Regulation of insulin secretion and β-cell mass by activating signal cointegrator 2

Seon Yong Yeom; Geun Hyang Kim; Chan Hee Kim; Heun Don Jung; So Yeon Kim; Joong Yeol Park; Youngmi Kim Pak; Dong Kwon Rhee; Shao Qing Kuang; Jianming Xu; Duck Jong Han; Dae Kyu Song; Jae Woon Lee; Ki Up Lee; Seung Whan Kim

doi:10.1128/MCB.01412-05

Regulation of insulin secretion and β-cell mass by activating signal cointegrator 2

Seon Yong Yeom, Geun Hyang Kim, Chan Hee Kim, Heun Don Jung, So Yeon Kim, Joong Yeol Park, Youngmi Kim Pak, Dong Kwon Rhee, Shao Qing Kuang, Jianming Xu, Duck Jong Han, Dae Kyu Song, Jae Woon Lee, Ki Up Lee, Seung Whan Kim

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

17 Scopus citations

Abstract

Activating signal cointegrator 2 (ASC-2) is a transcriptional coactivator of many nuclear receptors (NRs) and other transcription factors and contains two NR-interacting LXXLL motifs (NR boxes). In the pancreas, ASC-2 is expressed only in the endocrine cells of the islets of Langerhans, but not in the exocrine cells. Thus, we examined the potential role of ASC-2 in insulin secretion from pancreatic β-cells. Overexpressed ASC-2 increased glucose-elicited insulin secretion, whereas insulin secretion was decreased in islets from ASC-2 ^+/- mice. DN1 and DN2 are two dominant-negative fragments of ASC-2 that contain NR boxes 1 and 2, respectively, and block the interactions of cognate NRs with the endogenous ASC-2. Primary rat islets ectopically expressing DN1 or DN2 exhibited decreased insulin secretion. Furthermore, relative to the wild type, ASC-2^+/- mice showed reduced islet mass and number, which correlated with increased apoptosis and decreased proliferation of ASC-2 ^+/- islets. These results suggest that ASC-2 regulates insulin secretion and β-cell survival and that the regulatory role of ASC-2 in insulin secretion appears to involve, at least in part, its interaction with NRs via its two NR boxes.

Original language	English (US)
Pages (from-to)	4553-4563
Number of pages	11
Journal	Molecular and cellular biology
Volume	26
Issue number	12
DOIs	https://doi.org/10.1128/MCB.01412-05
State	Published - Jun 2006
Externally published	Yes

ASJC Scopus subject areas

Molecular Biology
Cell Biology

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title = "Regulation of insulin secretion and β-cell mass by activating signal cointegrator 2",

abstract = "Activating signal cointegrator 2 (ASC-2) is a transcriptional coactivator of many nuclear receptors (NRs) and other transcription factors and contains two NR-interacting LXXLL motifs (NR boxes). In the pancreas, ASC-2 is expressed only in the endocrine cells of the islets of Langerhans, but not in the exocrine cells. Thus, we examined the potential role of ASC-2 in insulin secretion from pancreatic β-cells. Overexpressed ASC-2 increased glucose-elicited insulin secretion, whereas insulin secretion was decreased in islets from ASC-2 +/- mice. DN1 and DN2 are two dominant-negative fragments of ASC-2 that contain NR boxes 1 and 2, respectively, and block the interactions of cognate NRs with the endogenous ASC-2. Primary rat islets ectopically expressing DN1 or DN2 exhibited decreased insulin secretion. Furthermore, relative to the wild type, ASC-2+/- mice showed reduced islet mass and number, which correlated with increased apoptosis and decreased proliferation of ASC-2 +/- islets. These results suggest that ASC-2 regulates insulin secretion and β-cell survival and that the regulatory role of ASC-2 in insulin secretion appears to involve, at least in part, its interaction with NRs via its two NR boxes.",

author = "Yeom, {Seon Yong} and Kim, {Geun Hyang} and Kim, {Chan Hee} and Jung, {Heun Don} and Kim, {So Yeon} and Park, {Joong Yeol} and Pak, {Youngmi Kim} and Rhee, {Dong Kwon} and Kuang, {Shao Qing} and Jianming Xu and Han, {Duck Jong} and Song, {Dae Kyu} and Lee, {Jae Woon} and Lee, {Ki Up} and Kim, {Seung Whan}",

year = "2006",

month = jun,

doi = "10.1128/MCB.01412-05",

language = "English (US)",

volume = "26",

pages = "4553--4563",

journal = "Molecular and cellular biology",

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AU - Yeom, Seon Yong

AU - Kim, Geun Hyang

AU - Kim, Chan Hee

AU - Jung, Heun Don

AU - Kim, So Yeon

AU - Park, Joong Yeol

AU - Pak, Youngmi Kim

AU - Rhee, Dong Kwon

AU - Kuang, Shao Qing

AU - Xu, Jianming

AU - Han, Duck Jong

AU - Song, Dae Kyu

AU - Lee, Jae Woon

AU - Lee, Ki Up

AU - Kim, Seung Whan

PY - 2006/6

Y1 - 2006/6

N2 - Activating signal cointegrator 2 (ASC-2) is a transcriptional coactivator of many nuclear receptors (NRs) and other transcription factors and contains two NR-interacting LXXLL motifs (NR boxes). In the pancreas, ASC-2 is expressed only in the endocrine cells of the islets of Langerhans, but not in the exocrine cells. Thus, we examined the potential role of ASC-2 in insulin secretion from pancreatic β-cells. Overexpressed ASC-2 increased glucose-elicited insulin secretion, whereas insulin secretion was decreased in islets from ASC-2 +/- mice. DN1 and DN2 are two dominant-negative fragments of ASC-2 that contain NR boxes 1 and 2, respectively, and block the interactions of cognate NRs with the endogenous ASC-2. Primary rat islets ectopically expressing DN1 or DN2 exhibited decreased insulin secretion. Furthermore, relative to the wild type, ASC-2+/- mice showed reduced islet mass and number, which correlated with increased apoptosis and decreased proliferation of ASC-2 +/- islets. These results suggest that ASC-2 regulates insulin secretion and β-cell survival and that the regulatory role of ASC-2 in insulin secretion appears to involve, at least in part, its interaction with NRs via its two NR boxes.

AB - Activating signal cointegrator 2 (ASC-2) is a transcriptional coactivator of many nuclear receptors (NRs) and other transcription factors and contains two NR-interacting LXXLL motifs (NR boxes). In the pancreas, ASC-2 is expressed only in the endocrine cells of the islets of Langerhans, but not in the exocrine cells. Thus, we examined the potential role of ASC-2 in insulin secretion from pancreatic β-cells. Overexpressed ASC-2 increased glucose-elicited insulin secretion, whereas insulin secretion was decreased in islets from ASC-2 +/- mice. DN1 and DN2 are two dominant-negative fragments of ASC-2 that contain NR boxes 1 and 2, respectively, and block the interactions of cognate NRs with the endogenous ASC-2. Primary rat islets ectopically expressing DN1 or DN2 exhibited decreased insulin secretion. Furthermore, relative to the wild type, ASC-2+/- mice showed reduced islet mass and number, which correlated with increased apoptosis and decreased proliferation of ASC-2 +/- islets. These results suggest that ASC-2 regulates insulin secretion and β-cell survival and that the regulatory role of ASC-2 in insulin secretion appears to involve, at least in part, its interaction with NRs via its two NR boxes.

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Regulation of insulin secretion and β-cell mass by activating signal cointegrator 2

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