Literature DB >> 19887571

Different degrees of somatotroph ablation compromise pituitary growth hormone cell network structure and other pituitary endocrine cell types.

Eleanor Waite1, Chrystel Lafont, Danielle Carmignac, Norbert Chauvet, Nathalie Coutry, Helen Christian, Iain Robinson, Patrice Mollard, Paul Le Tissier.   

Abstract

We have generated transgenic mice with somatotroph-specific expression of a modified influenza virus ion channel, (H37A)M2, leading to ablation of GH cells with three levels of severity, dependent on transgene copy number. GH-M2(low) mice grow normally and have normal-size pituitaries but 40-50% reduction in pituitary GH content in adult animals. GH-M2(med) mice have male-specific transient growth retardation and a reduction in pituitary GH content by 75% at 42 d and 97% by 100 d. GH-M2(high) mice are severely dwarfed with undetectable pituitary GH. The GH secretory response of GH-M2(low) and GH-M2(med) mice to GH-releasing peptide-6 and GHRH was markedly attenuated. The content of other pituitary hormones was affected depending on transgene copy number: no effect in GH-M2(low) mice, prolactin and TSH reduced in GH-M2(med) mice, and all hormones reduced in GH-M2(high) mice. The effect on non-GH hormone content was associated with increased macrophage invasion of the pituitary. Somatotroph ablation affected GH cell network organization with limited disruption in GH-M2(low) mice but more severe disruption in GH-M2(med) mice. The remaining somatotrophs formed tight clusters after puberty, which contrasts with GHRH-M2 mice with a secondary reduction in somatotrophs that do not form clusters. A reduction in pituitary beta-catenin staining was correlated with GH-M2 transgene copy number, suggesting M2 expression has an effect on cell-cell communication in somatotrophs and other pituitary cell types. GH-M2 transgenic mice demonstrate that differing degrees of somatotroph ablation lead to correlated secondary effects on cell populations and cellular network organization.

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Year:  2009        PMID: 19887571     DOI: 10.1210/en.2009-0539

Source DB:  PubMed          Journal:  Endocrinology        ISSN: 0013-7227            Impact factor:   4.736


  11 in total

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Journal:  Proc Natl Acad Sci U S A       Date:  2011-07-11       Impact factor: 11.205

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4.  PROP1-Dependent Retinoic Acid Signaling Regulates Developmental Pituitary Morphogenesis and Hormone Expression.

Authors:  Leonard Y M Cheung; Sally A Camper
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5.  Loss of basal and TRH-stimulated Tshb expression in dispersed pituitary cells.

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Journal:  Endocrinology       Date:  2015-01       Impact factor: 4.736

6.  Dmrt5 controls corticotrope and gonadotrope differentiation in the zebrafish pituitary.

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7.  Pituitary growth hormone network responses are sexually dimorphic and regulated by gonadal steroids in adulthood.

Authors:  Claudia Sanchez-Cardenas; Pierre Fontanaud; Zhenhe He; Chrystel Lafont; Anne-Cécile Meunier; Marie Schaeffer; Danielle Carmignac; François Molino; Nathalie Coutry; Xavier Bonnefont; Laurie-Anne Gouty-Colomer; Elodie Gavois; David J Hodson; Paul Le Tissier; Iain C A F Robinson; Patrice Mollard
Journal:  Proc Natl Acad Sci U S A       Date:  2010-11-22       Impact factor: 11.205

8.  Pituitary phenotypes of mice lacking the notch signalling ligand delta-like 1 homologue.

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9.  Loss of Foxm1 Results in Reduced Somatotrope Cell Number during Mouse Embryogenesis.

Authors:  Michael J Calderon; Adam G Ploegman; Brock Bailey; Deborah O Jung; Amy M Navratil; Buffy S Ellsworth
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Review 10.  Functional Pituitary Networks in Vertebrates.

Authors:  Yorgui Santiago-Andres; Matan Golan; Tatiana Fiordelisio
Journal:  Front Endocrinol (Lausanne)       Date:  2021-01-27       Impact factor: 5.555

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