A novel mutation in exon 2 of FGB caused by c.221G>T(†) substitution, predicting the replacement of the native Arginine at position 74 with a Leucine (p.Arg74Leu(†)) in a proband from a Kurdish family with dysfibrinogenaemia and familial venous and arterial thrombosis

Dysfibrinogenaemias may present in either congenital or acquired form and are disorders of fibrinogen structure which may or may not be associated with abnormal function. More than 100 point mutations with single amino acid substitutions have been identified in over 400 families. These lead to defec...

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Autores principales: Shlebak, Abdul A., Katsarou, Alexia D., Adams, George, Fernando, Fiona
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer US 2016
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5318484/
https://www.ncbi.nlm.nih.gov/pubmed/27812779
http://dx.doi.org/10.1007/s11239-016-1439-z
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author Shlebak, Abdul A.
Katsarou, Alexia D.
Adams, George
Fernando, Fiona
author_facet Shlebak, Abdul A.
Katsarou, Alexia D.
Adams, George
Fernando, Fiona
author_sort Shlebak, Abdul A.
collection PubMed
description Dysfibrinogenaemias may present in either congenital or acquired form and are disorders of fibrinogen structure which may or may not be associated with abnormal function. More than 100 point mutations with single amino acid substitutions have been identified in over 400 families. These lead to defective DNA in the translated fibrinogen molecule. Such cases have improved our understanding of the fibrinogen–fibrin structure. Six members of a consanguineous family including a female proband, a female sibling, three male siblings and a daughter, with ages between 29 years and 53 years presented with early onset venous and premature arterial thromboembolic disease were investigated for a pro-thrombotic tendency associated with dysfibrinogenaemia. The family was investigated using standard coagulation assays and DNA sequencing of the genes encoding the FGA, FGB and FGG. All cases have dysfibrinogenaemia with a fibrinogen level 1.4 to 1.5 (1.9–4.3 g/L). Thrombophilia testing (including AT, PS & PC, F5 G1691A (FV Leiden)/F2 (prothombin G20210A) genotypes, homocysteine, antiphosphlipid antibody, paroxysmal nocturnal haemoglobinuria by flow cytometry and Janus Kinase-2 (exon 14)) were normal. PCR amplification and sequencing of exon 2 of FBG revealed a heterozygous mutation for a c.221G> T(†)substitution, predicting the replacement of the native Arginine at position 74 with a Leucine (p.Arg74Leu(†)). In silico analysis of p.Arg74Leu strongly support pathogenicity. A novel mutation was identified in exon 2 of FGB caused by c.221G> T(†) substitution, predicting the replacement of Arginine at position 74 with a Leucine (p.Arg74Leu(†)) in a proband from a Kurdish family with dysfibrinogenaemia and familial venous and arterial thrombosis.
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spelling pubmed-53184842017-03-06 A novel mutation in exon 2 of FGB caused by c.221G>T(†) substitution, predicting the replacement of the native Arginine at position 74 with a Leucine (p.Arg74Leu(†)) in a proband from a Kurdish family with dysfibrinogenaemia and familial venous and arterial thrombosis Shlebak, Abdul A. Katsarou, Alexia D. Adams, George Fernando, Fiona J Thromb Thrombolysis Article Dysfibrinogenaemias may present in either congenital or acquired form and are disorders of fibrinogen structure which may or may not be associated with abnormal function. More than 100 point mutations with single amino acid substitutions have been identified in over 400 families. These lead to defective DNA in the translated fibrinogen molecule. Such cases have improved our understanding of the fibrinogen–fibrin structure. Six members of a consanguineous family including a female proband, a female sibling, three male siblings and a daughter, with ages between 29 years and 53 years presented with early onset venous and premature arterial thromboembolic disease were investigated for a pro-thrombotic tendency associated with dysfibrinogenaemia. The family was investigated using standard coagulation assays and DNA sequencing of the genes encoding the FGA, FGB and FGG. All cases have dysfibrinogenaemia with a fibrinogen level 1.4 to 1.5 (1.9–4.3 g/L). Thrombophilia testing (including AT, PS & PC, F5 G1691A (FV Leiden)/F2 (prothombin G20210A) genotypes, homocysteine, antiphosphlipid antibody, paroxysmal nocturnal haemoglobinuria by flow cytometry and Janus Kinase-2 (exon 14)) were normal. PCR amplification and sequencing of exon 2 of FBG revealed a heterozygous mutation for a c.221G> T(†)substitution, predicting the replacement of the native Arginine at position 74 with a Leucine (p.Arg74Leu(†)). In silico analysis of p.Arg74Leu strongly support pathogenicity. A novel mutation was identified in exon 2 of FGB caused by c.221G> T(†) substitution, predicting the replacement of Arginine at position 74 with a Leucine (p.Arg74Leu(†)) in a proband from a Kurdish family with dysfibrinogenaemia and familial venous and arterial thrombosis. Springer US 2016-11-03 2017 /pmc/articles/PMC5318484/ /pubmed/27812779 http://dx.doi.org/10.1007/s11239-016-1439-z Text en © The Author(s) 2016 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.
spellingShingle Article
Shlebak, Abdul A.
Katsarou, Alexia D.
Adams, George
Fernando, Fiona
A novel mutation in exon 2 of FGB caused by c.221G>T(†) substitution, predicting the replacement of the native Arginine at position 74 with a Leucine (p.Arg74Leu(†)) in a proband from a Kurdish family with dysfibrinogenaemia and familial venous and arterial thrombosis
title A novel mutation in exon 2 of FGB caused by c.221G>T(†) substitution, predicting the replacement of the native Arginine at position 74 with a Leucine (p.Arg74Leu(†)) in a proband from a Kurdish family with dysfibrinogenaemia and familial venous and arterial thrombosis
title_full A novel mutation in exon 2 of FGB caused by c.221G>T(†) substitution, predicting the replacement of the native Arginine at position 74 with a Leucine (p.Arg74Leu(†)) in a proband from a Kurdish family with dysfibrinogenaemia and familial venous and arterial thrombosis
title_fullStr A novel mutation in exon 2 of FGB caused by c.221G>T(†) substitution, predicting the replacement of the native Arginine at position 74 with a Leucine (p.Arg74Leu(†)) in a proband from a Kurdish family with dysfibrinogenaemia and familial venous and arterial thrombosis
title_full_unstemmed A novel mutation in exon 2 of FGB caused by c.221G>T(†) substitution, predicting the replacement of the native Arginine at position 74 with a Leucine (p.Arg74Leu(†)) in a proband from a Kurdish family with dysfibrinogenaemia and familial venous and arterial thrombosis
title_short A novel mutation in exon 2 of FGB caused by c.221G>T(†) substitution, predicting the replacement of the native Arginine at position 74 with a Leucine (p.Arg74Leu(†)) in a proband from a Kurdish family with dysfibrinogenaemia and familial venous and arterial thrombosis
title_sort novel mutation in exon 2 of fgb caused by c.221g>t(†) substitution, predicting the replacement of the native arginine at position 74 with a leucine (p.arg74leu(†)) in a proband from a kurdish family with dysfibrinogenaemia and familial venous and arterial thrombosis
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5318484/
https://www.ncbi.nlm.nih.gov/pubmed/27812779
http://dx.doi.org/10.1007/s11239-016-1439-z
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