Is the activated partial thromboplastin time suitable to screen for von Willebrand factor deficiencies?

Lippi, Giuseppe; Franchini, Massimo; Poli, Giovanni; Salvagno, Gian Luca; Montagnana, Martina; Guidi, Gian Cesare

doi:10.1097/mbc.0b013e32810fd872

Cited by 6 publications

(7 citation statements)

References 16 publications

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“…The association between cortisol and von Willebrand factor reported by von Känel et al is not necessary in disagreement with our findings, since APTT is a global coagulation test, which might be shortened not only by elevated levels of von Willebrand factor, but also by an increased activity of a variety of additional coagulation factors, such as VIII, IX and XI [4,5]. Moreover, although reduced levels of von Willebrand factor in plasma produce a prolonged APTT values [6], there is no conclusive evidence that increased levels might be associated with a shortened coagulation time.…”

Section: ó Springer Science+business Media Llc 2007contrasting

confidence: 76%

Higher morning serum cortisol level predicts increased fibrinogen but not shortened APTT

Lippi

Franchini

Salvagno

et al. 2007

J Thromb Thrombolysis

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Section: ó Springer Science+business Media Llc 2007contrasting

confidence: 76%

Higher morning serum cortisol level predicts increased fibrinogen but not shortened APTT

Lippi

Franchini

Salvagno

et al. 2007

J Thromb Thrombolysis

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“…The diagnosis of VWD requires clinical and laboratory components: a personal history of excessive mucocutaneous bleeding, a family history of excessive bleeding, and a laboratory evaluation. Besides the laboratory screening tests for VWD [closure time with PFA‐100™ (Siemens Healthcare Diagnostics, Marburg, Germany), platelet count and activated partial thromboplastin time (APTT)] more specific assays are required to diagnose VWD . Confirmatory laboratory tests include measurement of FVIII coagulant activity (FVIII:C), the VWF antigen (VWF:Ag), and the activity of the VWF, as up to 30% of cases have a qualitative type 2 defect .…”

Section: Introductionmentioning

confidence: 99%

Validation of a new panel of automated chemiluminescence assays for von Willebrand factor antigen and activity in the screening for von Willebrand disease

Verfaillie

Witte

Devreese

2013

Int J Lab Hematology

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“…von Willebrand disease, caused by vWF deficiency, is a common genetic disease and can prolong the aPTT (21). rs2229446 is a non-synonymous variant of VWF (Arg2185Gln), and its minor allele (T) was associated with lower vWF and factor VIII activity levels in the AA cohort from the NHLBI Exome Sequencing Project (22).…”

Section: Discussionmentioning

confidence: 99%

A genetic association study of activated partial thromboplastin time in European Americans and African Americans: the ARIC Study

Weng

Cushman

Pankow

et al. 2014

Human Molecular Genetics

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Reduced activated partial thromboplastin time (aPTT) is a risk marker for incident and recurrent venous thromboembolism (VTE). Genetic factors influencing aPTT are not well understood, especially in populations of non-European ancestry. The present study aimed to identify aPTT-related gene variants in both European Americans (EAs) and African Americans (AAs). We conducted a genetic association study for aPTT in 9719 EAs and 2799 AAs from the Atherosclerosis Risk in Communities (ARIC) study. Using the Candidate Gene Association Resource (CARe) consortium candidate gene array, the analyses were based on ∼50 000 SNPs in ∼2000 candidate genes. In EAs, the analyses identified a new independent association for aPTT in F5 (rs2239852, P-value = 1.9 × 10(-8)), which clusters with a coding variant rs6030 (P-value = 7.8 × 10(-7)). The remaining significant signals were located on F5, HRG, KNG1, F11, F12 and ABO and have been previously reported in EA populations. In AAs, significant signals were identified in KNG1, HRG, F12, ABO and VWF, with the leading variants in KNG1, HRG and F12 being the same as in the EAs; the significant variant in VWF (rs2229446, P-value = 1.2 × 10(-6)) was specific to the AA sample (minor allele frequency = 19% in AAs and 0.2% in EAs) and has not been previously reported. This is the first study to report aPTT-related genetic variants in AAs. Our findings in AAs demonstrate transferability of previously reported associations with KNG1, HRG and F12 in EAs. We also identified new associations at F5 in EAs and VWF in AAs that have not been previously reported for aPTT.

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Is the activated partial thromboplastin time suitable to screen for von Willebrand factor deficiencies?

Cited by 6 publications

References 16 publications

Higher morning serum cortisol level predicts increased fibrinogen but not shortened APTT

Higher morning serum cortisol level predicts increased fibrinogen but not shortened APTT

Validation of a new panel of automated chemiluminescence assays for von Willebrand factor antigen and activity in the screening for von Willebrand disease

A genetic association study of activated partial thromboplastin time in European Americans and African Americans: the ARIC Study

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