itaka, Kazunori Kataoka, Seiji Shioda, Akira Niijima, Tetsuya Yamada, Hideki Katagiri, Ryozo Nagai, Nobuhiro Yamada, Takashi KadowakiHitoshi Shimano

MED - Medical Sciences

Research output: Contribution to journal › Article › peer-review

70 Citations (Scopus)

Abstract

During fasting, animals maintain their energy balance by shifting their energy source from carbohydrates to triglycerides. However, the trigger for this switch has not yet been entirely elucidated. Here we show that a selective hepatic vagotomy slows the speed of fat consumption by attenuating sympathetic nerve-mediated lipolysis in adipose tissue. Hepatic glycogen pre-loading by the adenoviral overexpression of glycogen synthase or the transcription factor TFE3 abolished this liver-brain-adipose axis activation. Moreover, the blockade of glycolysis through the knockdown of the glycogen phosphorylase gene and the resulting elevation in the glycogen content abolished the lipolytic signal from the liver, indicating that glycogen is the key to triggering this neurocircuitry. These results demonstrate that liver glycogen shortage activates a liver-brain-adipose neural axis that has an important role in switching the fuel source from glycogen to triglycerides under prolonged fasting conditions.

Original language	English
Article number	2316
Journal	Nature Communications
Volume	4
DOIs	https://doi.org/10.1038/ncomms3316
Publication status	Published - 2013

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Izumida, Y., Yahagi, N., Takeuchi, Y., Nishi, M., Shikama, A., Takarada, A., Masuda, Y., Kubota, M., Matsuzaka, T., Nakagawa, Y., Iizuka, Y., Itaka, K., Kataoka, K., Shioda, S., Niijima, A., Yamada, T., Katagiri, H., Nagai, R., Yamada, N., ... Shimano, H. (2013). Glycogen shortage during fasting triggers liver-brain-adipose neurocircuitry to facilitate fat utilization. Nature Communications, 4, Article 2316. https://doi.org/10.1038/ncomms3316

@article{e304625fbef54a0b953663f99449af8a,

title = "Glycogen shortage during fasting triggers liver-brain-adipose neurocircuitry to facilitate fat utilization",

abstract = "During fasting, animals maintain their energy balance by shifting their energy source from carbohydrates to triglycerides. However, the trigger for this switch has not yet been entirely elucidated. Here we show that a selective hepatic vagotomy slows the speed of fat consumption by attenuating sympathetic nerve-mediated lipolysis in adipose tissue. Hepatic glycogen pre-loading by the adenoviral overexpression of glycogen synthase or the transcription factor TFE3 abolished this liver-brain-adipose axis activation. Moreover, the blockade of glycolysis through the knockdown of the glycogen phosphorylase gene and the resulting elevation in the glycogen content abolished the lipolytic signal from the liver, indicating that glycogen is the key to triggering this neurocircuitry. These results demonstrate that liver glycogen shortage activates a liver-brain-adipose neural axis that has an important role in switching the fuel source from glycogen to triglycerides under prolonged fasting conditions.",

author = "Yoshihiko Izumida and Naoya Yahagi and Yoshinori Takeuchi and Makiko Nishi and Akito Shikama and Ayako Takarada and Yukari Masuda and Midori Kubota and Takashi Matsuzaka and Yoshimi Nakagawa and Yoko Iizuka and Keiji Itaka and Kazunori Kataoka and Seiji Shioda and Akira Niijima and Tetsuya Yamada and Hideki Katagiri and Ryozo Nagai and Nobuhiro Yamada and Takashi Kadowaki and Hitoshi Shimano",

note = "Funding Information: This work was supported by Grants-in-aid from the Ministry of Science, Education, Culture and Technology of Japan (to Y.I. and N.Y.), especially by a MEXT Grant-in-Aid Project (Scientific Research on Innovative Areas) {\textquoteleft}Crosstalk between transcriptional control and energy pathways, mediated by hub metabolites{\textquoteright} (to N.Y.). It was also supported by research Grants from the Uehara Memorial Foundation, ONO Medical Research Foundation, Takeda Science Foundation, Suzuken Memorial Foundation, Japan Heart Foundation, Kanae Foundation for the Promotion of Medical Science, Senri Life Science Foundation, Japan Diabetes Foundation, Japan Foundation for Applied Enzymology and Okinaka Memorial Institute for Medical Research (to N.Y.).",

year = "2013",

doi = "10.1038/ncomms3316",

language = "English",

volume = "4",

journal = "Nature Communications",

issn = "2041-1723",

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Izumida, Y, Yahagi, N, Takeuchi, Y, Nishi, M, Shikama, A, Takarada, A, Masuda, Y, Kubota, M, Matsuzaka, T, Nakagawa, Y, Iizuka, Y, Itaka, K, Kataoka, K, Shioda, S, Niijima, A, Yamada, T, Katagiri, H, Nagai, R, Yamada, N, Kadowaki, T & Shimano, H 2013, 'Glycogen shortage during fasting triggers liver-brain-adipose neurocircuitry to facilitate fat utilization', Nature Communications, vol. 4, 2316. https://doi.org/10.1038/ncomms3316

