Nuclear SREBP-1a causes loss of pancreatic β-cells and impaired insulin secretion

Yuko Iwasaki; Hitoshi Iwasaki; Shigeru Yatoh; Mayumi Ishikawa; Toyonori Kato; Takashi Matsuzaka; Yoshimi Nakagawa; Naoya Yahagi; Kazuto Kobayashi; Akimitsu Takahashi; Hiroaki Suzuki; Nobuhiro Yamada; Hitoshi Shimano

doi:10.1016/j.bbrc.2008.11.105

Nuclear SREBP-1a causes loss of pancreatic β-cells and impaired insulin secretion

Yuko Iwasaki, Hitoshi Iwasaki, Shigeru Yatoh, Mayumi Ishikawa, Toyonori Kato, Takashi Matsuzaka, Yoshimi Nakagawa, Naoya Yahagi, Kazuto Kobayashi, Akimitsu Takahashi, Hiroaki Suzuki, Nobuhiro Yamada, Hitoshi Shimano^*

^*この論文の責任著者

和漢医薬学総合研究所研究開発部門複雑系解析分野

研究成果: ジャーナルへの寄稿 › 学術論文 › 査読

16 被引用数 (Scopus)

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Transgenic mice expressing nuclear sterol regulatory element-binding protein-1a under the control of the insulin promoter were generated to determine the role of SREBP-1a in pancreatic β-cells. Only low expressors could be established, which exhibited mild hyperglycemia, impaired glucose tolerance, and reduced plasma insulin levels compared to C57BL/6 controls. The islets isolated from the transgenic mice were fewer and smaller, and had decreased insulin content and unaltered glucagon staining. Both glucose- and potassium-stimulated insulin secretions were decreased. The transgenic islets consistently expressed genes for fatty acids and cholesterol synthesis, resulting in accumulation of triglycerides but not cholesterol. PDX-1, ΒΕΤΑ2, MafA, and IRS-2 were suppressed, partially explaining the loss and dysfunction of β-cell mass. The transgenic mice on a high fat/high sucrose diet still exhibited impaired insulin secretion and continuous β-cell growth defect. Therefore, nuclear SREBP-1a, even at a low level, strongly disrupts β-cell mass and function.

本文言語	英語
ページ（範囲）	545-550
ページ数	6
ジャーナル	Biochemical and Biophysical Research Communications
巻	378
号	3
DOI	https://doi.org/10.1016/j.bbrc.2008.11.105
出版ステータス	出版済み - 2009/01/16

ASJC Scopus 主題領域

生物理学
生化学
分子生物学
細胞生物学

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10.1016/j.bbrc.2008.11.105

引用スタイル

Iwasaki, Y., Iwasaki, H., Yatoh, S., Ishikawa, M., Kato, T., Matsuzaka, T., Nakagawa, Y., Yahagi, N., Kobayashi, K., Takahashi, A., Suzuki, H., Yamada, N., & Shimano, H. (2009). Nuclear SREBP-1a causes loss of pancreatic β-cells and impaired insulin secretion. Biochemical and Biophysical Research Communications, 378(3), 545-550. https://doi.org/10.1016/j.bbrc.2008.11.105

@article{63bc47d4ce214fb490f0c8c477d3fc03,

title = "Nuclear SREBP-1a causes loss of pancreatic β-cells and impaired insulin secretion",

abstract = "Transgenic mice expressing nuclear sterol regulatory element-binding protein-1a under the control of the insulin promoter were generated to determine the role of SREBP-1a in pancreatic β-cells. Only low expressors could be established, which exhibited mild hyperglycemia, impaired glucose tolerance, and reduced plasma insulin levels compared to C57BL/6 controls. The islets isolated from the transgenic mice were fewer and smaller, and had decreased insulin content and unaltered glucagon staining. Both glucose- and potassium-stimulated insulin secretions were decreased. The transgenic islets consistently expressed genes for fatty acids and cholesterol synthesis, resulting in accumulation of triglycerides but not cholesterol. PDX-1, ΒΕΤΑ2, MafA, and IRS-2 were suppressed, partially explaining the loss and dysfunction of β-cell mass. The transgenic mice on a high fat/high sucrose diet still exhibited impaired insulin secretion and continuous β-cell growth defect. Therefore, nuclear SREBP-1a, even at a low level, strongly disrupts β-cell mass and function.",

