ABCC7 p.Gly194Arg
[switch to full view]Comments [show]
None has been submitted yet.
PMID: 17003641
[PubMed]
Keiles S et al: "Identification of CFTR, PRSS1, and SPINK1 mutations in 381 patients with pancreatitis."
No.
Sentence
Comment
4
Results: The results identified 32% (122/381) of patients with 166 mutant CFTR alleles, including 12 novel CFTR variants: 4375-20 A9G, F575Y, K598E, L1260P, G194R, F834L, S573C, 2789 +17 C9T, 621+83 A9G, T164S, 621+25 A9G, and 3500-19 G9A.
X
ABCC7 p.Gly194Arg 17003641:4:157
status: NEW54 Patients With More Than 1 CFTR Mutation CFTR Mutation 1 CFTR Mutation 2 CFTR Mutation 3 No. of Patients deltaF508 5T 3 deltaF508 D1152H 1 deltaF508 deltaF508 1 deltaF508 F575Y 1 deltaF508 K598E 1 deltaF508 T164S 1 deltaF508 R74W D1270N 1 deltaF508 Q1476X 1 deltaF508 L997F 1 R553X D1152H 1 R553X G1069R 1 2789+5 G9A 2183 AA9G 1 3849+10kb C9T L1260P 1 711+3 A to G I1139V 1 1341+1 G9A G194R 5T 1 621+25 A9G 3500-19 C9T 1 R74W V855I 1 G542X R117H 1 G551D F311L 1 G576A R668C 2 K710X L997F 1 L997F L320V 1 G1069R 5T 1 1818+18 G9A 5T 1 F1074L 5T 1 F834L 5T 1 R74Q R297Q 1 R74Q R297Q 5T 1 R785Q 5T 1 R117H 5T 3 deltaF508 I1027T 1 Total patients 36 MutationsinboldfacewouldnothavebeendetectedbytheAmericanCollegeofObstetrics and Gynecology (ACOG)/American College of Medical Genetics (ACMG) mutation panel.
X
ABCC7 p.Gly194Arg 17003641:54:384
status: NEW74 G194R A 4-month-old African-American female infant with acute pancreatitis has a G9A transversion at nucleotide position 712. This variation changes a glycine to an arginine at codon 194 within exon 6a of the CFTR gene. This patient also carries a 1341+1 G9A mutation and a 5T variant in intron 8.
X
ABCC7 p.Gly194Arg 17003641:74:0
status: NEW76 However, a G9T substitution at nucleotide position 713 results in a deleterious mutation G194V.29 We have also reported the G194R, 1341+1 G9A, and 5T variants in another African-American patient with CF from the same city.
X
ABCC7 p.Gly194Arg 17003641:76:124
status: NEW
No.
Sentence
Comment
53
Interpretation of Mutations Requires an Understanding of Their Functional Consequences Mutation group Reported mutations Complex allele: These mutations are recognized to occur on a single allele R117H ϩ T G576A ϩ R668C F508del ϩ I1027T Benign sequence alterations: These mutations have no known clinical consequence R74Q R297Q R74W 621 * 25 AϾG 3500-19 CϾT T164S C855I I1139V CFTR-related disorder associated: These mutations have been described in individuals with CF-like single organ disease (such as pancreatitis, sinopulmonary disease, or obstructive azoospermia), but do not fulfill the diagnostic criteria for CF 5T R117H D1270N L320V Q1352H 1818-18 GϾA S1235R CF causing F508del Q1476X R553X K710X G542X G551D F311L 2789-5 GϾA 2183AAϾG 711ϩ3 AϾG 3849ϩ10kb CϾT 1341ϩ1GϾA D1152Ha F1074La R553X Unknown clinical consequence F575Y L1260P G194R G1069R L997F K598E F834L R785Q To illustrate this point, mutations identified by extensive mutation testing in a cohort of patients with recurrent acute or chronic pancre- atitis14 are listed according to their clinical consequences (based on current consensus guidelines13 and functional and/or clinical reports; available: http://www.genet.sickkids.on.ca).
X
ABCC7 p.Gly194Arg 20416310:53:927
status: NEW