ABCC7 p.Glu92Asn

ClinVar: c.274G>T , p.Glu92* D , Pathogenic
c.276A>T , p.Glu92Asp ? , not provided
c.274G>A , p.Glu92Lys D , Pathogenic
CF databases: c.274G>T , p.Glu92* D , CF-causing
c.274G>A , p.Glu92Lys D , CF-causing ; CFTR1: E92K was detected in one Spanish chromosome out of 100 non-[delta]F508 chromosomes studied. The mutation on the other chromosome of this patient is unknown, but has the haplotype C/D. The mutation has been detected by SSCP analysis of exon 4 PCR product using intronic primers. Th ebase change has been confirmed after recovering the mutated strand from the SSCP gel, purified and directly sequenced using an automatic sequencer.
c.276A>T , p.Glu92Asp (CFTR1) ? , The patient carries two other mutations: 3849+10kbC>T and R668C (2134C>T). Although segregation analysis was not performed, we suggest the putative 3849+10kbC>T;R668C/E92D compound genotype in the patient, as we already found the complex allele 3849+10kbC>T;R668C in another patient. Residue E92 is conserved between species but not in other proteins of the CFTR family, where Asp can be found instead. A mild splicing effect of the mutation is also possible.
Predicted by SNAP2: A: D (91%), C: D (95%), D: D (91%), F: D (95%), G: D (95%), H: D (95%), I: D (95%), K: N (53%), L: D (95%), M: D (91%), N: D (95%), P: D (95%), Q: D (85%), R: D (95%), S: D (95%), T: D (95%), V: D (95%), W: D (95%), Y: D (95%),
Predicted by PROVEAN: A: D, C: D, D: N, F: D, G: D, H: D, I: D, K: D, L: D, M: D, N: N, P: D, Q: N, R: D, S: N, T: D, V: D, W: D, Y: D,

[switch to compact view]
Comments [show]
Publications
[hide] El-Seedy A, Girodon E, Norez C, Pajaud J, Pasquet MC, de Becdelievre A, Bienvenu T, des Georges M, Cabet F, Lalau G, Bieth E, Blayau M, Becq F, Kitzis A, Fanen P, Ladeveze V
CFTR mutation combinations producing frequent complex alleles with different clinical and functional outcomes.
Hum Mutat. 2012 Nov;33(11):1557-65. doi: 10.1002/humu.22129. Epub 2012 Jul 2., [PMID:22678879]

Abstract [show]
Comments [show]
Sentences [show]