Impaired genome maintenance suppresses the growth hormone-insulin-like growth factor 1 axis in mice with cockayne syndrome

Ingrid Van Der Pluijm; George A. Garinis; Renata M.C. Brandt; Theo G.M.F. Gorgels; Susan W. Wijnhoven; Karin E.M. Diderich; Jan De Wit; James R. Mitchell; Conny Van Oostrom; Rudolf Beems; Laura J. Niedernhofer; Susana Velasco; Errol C. Friedberg; Kiyoji Tanaka; Harry Van Steeg; Jan H.J. Hoeijmakers; Gijsbertus T.J. Van Der Horst

doi:10.1371/journal.pbio.0050002

Impaired genome maintenance suppresses the growth hormone-insulin-like growth factor 1 axis in mice with cockayne syndrome

Ingrid Van Der Pluijm
, George A. Garinis
, Renata M.C. Brandt
, Theo G.M.F. Gorgels
, Susan W. Wijnhoven
, Karin E.M. Diderich
, Jan De Wit
, James R. Mitchell
, Conny Van Oostrom
, Rudolf Beems
, Laura J. Niedernhofer
, Susana Velasco
, Errol C. Friedberg
, Kiyoji Tanaka
, Harry Van Steeg
, Jan H.J. Hoeijmakers
, Gijsbertus T.J. Van Der Horst

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

216 Citations (Scopus)

Abstract

Cockayne syndrome (CS) is a photosensitive, DNA repair disorder associated with progeria that is caused by a defect in the transcription-coupled repair subpathway of nucleotide excision repair (NER). Here, complete inactivation of NER in Csb^m/m/Xpa^-/- mutants causes a phenotype that reliably mimics the human progeroid CS syndrome. Newborn Csb^m/m/ Xpa^-/- mice display attenuated growth, progressive neurological dysfunction, retinal degeneration, cachexia, kyphosis, and die before weaning. Mouse liver transcriptome analysis and several physiological endpoints revealed systemic suppression of the growth hormone/insulin-like growth factor 1 (GH/IGF1) somatotroph axis and oxidative metabolism, increased antioxidant responses, and hypoglycemia together with hepatic glycogen and fat accumulation. Broad genome-wide parallels between Csb^m/m/Xpa^-/- and naturally aged mouse liver transcriptomes suggested that these changes are intrinsic to natural ageing and the DNA repair-deficient mice. Importantly, wild-type mice exposed to a low dose of chronic genotoxic stress recapitulated this response, thereby pointing to a novel link between genome instability and the age-related decline of the somatotroph axis.

Original language	English
Pages (from-to)	23-38
Number of pages	16
Journal	PLoS biology
Volume	5
Issue number	1
DOIs	https://doi.org/10.1371/journal.pbio.0050002
Publication status	Published - Jan 2007
Externally published	Yes

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Van Der Pluijm, I., Garinis, G. A., Brandt, R. M. C., Gorgels, T. G. M. F., Wijnhoven, S. W., Diderich, K. E. M., De Wit, J., Mitchell, J. R., Van Oostrom, C., Beems, R., Niedernhofer, L. J., Velasco, S., Friedberg, E. C., Tanaka, K., Van Steeg, H., Hoeijmakers, J. H. J., & Van Der Horst, G. T. J. (2007). Impaired genome maintenance suppresses the growth hormone-insulin-like growth factor 1 axis in mice with cockayne syndrome. PLoS biology, 5(1), 23-38. https://doi.org/10.1371/journal.pbio.0050002

@article{20df6674b512470383c39c11a1059a10,

title = "Impaired genome maintenance suppresses the growth hormone-insulin-like growth factor 1 axis in mice with cockayne syndrome",

abstract = "Cockayne syndrome (CS) is a photosensitive, DNA repair disorder associated with progeria that is caused by a defect in the transcription-coupled repair subpathway of nucleotide excision repair (NER). Here, complete inactivation of NER in Csbm/m/Xpa-/- mutants causes a phenotype that reliably mimics the human progeroid CS syndrome. Newborn Csbm/m/ Xpa-/- mice display attenuated growth, progressive neurological dysfunction, retinal degeneration, cachexia, kyphosis, and die before weaning. Mouse liver transcriptome analysis and several physiological endpoints revealed systemic suppression of the growth hormone/insulin-like growth factor 1 (GH/IGF1) somatotroph axis and oxidative metabolism, increased antioxidant responses, and hypoglycemia together with hepatic glycogen and fat accumulation. Broad genome-wide parallels between Csbm/m/Xpa-/- and naturally aged mouse liver transcriptomes suggested that these changes are intrinsic to natural ageing and the DNA repair-deficient mice. Importantly, wild-type mice exposed to a low dose of chronic genotoxic stress recapitulated this response, thereby pointing to a novel link between genome instability and the age-related decline of the somatotroph axis.",

