2015
DOI: 10.1586/17474086.2015.1039978
|View full text |Cite
|
Sign up to set email alerts
|

Detection of mild inherited disorders of blood coagulation: current options and personal recommendations

Abstract: Although assessment of prior personal and familial bleeding history is an important aspect of the diagnosis of bleeding disorders, patients with mild inherited bleeding disorders are sometimes clinically asymptomatic until presented with a hemostatic challenge. However, bleeding may occur after incursion of trauma or surgery, so detection of these conditions reflects an important facet of clinical and laboratory practice. Mild bleeding disorders may be detected as a result of family studies or following identi… Show more

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
2
1
1
1

Citation Types

0
24
0

Year Published

2016
2016
2023
2023

Publication Types

Select...
4
3

Relationship

2
5

Authors

Journals

citations
Cited by 28 publications
(24 citation statements)
references
References 106 publications
(124 reference statements)
0
24
0
Order By: Relevance
“…These tests can then be either manually or automatically activated (eg by adopting specific rules in the software of the analyzers) within the laboratory, on the same plasma sample used for routine analyses, should this be permitted in a given jurisdiction or by the local health care provider. On the other hand, normal routine coagulation tests do not necessarily exclude a bleeding disorder, and abnormal test results do not necessarily reflect a bleeding disorder . Indeed, most “abnormal” coagulation tests in normal laboratory practice probably reflect either anticoagulation therapy (heparin, vitamin K antagonists and increasingly the direct anti‐thrombin or anti‐Xa anticoagulants), or “benign” deficiencies of FXII, or other nonhaemorrhagic conditions such as lupus anticoagulants .…”
Section: Initial Limited Clinical Requests As An Important Consideratmentioning
confidence: 99%
See 3 more Smart Citations
“…These tests can then be either manually or automatically activated (eg by adopting specific rules in the software of the analyzers) within the laboratory, on the same plasma sample used for routine analyses, should this be permitted in a given jurisdiction or by the local health care provider. On the other hand, normal routine coagulation tests do not necessarily exclude a bleeding disorder, and abnormal test results do not necessarily reflect a bleeding disorder . Indeed, most “abnormal” coagulation tests in normal laboratory practice probably reflect either anticoagulation therapy (heparin, vitamin K antagonists and increasingly the direct anti‐thrombin or anti‐Xa anticoagulants), or “benign” deficiencies of FXII, or other nonhaemorrhagic conditions such as lupus anticoagulants .…”
Section: Initial Limited Clinical Requests As An Important Consideratmentioning
confidence: 99%
“…Normal screening test results will not necessarily exclude a bleeding disorder, and abnormal screening test results will not necessarily confirm a bleeding disorder. Screening tests are not sensitive to all bleeding disorders (FXIII deficiency is probably the most paradigmatic example), and abnormal test results may result as such for a variety of reasons …”
Section: Initial Limited Clinical Requests As An Important Consideratmentioning
confidence: 99%
See 2 more Smart Citations
“…The essential function of these proteins is to prevent undue (or excess) activation of hemostasis, so that deficiencies of these natural anticoagulants are now clearly recognized as powerful risk factors for venous thrombosis. 5 FVIII deficiency (i.e., hemophilia A) and FIX deficiency (i.e., hemophilia B) are the most prevalent inherited disorders of secondary hemostasis (i.e., $1:5,000 and $1:50,000, respectively), whereas other coagulation factor deficiencies are conventionally called "rare disorders" since they usually affect fewer than 200,000 subjects, 6 with the exception of von Willebrand disease (VWD), exhibiting an overall frequency close to that of hemophilia A (i.e., $1:10,000). 7 The activity of VWF cannot be clearly confined within the boundaries of primary or secondary hemostasis (VWF promotes platelet aggregation, a primary hemostasis mechanism, but also effectively protects FVIII from degradation in vivo, thereby supporting secondary hemostasis).…”
Section: Brief Overview On Physiological Hemostasismentioning
confidence: 99%