TY - JOUR

T1 - Glycogen shortage during fasting triggers liver-brain-adipose neurocircuitry to facilitate fat utilization

AU - Izumida, Yoshihiko

AU - Yahagi, Naoya

AU - Takeuchi, Yoshinori

AU - Nishi, Makiko

AU - Shikama, Akito

AU - Takarada, Ayako

AU - Masuda, Yukari

AU - Kubota, Midori

AU - Matsuzaka, Takashi

AU - Nakagawa, Yoshimi

AU - Iizuka, Yoko

AU - Itaka, Keiji

AU - Kataoka, Kazunori

AU - Shioda, Seiji

AU - Niijima, Akira

AU - Yamada, Tetsuya

AU - Katagiri, Hideki

AU - Nagai, Ryozo

AU - Yamada, Nobuhiro

AU - Kadowaki, Takashi

AU - Shimano, Hitoshi

N1 - Funding Information: This work was supported by Grants-in-aid from the Ministry of Science, Education, Culture and Technology of Japan (to Y.I. and N.Y.), especially by a MEXT Grant-in-Aid Project (Scientific Research on Innovative Areas) ‘Crosstalk between transcriptional control and energy pathways, mediated by hub metabolites’ (to N.Y.). It was also supported by research Grants from the Uehara Memorial Foundation, ONO Medical Research Foundation, Takeda Science Foundation, Suzuken Memorial Foundation, Japan Heart Foundation, Kanae Foundation for the Promotion of Medical Science, Senri Life Science Foundation, Japan Diabetes Foundation, Japan Foundation for Applied Enzymology and Okinaka Memorial Institute for Medical Research (to N.Y.).

PY - 2013

Y1 - 2013

N2 - During fasting, animals maintain their energy balance by shifting their energy source from carbohydrates to triglycerides. However, the trigger for this switch has not yet been entirely elucidated. Here we show that a selective hepatic vagotomy slows the speed of fat consumption by attenuating sympathetic nerve-mediated lipolysis in adipose tissue. Hepatic glycogen pre-loading by the adenoviral overexpression of glycogen synthase or the transcription factor TFE3 abolished this liver-brain-adipose axis activation. Moreover, the blockade of glycolysis through the knockdown of the glycogen phosphorylase gene and the resulting elevation in the glycogen content abolished the lipolytic signal from the liver, indicating that glycogen is the key to triggering this neurocircuitry. These results demonstrate that liver glycogen shortage activates a liver-brain-adipose neural axis that has an important role in switching the fuel source from glycogen to triglycerides under prolonged fasting conditions.

AB - During fasting, animals maintain their energy balance by shifting their energy source from carbohydrates to triglycerides. However, the trigger for this switch has not yet been entirely elucidated. Here we show that a selective hepatic vagotomy slows the speed of fat consumption by attenuating sympathetic nerve-mediated lipolysis in adipose tissue. Hepatic glycogen pre-loading by the adenoviral overexpression of glycogen synthase or the transcription factor TFE3 abolished this liver-brain-adipose axis activation. Moreover, the blockade of glycolysis through the knockdown of the glycogen phosphorylase gene and the resulting elevation in the glycogen content abolished the lipolytic signal from the liver, indicating that glycogen is the key to triggering this neurocircuitry. These results demonstrate that liver glycogen shortage activates a liver-brain-adipose neural axis that has an important role in switching the fuel source from glycogen to triglycerides under prolonged fasting conditions.

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U2 - 10.1038/ncomms3316

DO - 10.1038/ncomms3316

M3 - Article

C2 - 23939267

AN - SCOPUS:84883104388

SN - 2041-1723

VL - 4

JO - Nature Communications

JF - Nature Communications

M1 - 2316

ER -

Glycogen shortage during fasting triggers liver-brain-adipose neurocircuitry to facilitate fat utilization

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