Cystic fibrosis, also known as mucoviscidosis, is the most frequent severe autosomal recessive genetic disorder in the German-speaking world. In Central Europe, 1 in about 2500 newborns is found to be affected by CF. These children have inherited a defective copy of the mucoviscidosis gene CFTR (cystic fibrosis transmembrane conductance regulator) from both parents.
Cystic fibrosis is a multi-organ disease: all exocrine glands in the body which express the mucoviscidosis gene CFTR are affected. In a typical course of disease, the main symptoms occur already in the earliest stages of childhood. Characteric features are recurrent airway disease, chronic colonization with opportunistic pathogens and a steadily progressive worsening of lung function, which shortens the life expectancy of the patient. Further development of the symptomatic therapies and standardized CF treatment have, in the meantime, increased the average survival time to about 40 years.
The mucoviscidosis gene CFTR codes for a cAMP-dependent chloride and bicarbonate channel in the epithelial cells, which form the outermost cell layer in the lung, the so-called airway epithelium. The ion channel CFTR, is integrated in a multi-layer molecular network of the cell and thus has a regulatory influence on the activity of other ion channels like the sodium channel ENaC.
Innovations in this area include:
The aim of the researchers is to significantly improve the treatment of CF and the quality of life of the affected patients.