Severe coagulation factor V deficiency caused by a 4 bp deletion in the factor V gene

Guasch, Joan Francesc; Cannegieter, Suzanne C.; Reitsma, Pieter H.; Veer-Korthof, Elizabeth T. Van 't; Bertina, Rogier M.

doi:10.1046/j.1365-2141.1998.00664.x

Cited by 61 publications

(56 citation statements)

References 42 publications

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“…The remaining exons were amplified by the use of published primer sequences. 11 PCR products purified by ultrafiltration were sequenced by ABI 310 Genetic Analyzer (Applied Biosystems, Foster City, CA).…”

Section: Polymerase Chain Reaction Amplification and Sequencingmentioning

confidence: 99%

“…8,9 More than 200 factor V-deficient cases have been reported in the literature, but the molecular basis for factor V deficiency has been established in only a few cases. [10][11][12][13] Additional molecular defects in the factor V gene have been identified in patients with "pseudohomozygosity" for factor V Leiden (the Leiden allele plus the null allele). These patients may be identified on the basis of thrombotic problems (reviewed in Kane 1 ).…”

Section: Introductionmentioning

confidence: 99%

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Severe coagulation factor V deficiency caused by 2 novel frameshift mutations: 2952delT in exon 13 and 5493insG in exon 16 of factor 5 gene

Ajzner

Balogh

Szabó

et al. 2002

Blood

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Section: Polymerase Chain Reaction Amplification and Sequencingmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Severe coagulation factor V deficiency caused by 2 novel frameshift mutations: 2952delT in exon 13 and 5493insG in exon 16 of factor 5 gene

Ajzner

Balogh

Szabó

et al. 2002

Blood

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“…Despite this important observation, platelet FV is not routinely evaluated in FV-deficient patients and only 3 other studies report platelet FV levels in patients with severe FV deficiency. [32][33][34] No platelet FV antigen or activity could be demonstrated in 2 patients with undetectable plasma FV. 32,33 In another FV-deficient patient, platelet FV could be visualized by Western blotting, but its activity was not determined.…”

Section: Introductionmentioning

confidence: 96%

Residual platelet factor V ensures thrombin generation in patients with severe congenital factor V deficiency and mild bleeding symptoms

Duckers

Simioni

Spiezia

et al. 2010

Blood

120

134

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“…In the proband, we identified 2 novel homozygous genetic alterations and 17 previously described, clinically innocent polymorphisms (Whitehead cSNP database, http://waldo.wi.mit.edu/cvar_snps/). 6,9,10 From the Department of Pathology, Stanford University School of Medicine, and the Department of Pediatric Hematology, University of California at San Francisco. …”

Section: Resultsmentioning

confidence: 99%

Homozygous factor V splice site mutation associated with severe factor V deficiency

Schrijver

Koerper

Jones

et al. 2002

Blood

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We investigated a family whose proband has a severe bleeding disorder and factor V antigenic and functional levels of 8% and less than 1% of control values, respectively. Molecular analysis of the factor V gene revealed a novel homozygous mutation in the last nucleotide of exon 10. 1701G>T causes activation of a cryptic exonic splice site in exon 10, which encodes part of the factor V heavy chain (A2 domain). This leads to the deletion of 35 nucleotides and results in a frameshift with a premature stop codon at amino acid position 498. The G1701 and corresponding Gln509 are conserved in murine, bovine, and porcine factor V and in human factor VIII. Few factor V deficiency mutations have been identified as yet.Several are present in the heterozygous form in combination with factor V Leiden (Arg506Gln). This is the first reported homozygous splice site mutation in a patient with factor V deficiency. IntroductionAutosomal recessive factor V deficiency is a rare coagulation defect, equally affecting both sexes and diagnosed in multiple ethnic backgrounds. 1 In most patients, the phenotype is clinically benign and is characterized by mild bleeding only. [1][2][3][4] The factor V gene is located on chromosome 1q23, 5 spans more than 80 kb, and contains 25 exons. 6 The 5Ј untranslated sequence, a signal peptide, and the factor V heavy chain (protein domains A1 and A2) are encoded by exons 1 to 12. Exon 13 encodes the B domain, which is posttranslationally removed during activation by thrombin. The light chain (protein domains A3, C1, and C2) and the 3Ј untranslated region are encompassed by exons 14 to 25. 6 Few mutations associated with factor V deficiency have been reported. 7 We investigated the genetic basis of factor V deficiency in a patient with umbilical bleeding at birth, gingival bleeding, and repeated spontaneous central nervous system hemorrhage. She requires weekly prophylactic fresh frozen plasma transfusions. The parents may be distantly related. Both parents and the patient's siblings are clinically unaffected. Study designFactor V activity and antigen assays Factor V coagulant activity was determined in the proband and 5 family members ( Figure 1) by a clotting assay using an MLA 1200 instrument (Medical Laboratory Automation, Pleasantville, NY). Factor V antigen concentrations were investigated with a paired antibody enzyme-linked immunosorbent assay as recommended by the manufacturer (Cedarlane Laboratories, Hornby, BC, Canada). Polymerase chain reaction amplification and sequencingGenomic DNA was isolated from the index patient and 5 relatives. Amplification of 24 factor V exons was achieved by the use of intronic primers. Exon 13 was amplified in 7 overlapping segments because of its large size. All primers and polymerase chain reaction (PCR) conditions are available on www.stanford.edu/ϳzehnder.After identification of the 1701GϾT mutation, only RNA from the proband was available for further studies. RNA was extracted from peripheral blood mononuclear cells according to standard procedures. Revers...

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Severe coagulation factor V deficiency caused by a 4 bp deletion in the factor V gene

Cited by 61 publications

References 42 publications

Severe coagulation factor V deficiency caused by 2 novel frameshift mutations: 2952delT in exon 13 and 5493insG in exon 16 of factor 5 gene

Severe coagulation factor V deficiency caused by 2 novel frameshift mutations: 2952delT in exon 13 and 5493insG in exon 16 of factor 5 gene

Residual platelet factor V ensures thrombin generation in patients with severe congenital factor V deficiency and mild bleeding symptoms

Homozygous factor V splice site mutation associated with severe factor V deficiency

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