Multiple developmental defects derived from impaired recruitment of ASC-2 to nuclear receptors in mice: Implication for posterior lenticonus with cataract

Seung Whan Kim; Cheolho Cheong; Young Chang Sohn; Young Hwa Goo; Wan Je Oh; Jung Hwan Park; So Young Joe; Hyen Sam Kang; Duk Kyung Kim; Changwon Kee; Jae Woon Lee; Han Woong Lee

doi:10.1128/MCB.22.24.8409-8414.2002

Multiple developmental defects derived from impaired recruitment of ASC-2 to nuclear receptors in mice: Implication for posterior lenticonus with cataract

Seung Whan Kim
, Cheolho Cheong
, Young Chang Sohn
, Young Hwa Goo
, Wan Je Oh
, Jung Hwan Park
, So Young Joe
, Hyen Sam Kang
, Duk Kyung Kim
, Changwon Kee
, Jae Woon Lee
, Han Woong Lee

Biological Sciences

Pohang University of Science and Technology
Seoul National University
Sungkyunkwan University
Sungkyunkwan University

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

28 Scopus citations

Abstract

ASC-2, a recently isolated transcriptional coactivator molecule, stimulates transactivation by multiple transcription factors, including nuclear receptors. We generated a potent dominant negative fragment of ASC-2, encompassing the N-terminal LXXLL motif that binds a broad range of nuclear receptors. This fragment, termed DN1, specifically inhibited endogenous ASC-2 from binding these receptors in vivo, whereas DN1/m, in which the LXXLL motif was mutated to LXXAA to abolish the receptor interactions, was inert. Interestingly, DN1 transgenic mice but not DN1/m transgenic mice exhibited severe microphthalmia and posterior lenticonus with cataract as well as a variety of pathophysiological phenotypes in many other organs. Our results provide a novel insight into the molecular and histopathological mechanism of posterior lenticonus with cataract and attest to the importance of ASC-2 as a pivotal transcriptional coactivator of nuclear receptors in vivo.

Original language	English
Pages (from-to)	8409-8414
Number of pages	6
Journal	Molecular and Cellular Biology
Volume	22
Issue number	24
DOIs	https://doi.org/10.1128/MCB.22.24.8409-8414.2002
State	Published - Dec 2002

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Kim, S. W., Cheong, C., Sohn, Y. C., Goo, Y. H., Oh, W. J., Park, J. H., Joe, S. Y., Kang, H. S., Kim, D. K., Kee, C., Lee, J. W., & Lee, H. W. (2002). Multiple developmental defects derived from impaired recruitment of ASC-2 to nuclear receptors in mice: Implication for posterior lenticonus with cataract. Molecular and Cellular Biology, 22(24), 8409-8414. https://doi.org/10.1128/MCB.22.24.8409-8414.2002

@article{a2b4f4d4fa674468a225921971f4606f,

title = "Multiple developmental defects derived from impaired recruitment of ASC-2 to nuclear receptors in mice: Implication for posterior lenticonus with cataract",

abstract = "ASC-2, a recently isolated transcriptional coactivator molecule, stimulates transactivation by multiple transcription factors, including nuclear receptors. We generated a potent dominant negative fragment of ASC-2, encompassing the N-terminal LXXLL motif that binds a broad range of nuclear receptors. This fragment, termed DN1, specifically inhibited endogenous ASC-2 from binding these receptors in vivo, whereas DN1/m, in which the LXXLL motif was mutated to LXXAA to abolish the receptor interactions, was inert. Interestingly, DN1 transgenic mice but not DN1/m transgenic mice exhibited severe microphthalmia and posterior lenticonus with cataract as well as a variety of pathophysiological phenotypes in many other organs. Our results provide a novel insight into the molecular and histopathological mechanism of posterior lenticonus with cataract and attest to the importance of ASC-2 as a pivotal transcriptional coactivator of nuclear receptors in vivo.",

