Literature DB >> 18097769

Systemic overexpression of growth hormone (GH) in transgenic FVB/N inbred mice: an optimized model for holistic studies of molecular mechanisms underlying GH-induced kidney pathology.

Dagmar C von Waldthausen1, Marlon R Schneider, Ingrid Renner-Müller, Dirk N Rauleder, Nadja Herbach, Bernhard Aigner, Rüdiger Wanke, Eckhard Wolf.   

Abstract

Transgenic mice overexpressing growth hormone (GH) display a plethora of phenotypic alterations and provide unique models for studying and influencing consequences of chronic GH excess. Since the first report on GH transgenic mice was published in 1982, many different mouse models overexpressing GH from various species at different levels and with different tissue specificities were established, most of them on random-bred or hybrid genetic background. We have generated a new transgenic mouse model on FVB/N inbred background, expressing bovine (b) GH under the control of the chicken beta-actin promoter (cbetaa). cbetaa-bGH transgenic mice exhibit ubiquitous expression of bGH mRNA and protein and circulating bGH levels in the range of several microg/ml, resulting in markedly stimulated growth and the characteristic spectrum of pathological lesions which were described in previous GH overexpressing mouse models. Importantly, a consistent sequence of renal alterations is observed, mimicking progressive kidney disease in human patients. The novel, genetically standardized GH transgenic mouse model is ideal for holistic transcriptome and proteome studies aiming at the identification of the molecular mechanisms underlying GH-induced pathological alterations especially in the kidney. Moreover, genetically defined cbetaa-bGH mice facilitate random mutagenesis screens for modifier genes which influence the effects of chronic GH excess and associated pathological lesions.

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Year:  2007        PMID: 18097769     DOI: 10.1007/s11248-007-9163-2

Source DB:  PubMed          Journal:  Transgenic Res        ISSN: 0962-8819            Impact factor:   2.788


  44 in total

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Authors:  E J H Schenck; C L Brooks
Journal:  Exp Biol Med (Maywood)       Date:  2006-03

10.  Genotype-specific environmental impact on the variance of blood values in inbred and F1 hybrid mice.

Authors:  Martina Klempt; Birgit Rathkolb; Edith Fuchs; Martin Hrabé de Angelis; Eckhard Wolf; Bernhard Aigner
Journal:  Mamm Genome       Date:  2006-02-07       Impact factor: 2.957

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  4 in total

1.  Expression of functional recombinant human growth hormone in transgenic soybean seeds.

Authors:  Nicolau B Cunha; André M Murad; Thaís M Cipriano; Ana Cláudia G Araújo; Francisco J L Aragão; Adilson Leite; Giovanni R Vianna; Timothy R McPhee; Gustavo H M F Souza; Michael J Waters; Elíbio L Rech
Journal:  Transgenic Res       Date:  2010-11-11       Impact factor: 2.788

2.  Metabolic adaptation of short-living growth hormone transgenic mice to methionine restriction and supplementation.

Authors:  Holly M Brown-Borg; Sharlene Rakoczy; Joseph A Wonderlich; Kurt E Borg; Lalida Rojanathammanee
Journal:  Ann N Y Acad Sci       Date:  2018-04       Impact factor: 5.691

3.  Growth hormone signaling is necessary for lifespan extension by dietary methionine.

Authors:  Holly M Brown-Borg; Sharlene G Rakoczy; Joseph A Wonderlich; Lalida Rojanathammanee; John J Kopchick; Vanessa Armstrong; Debbie Raasakka
Journal:  Aging Cell       Date:  2014-09-19       Impact factor: 9.304

4.  Growth hormone (GH)-transgenic insulin-like growth factor 1 (IGF1)-deficient mice allow dissociation of excess GH and IGF1 effects on glomerular and tubular growth.

Authors:  Andreas Blutke; Marlon R Schneider; Eckhard Wolf; Rüdiger Wanke
Journal:  Physiol Rep       Date:  2016-03
  4 in total

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