Spontaneous rescue from cystic fibrosis in a mouse model

BACKGROUND: From the original Cftr(TgH(neoim)Hgu )mutant mouse model with a divergent genetic background (129P2, C57BL/6, MF1) we have generated two inbred Cftr(TgH(neoim)Hgu )mutant strains named CF/1-Cftr(TgH(neoim)Hgu )and CF/3-Cftr(TgH(neoim)Hgu), which are fertile and show normal growth and lif...

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Autores principales: Charizopoulou, Nikoletta, Wilke, Martina, Dorsch, Martina, Bot, Alice, Jorna, Huub, Jansen, Silke, Stanke, Frauke, Hedrich, Hans J, de Jonge, Hugo R, Tümmler, Burkhard
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2006
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1448185/
https://www.ncbi.nlm.nih.gov/pubmed/16571105
http://dx.doi.org/10.1186/1471-2156-7-18
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author Charizopoulou, Nikoletta
Wilke, Martina
Dorsch, Martina
Bot, Alice
Jorna, Huub
Jansen, Silke
Stanke, Frauke
Hedrich, Hans J
de Jonge, Hugo R
Tümmler, Burkhard
author_facet Charizopoulou, Nikoletta
Wilke, Martina
Dorsch, Martina
Bot, Alice
Jorna, Huub
Jansen, Silke
Stanke, Frauke
Hedrich, Hans J
de Jonge, Hugo R
Tümmler, Burkhard
author_sort Charizopoulou, Nikoletta
collection PubMed
description BACKGROUND: From the original Cftr(TgH(neoim)Hgu )mutant mouse model with a divergent genetic background (129P2, C57BL/6, MF1) we have generated two inbred Cftr(TgH(neoim)Hgu )mutant strains named CF/1-Cftr(TgH(neoim)Hgu )and CF/3-Cftr(TgH(neoim)Hgu), which are fertile and show normal growth and lifespan. Initial genome wide scan analysis with microsatellite markers indicated that the two inbred strains differed on the genetic level. In order to further investigate whether these genetic differences have an impact on the disease phenotype of cystic fibrosis we characterised the phenotype of the two inbred strains. RESULTS: Reduced amounts, compared to wild type control animals, of correctly spliced Cftr mRNA were detected in the nasal epithelia, lungs and the intestine of both inbred Cftr(TgH(neoim)Hgu )strains, with higher residual amount observed for CF/1-Cftr(TgH(neoim)Hgu )than CF/3-Cftr(TgH(neoim)Hgu )for every investigated tissue. Accordingly the amounts of wild type Cftr protein in the intestine were 9% for CF/1-Cftr(TgH(neoim)Hgu )and 4% for CF/3-Cftr(TgH(neoim)Hgu). Unlike the apparent strain and/or tissue specific regulation of Cftr mRNA splicing, short circuit current measurements in the respiratory and intestinal epithelium revealed that both strains have ameliorated the basic defect of cystic fibrosis with a presentation of a normal electrophysiology in both tissues. CONCLUSION: Unlike the outbred Cftr(TgH(neoim)Hgu )insertional mouse model, which displayed the electrophysiological defect in the gastrointestinal and respiratory tracts characteristic of cystic fibrosis, both inbred Cftr(TgH(neoim)Hgu )strains have ameliorated the electrophysiological defect. On the basis of these findings both CF/1-Cftr(TgH(neoim)Hgu )and CF/3-Cftr(TgH(neoim)Hgu )offer an excellent model whereby determination of the minimal levels of protein required for the restoration of the basic defect of cystic fibrosis can be studied, along with the modulating factors which may affect this outcome.
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spelling pubmed-14481852006-04-27 Spontaneous rescue from cystic fibrosis in a mouse model Charizopoulou, Nikoletta Wilke, Martina Dorsch, Martina Bot, Alice Jorna, Huub Jansen, Silke Stanke, Frauke Hedrich, Hans J de Jonge, Hugo R Tümmler, Burkhard BMC Genet Research Article BACKGROUND: From the original Cftr(TgH(neoim)Hgu )mutant mouse model with a divergent genetic background (129P2, C57BL/6, MF1) we have generated two inbred Cftr(TgH(neoim)Hgu )mutant strains named CF/1-Cftr(TgH(neoim)Hgu )and CF/3-Cftr(TgH(neoim)Hgu), which are fertile and show normal growth and lifespan. Initial genome wide scan analysis with microsatellite markers indicated that the two inbred strains differed on the genetic level. In order to further investigate whether these genetic differences have an impact on the disease phenotype of cystic fibrosis we characterised the phenotype of the two inbred strains. RESULTS: Reduced amounts, compared to wild type control animals, of correctly spliced Cftr mRNA were detected in the nasal epithelia, lungs and the intestine of both inbred Cftr(TgH(neoim)Hgu )strains, with higher residual amount observed for CF/1-Cftr(TgH(neoim)Hgu )than CF/3-Cftr(TgH(neoim)Hgu )for every investigated tissue. Accordingly the amounts of wild type Cftr protein in the intestine were 9% for CF/1-Cftr(TgH(neoim)Hgu )and 4% for CF/3-Cftr(TgH(neoim)Hgu). Unlike the apparent strain and/or tissue specific regulation of Cftr mRNA splicing, short circuit current measurements in the respiratory and intestinal epithelium revealed that both strains have ameliorated the basic defect of cystic fibrosis with a presentation of a normal electrophysiology in both tissues. CONCLUSION: Unlike the outbred Cftr(TgH(neoim)Hgu )insertional mouse model, which displayed the electrophysiological defect in the gastrointestinal and respiratory tracts characteristic of cystic fibrosis, both inbred Cftr(TgH(neoim)Hgu )strains have ameliorated the electrophysiological defect. On the basis of these findings both CF/1-Cftr(TgH(neoim)Hgu )and CF/3-Cftr(TgH(neoim)Hgu )offer an excellent model whereby determination of the minimal levels of protein required for the restoration of the basic defect of cystic fibrosis can be studied, along with the modulating factors which may affect this outcome. BioMed Central 2006-03-29 /pmc/articles/PMC1448185/ /pubmed/16571105 http://dx.doi.org/10.1186/1471-2156-7-18 Text en Copyright © 2006 Charizopoulou et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Charizopoulou, Nikoletta
Wilke, Martina
Dorsch, Martina
Bot, Alice
Jorna, Huub
Jansen, Silke
Stanke, Frauke
Hedrich, Hans J
de Jonge, Hugo R
Tümmler, Burkhard
Spontaneous rescue from cystic fibrosis in a mouse model
title Spontaneous rescue from cystic fibrosis in a mouse model
title_full Spontaneous rescue from cystic fibrosis in a mouse model
title_fullStr Spontaneous rescue from cystic fibrosis in a mouse model
title_full_unstemmed Spontaneous rescue from cystic fibrosis in a mouse model
title_short Spontaneous rescue from cystic fibrosis in a mouse model
title_sort spontaneous rescue from cystic fibrosis in a mouse model
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1448185/
https://www.ncbi.nlm.nih.gov/pubmed/16571105
http://dx.doi.org/10.1186/1471-2156-7-18
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