author = "Kim, \{Seung Whan\} and Cheolho Cheong and Sohn, \{Young Chang\} and Goo, \{Young Hwa\} and Oh, \{Wan Je\} and Park, \{Jung Hwan\} and Joe, \{So Young\} and Kang, \{Hyen Sam\} and Kim, \{Duk Kyung\} and Changwon Kee and Lee, \{Jae Woon\} and Lee, \{Han Woong\}",

year = "2002",

month = dec,

doi = "10.1128/MCB.22.24.8409-8414.2002",

language = "English",

volume = "22",

pages = "8409--8414",

journal = "Molecular and Cellular Biology",

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Kim, SW, Cheong, C, Sohn, YC, Goo, YH, Oh, WJ, Park, JH, Joe, SY, Kang, HS, Kim, DK, Kee, C, Lee, JW & Lee, HW 2002, 'Multiple developmental defects derived from impaired recruitment of ASC-2 to nuclear receptors in mice: Implication for posterior lenticonus with cataract', Molecular and Cellular Biology, vol. 22, no. 24, pp. 8409-8414. https://doi.org/10.1128/MCB.22.24.8409-8414.2002

TY - JOUR

T1 - Multiple developmental defects derived from impaired recruitment of ASC-2 to nuclear receptors in mice

T2 - Implication for posterior lenticonus with cataract

AU - Kim, Seung Whan

AU - Cheong, Cheolho

AU - Sohn, Young Chang

AU - Goo, Young Hwa

AU - Oh, Wan Je

AU - Park, Jung Hwan

AU - Joe, So Young

AU - Kang, Hyen Sam

AU - Kim, Duk Kyung

AU - Kee, Changwon

AU - Lee, Jae Woon

AU - Lee, Han Woong

PY - 2002/12

Y1 - 2002/12

N2 - ASC-2, a recently isolated transcriptional coactivator molecule, stimulates transactivation by multiple transcription factors, including nuclear receptors. We generated a potent dominant negative fragment of ASC-2, encompassing the N-terminal LXXLL motif that binds a broad range of nuclear receptors. This fragment, termed DN1, specifically inhibited endogenous ASC-2 from binding these receptors in vivo, whereas DN1/m, in which the LXXLL motif was mutated to LXXAA to abolish the receptor interactions, was inert. Interestingly, DN1 transgenic mice but not DN1/m transgenic mice exhibited severe microphthalmia and posterior lenticonus with cataract as well as a variety of pathophysiological phenotypes in many other organs. Our results provide a novel insight into the molecular and histopathological mechanism of posterior lenticonus with cataract and attest to the importance of ASC-2 as a pivotal transcriptional coactivator of nuclear receptors in vivo.

AB - ASC-2, a recently isolated transcriptional coactivator molecule, stimulates transactivation by multiple transcription factors, including nuclear receptors. We generated a potent dominant negative fragment of ASC-2, encompassing the N-terminal LXXLL motif that binds a broad range of nuclear receptors. This fragment, termed DN1, specifically inhibited endogenous ASC-2 from binding these receptors in vivo, whereas DN1/m, in which the LXXLL motif was mutated to LXXAA to abolish the receptor interactions, was inert. Interestingly, DN1 transgenic mice but not DN1/m transgenic mice exhibited severe microphthalmia and posterior lenticonus with cataract as well as a variety of pathophysiological phenotypes in many other organs. Our results provide a novel insight into the molecular and histopathological mechanism of posterior lenticonus with cataract and attest to the importance of ASC-2 as a pivotal transcriptional coactivator of nuclear receptors in vivo.

UR - https://www.scopus.com/pages/publications/18744403340

U2 - 10.1128/MCB.22.24.8409-8414.2002

DO - 10.1128/MCB.22.24.8409-8414.2002

M3 - Article

C2 - 12446761

AN - SCOPUS:18744403340

SN - 0270-7306

VL - 22

SP - 8409

EP - 8414

JO - Molecular and Cellular Biology

JF - Molecular and Cellular Biology

IS - 24

ER -

Multiple developmental defects derived from impaired recruitment of ASC-2 to nuclear receptors in mice: Implication for posterior lenticonus with cataract

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