author = "\{Van Der Pluijm\}, Ingrid and Garinis, \{George A.\} and Brandt, \{Renata M.C.\} and Gorgels, \{Theo G.M.F.\} and Wijnhoven, \{Susan W.\} and Diderich, \{Karin E.M.\} and \{De Wit\}, Jan and Mitchell, \{James R.\} and \{Van Oostrom\}, Conny and Rudolf Beems and Niedernhofer, \{Laura J.\} and Susana Velasco and Friedberg, \{Errol C.\} and Kiyoji Tanaka and \{Van Steeg\}, Harry and Hoeijmakers, \{Jan H.J.\} and \{Van Der Horst\}, \{Gijsbertus T.J.\}",

year = "2007",

month = jan,

doi = "10.1371/journal.pbio.0050002",

language = "English",

volume = "5",

pages = "23--38",

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issn = "1544-9173",

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Van Der Pluijm, I, Garinis, GA, Brandt, RMC, Gorgels, TGMF, Wijnhoven, SW, Diderich, KEM, De Wit, J, Mitchell, JR, Van Oostrom, C, Beems, R, Niedernhofer, LJ, Velasco, S, Friedberg, EC, Tanaka, K, Van Steeg, H, Hoeijmakers, JHJ & Van Der Horst, GTJ 2007, 'Impaired genome maintenance suppresses the growth hormone-insulin-like growth factor 1 axis in mice with cockayne syndrome', PLoS biology, vol. 5, no. 1, pp. 23-38. https://doi.org/10.1371/journal.pbio.0050002

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T1 - Impaired genome maintenance suppresses the growth hormone-insulin-like growth factor 1 axis in mice with cockayne syndrome

AU - Van Der Pluijm, Ingrid

AU - Garinis, George A.

AU - Brandt, Renata M.C.

AU - Gorgels, Theo G.M.F.

AU - Wijnhoven, Susan W.

AU - Diderich, Karin E.M.

AU - De Wit, Jan

AU - Mitchell, James R.

AU - Van Oostrom, Conny

AU - Beems, Rudolf

AU - Niedernhofer, Laura J.

AU - Velasco, Susana

AU - Friedberg, Errol C.

AU - Tanaka, Kiyoji

AU - Van Steeg, Harry

AU - Hoeijmakers, Jan H.J.

AU - Van Der Horst, Gijsbertus T.J.

PY - 2007/1

Y1 - 2007/1

N2 - Cockayne syndrome (CS) is a photosensitive, DNA repair disorder associated with progeria that is caused by a defect in the transcription-coupled repair subpathway of nucleotide excision repair (NER). Here, complete inactivation of NER in Csbm/m/Xpa-/- mutants causes a phenotype that reliably mimics the human progeroid CS syndrome. Newborn Csbm/m/ Xpa-/- mice display attenuated growth, progressive neurological dysfunction, retinal degeneration, cachexia, kyphosis, and die before weaning. Mouse liver transcriptome analysis and several physiological endpoints revealed systemic suppression of the growth hormone/insulin-like growth factor 1 (GH/IGF1) somatotroph axis and oxidative metabolism, increased antioxidant responses, and hypoglycemia together with hepatic glycogen and fat accumulation. Broad genome-wide parallels between Csbm/m/Xpa-/- and naturally aged mouse liver transcriptomes suggested that these changes are intrinsic to natural ageing and the DNA repair-deficient mice. Importantly, wild-type mice exposed to a low dose of chronic genotoxic stress recapitulated this response, thereby pointing to a novel link between genome instability and the age-related decline of the somatotroph axis.

AB - Cockayne syndrome (CS) is a photosensitive, DNA repair disorder associated with progeria that is caused by a defect in the transcription-coupled repair subpathway of nucleotide excision repair (NER). Here, complete inactivation of NER in Csbm/m/Xpa-/- mutants causes a phenotype that reliably mimics the human progeroid CS syndrome. Newborn Csbm/m/ Xpa-/- mice display attenuated growth, progressive neurological dysfunction, retinal degeneration, cachexia, kyphosis, and die before weaning. Mouse liver transcriptome analysis and several physiological endpoints revealed systemic suppression of the growth hormone/insulin-like growth factor 1 (GH/IGF1) somatotroph axis and oxidative metabolism, increased antioxidant responses, and hypoglycemia together with hepatic glycogen and fat accumulation. Broad genome-wide parallels between Csbm/m/Xpa-/- and naturally aged mouse liver transcriptomes suggested that these changes are intrinsic to natural ageing and the DNA repair-deficient mice. Importantly, wild-type mice exposed to a low dose of chronic genotoxic stress recapitulated this response, thereby pointing to a novel link between genome instability and the age-related decline of the somatotroph axis.

UR - https://www.scopus.com/pages/publications/33846030099

U2 - 10.1371/journal.pbio.0050002

DO - 10.1371/journal.pbio.0050002

M3 - Article

C2 - 17326724

AN - SCOPUS:33846030099

SN - 1544-9173

VL - 5

SP - 23

EP - 38

JO - PLoS biology

JF - PLoS biology

IS - 1

ER -

Impaired genome maintenance suppresses the growth hormone-insulin-like growth factor 1 axis in mice with cockayne syndrome

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