Very mild disease phenotype of congenic CftrTgH(neoim)Hgu cystic fibrosis mice

Balázs Tóth; Martina Wilke; Frauke Stanke; Martina Dorsch; Silke Jansen; Dirk Wedekind; Nikoletta Charizopoulou; Alice Bot; Marion Burmester; Sabine Leonhard-Marek; Hugo R de Jonge; Hans-Jürgen Hedrich; Gerhard Breves; Burkhard Tümmler

doi:10.1186/1471-2156-9-28

Very mild disease phenotype of congenic CftrTgH(neoim)Hgu cystic fibrosis mice

BMC Genet. 2008 Apr 9:9:28. doi: 10.1186/1471-2156-9-28.

Authors

Balázs Tóth¹, Martina Wilke, Frauke Stanke, Martina Dorsch, Silke Jansen, Dirk Wedekind, Nikoletta Charizopoulou, Alice Bot, Marion Burmester, Sabine Leonhard-Marek, Hugo R de Jonge, Hans-Jürgen Hedrich, Gerhard Breves, Burkhard Tümmler

Affiliation

¹ Klinische Forschergruppe, OE 6710, Medizinische Hochschule Hannover, Carl-Neuberg-Strasse 1, D-30625 Hannover, Germany. balazs_toth@lycos.com

Abstract

Background: A major boost to cystic fibrosis disease research was given by the generation of various mouse models using gene targeting in embryonal stem cells. Moreover, the introduction of the same mutation on different inbred strains generating congenic strains facilitated the search for modifier genes. From the original CftrTgH(neoim)Hgu mouse model with a divergent genetic background (129/Sv, C57BL/6, HsdOla:MF1) two inbred mutant mouse strains CF/1-CftrTgH(neoim)Hgu and CF/3-CftrTgH(neoim)Hgu had been generated using strict brother x sister mating. CF/1-CftrTgH(neoim)Hgu and CF/3-CftrTgH(neoim)Hgu mice were fertile and showed normal growth and lifespan. In this work the CftrTgH(neoim)Hgu insertional mutation was backcrossed from CF/3-CftrTgH(neoim)Hgu onto the inbred backgrounds C57BL/6J and DBA/2J generating congenic animals in order to clarify the differential impact of the Cftr mutation and the genetic background on the disease phenotype of the cystic fibrosis mutant mice. Clinical and electrophysiological features of the two congenic strains were compared with those of CF/1-CftrTgH(neoim)Hgu and CF/3-CftrTgH(neoim)Hgu and wild type controls.

Results: Under the standardized housing conditions of the animal facility, the four mouse strains CF/1-CftrTgH(neoim)Hgu, CF/3-CftrTgH(neoim)Hgu, D2.129P2(CF/3)-CftrTgH(neoim)Hgu and B6.129P2(CF/3)-CftrTgH(neoim)Hgu exhibited normal life expectancy. Growth of congenic cystic fibrosis mice was comparable with that of wild type controls. All mice but D2.129P2(CF/3)-CftrTgH(neoim)Hgu females were fertile. Short circuit current measurements revealed characteristic response profiles of the HsdOla:MF1, DBA/2J and C57BL/6J backgrounds in nose, ileum and colon. All cystic fibrosis mouse lines showed the disease-typical hyperresponsiveness to amiloride in the respiratory epithelium. The mean chloride secretory responses to carbachol or forskolin were 15-100% of those of the cognate wild type control animals.

Conclusion: The amelioration of the clinical features and of the basic defect that had emerged during the generation of CF/3-CftrTgH(neoim)Hgu mice was retained in the congenic mice indicating that the Cftr linkage group or other loci shared between the inbred strains contain(s) the major modifier(s) of attenuation of cystic fibrosis symptoms.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Analysis of Variance
Animals
Body Weight
Carbachol / pharmacology
Chlorides / metabolism
Colforsin / pharmacology
Cystic Fibrosis / genetics*
Cystic Fibrosis / physiopathology
Cystic Fibrosis Transmembrane Conductance Regulator / genetics*
Disease Models, Animal*
Female
Fertility
Genetic Linkage
Genotype
Male
Mice
Mice, Congenic
Mice, Inbred CFTR
Microsatellite Repeats
Phenotype*

Substances

Chlorides
Cystic Fibrosis Transmembrane Conductance Regulator
Colforsin
Carbachol