keywords = "Cholesterol, Lipotoxicity, Sterol regulatory element-binding protein, Transcription factors, Triglycerides",

author = "Yuko Iwasaki and Hitoshi Iwasaki and Shigeru Yatoh and Mayumi Ishikawa and Toyonori Kato and Takashi Matsuzaka and Yoshimi Nakagawa and Naoya Yahagi and Kazuto Kobayashi and Akimitsu Takahashi and Hiroaki Suzuki and Nobuhiro Yamada 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. ",

year = "2009",

month = jan,

day = "16",

doi = "10.1016/j.bbrc.2008.11.105",

language = "英語",

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Iwasaki, Y, Iwasaki, H, Yatoh, S, Ishikawa, M, Kato, T, Matsuzaka, T, Nakagawa, Y, Yahagi, N, Kobayashi, K, Takahashi, A, Suzuki, H, Yamada, N & Shimano, H 2009, 'Nuclear SREBP-1a causes loss of pancreatic β-cells and impaired insulin secretion', Biochemical and Biophysical Research Communications, vol. 378, no. 3, pp. 545-550. https://doi.org/10.1016/j.bbrc.2008.11.105

TY - JOUR

T1 - Nuclear SREBP-1a causes loss of pancreatic β-cells and impaired insulin secretion

AU - Iwasaki, Yuko

AU - Iwasaki, Hitoshi

AU - Yatoh, Shigeru

AU - Ishikawa, Mayumi

AU - Kato, Toyonori

AU - Matsuzaka, Takashi

AU - Nakagawa, Yoshimi

AU - Yahagi, Naoya

AU - Kobayashi, Kazuto

AU - Takahashi, Akimitsu

AU - Suzuki, Hiroaki

AU - Yamada, Nobuhiro

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.

PY - 2009/1/16

Y1 - 2009/1/16

N2 - Transgenic mice expressing nuclear sterol regulatory element-binding protein-1a under the control of the insulin promoter were generated to determine the role of SREBP-1a in pancreatic β-cells. Only low expressors could be established, which exhibited mild hyperglycemia, impaired glucose tolerance, and reduced plasma insulin levels compared to C57BL/6 controls. The islets isolated from the transgenic mice were fewer and smaller, and had decreased insulin content and unaltered glucagon staining. Both glucose- and potassium-stimulated insulin secretions were decreased. The transgenic islets consistently expressed genes for fatty acids and cholesterol synthesis, resulting in accumulation of triglycerides but not cholesterol. PDX-1, ΒΕΤΑ2, MafA, and IRS-2 were suppressed, partially explaining the loss and dysfunction of β-cell mass. The transgenic mice on a high fat/high sucrose diet still exhibited impaired insulin secretion and continuous β-cell growth defect. Therefore, nuclear SREBP-1a, even at a low level, strongly disrupts β-cell mass and function.

AB - Transgenic mice expressing nuclear sterol regulatory element-binding protein-1a under the control of the insulin promoter were generated to determine the role of SREBP-1a in pancreatic β-cells. Only low expressors could be established, which exhibited mild hyperglycemia, impaired glucose tolerance, and reduced plasma insulin levels compared to C57BL/6 controls. The islets isolated from the transgenic mice were fewer and smaller, and had decreased insulin content and unaltered glucagon staining. Both glucose- and potassium-stimulated insulin secretions were decreased. The transgenic islets consistently expressed genes for fatty acids and cholesterol synthesis, resulting in accumulation of triglycerides but not cholesterol. PDX-1, ΒΕΤΑ2, MafA, and IRS-2 were suppressed, partially explaining the loss and dysfunction of β-cell mass. The transgenic mice on a high fat/high sucrose diet still exhibited impaired insulin secretion and continuous β-cell growth defect. Therefore, nuclear SREBP-1a, even at a low level, strongly disrupts β-cell mass and function.

KW - Cholesterol

KW - Lipotoxicity

KW - Sterol regulatory element-binding protein

KW - Transcription factors

KW - Triglycerides

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SP - 545

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JO - Biochemical and Biophysical Research Communications

JF - Biochemical and Biophysical Research Communications

IS - 3

ER -

Nuclear SREBP-1a causes loss of pancreatic β-cells and impaired insulin secretion

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