What can the CF registry tell us about rare CFTR-mutations? A Belgian study ...

Verfasser:	E. De Wachter M. Thomas S. Wanyama S. Seneca A. Malfroot
Dokumenttyp:	Datenquelle
Erscheinungsdatum:	2017
Verlag/Hrsg.:	Figshare
Schlagwörter:	Biochemistry / Medicine / Microbiology / FOS: Biological sciences / Genetics / Molecular Biology / 39999 Chemical Sciences not elsewhere classified / FOS: Chemical sciences / Sociology / FOS: Sociology / Immunology / FOS: Clinical medicine / Cancer / Hematology / Infectious Diseases / FOS: Health sciences
Sprache:	unknown
Permalink:	https://search.fid-benelux.de/Record/base-28885310
Datenquelle:	BASE; Originalkatalog
Powered By:	BASE
Link(s) :	https://dx.doi.org/10.6084/m9.figshare.c.3860524

Abstract Background CFTR2 provides clinical and functional information of the most common CFTR-mutations. Rare mutations (RMs) occur in only a few patients with limited reported clinical data. Their role in CF-disease liability is hardly documented. Methods Belgian CF-Registry 2013 data were analyzed to identify CF with at least 1 RM (CF+RM). Clinical data and sweat chloride of CF+RM were compared to CF-controls, carrying 2 class 1 to 3 mutations (CFclassic). Disease severity was compared between both groups. To avoid bias in the comparison, transplanted patients were excluded from each group. Results Seventy-seven CF+RM were identified (77/1183 = 6.5%). Sixty-four different RM were detected, of which 21 had not been previously reported. All RMs, corresponding to HGVS (Human Genome Variation Society) nomenclature, were listed in supplementary data. Seven transplanted CF+RM were excluded for further analysis. CF+RM had higher age at diagnosis [median (IQR)] [3.7 y (0.3–18.3) vs. 0.3y (0.1–2,0) (p ...