Use of a Reference Material Proposed by the International Federation of Clinical Chemistry and Laboratory Medicine to Evaluate Analytical Methods for the Determination of Plasma Lipoprotein(a)

Marcovina, Santica M.; Albers, John J.; Scanu, Angelo M.; Kennedy, Hal; Giaculli, Federico; Berg, Kåre; Couderc, Rémy; Dati, Francesco; Rifai, Nader; Sakurabayashi, Ikunosuke; Tate, Jillian R.; Steinmetz, Armin

doi:10.1093/clinchem/46.12.1956

Cited by 264 publications

(102 citation statements)

References 17 publications

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“…A normal value for plasma concentration has not been agreed upon: some authors consider this to be up to 20 mg dL − 1 [16] and others up to 30 mg dL − 1 [17], pointing out that the use of different monoclonal or polyclonal antibodies generates differences in results [18]. In order to assess concordance in results among different methods, a calibrator and a reference ELISA method have been evaluated and demonstrated to be insensitive to apo(a) isoform-size heterogeneity [19].…”

Section: Introductionmentioning

confidence: 99%

Functional approach to investigate Lp(a) in ischaemic heart and cerebral diseases

Peña-Dı́az

Cardoso-Saldaña

Zamora-González

et al. 2003

Eur J Clin Investigation

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Section: Introductionmentioning

confidence: 99%

Functional approach to investigate Lp(a) in ischaemic heart and cerebral diseases

Peña-Dı́az

Cardoso-Saldaña

Zamora-González

et al. 2003

Eur J Clin Investigation

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“…Lp(a) measurement was performed in a core laboratory certified by the NHLBI/CDC Prevention Lipid Standardization Program. We used the only commercially available assay, not affected by Kringle IV-Type 2 repeats, as assessed by a NHLBI and International Federation of Clinical Chemistry standardization group [12]. The turbidimetric assay used reagents and calibrators from Denka Seiken (Niigata, Japan) on the Hitachi 917 analyzer (Roche Diagnostics, Indianapolis, IN, USA).…”

mentioning

confidence: 99%

“…Strengths of this study include its prospective nature and use of a reliable mass-based assay [12] to measure circulating levels of Lp(a). Some of the prior discrepant findings of studies regarding Lp(a) levels and VTE may be due in part to difficulty in measuring Lp(a).…”

mentioning

confidence: 99%

Lipoprotein(a), polymorphisms in the LPA gene, and incident venous thromboembolism among 21 483 women

Danik

Buring

Chasman

et al. 2013

Journal of Thrombosis and Haemostasis

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“…Suitable protein-based assays for determination of APC-R [66,67], protein C, protein S and antithrombin activity, concentration of clottable fibrinogen, plasminogen activity, activities of coagulation factors VIIIC and XII, Lp(a) [68,69], histidine-rich glycoprotein, heparin cofactor II, and fasting homocysteine concentrations, should be investigated along with DNA-based assays, i. e. factor V G1691A mutation, prothrombin G20 210A variant and MTHFR C677T genotype.…”

Section: Screening For Risk Factors In Pediatric Patientsmentioning

confidence: 99%

DNA- and Plasma-based Screening for Risk Factors in Infants and Children with Symptomatic Thromboembolism/DNA- und plasmabasiertes Screening von Risikofaktoren bei Säuglingen und Kindern mit symptomatischen thromboembolischen Ereignissen

Nowak‐Göttl¹,

Kosch²,

Junker³

2002

LaboratoriumsMedizin

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Objective: Acquired and inherited prothrombotic risk factors increase the risk of thrombosis in neonates, infants and children. The aim was to determine which risk factors should be tested with respect to inherited and acquired clinical conditions, who should be tested, and when testing should be done. Methods: The study was based on reports in the literature on the presence of acquired and inherited prothrombotic risk factors in pediatric thromboembolism. Conclusions: After suffering thrombosis, pediatric patients should be screened for common gene mutations (factor V G1691A, prothrombin G20 210A and MTHFR C677T genotypes), rare inherited prothrombotic risk factors (deficiencies of protein C, protein S, antithrombin, and plasminogen), probably inherited risk factors (fibrinogen, factor VIIIC, factor XII), and new candidates (elevation of lipoprotein (a)), and fasting homocysteine concentrations. Re-testing is indicated for plasma-based assays 3±6 months after thrombotic onset and withdrawal of oral anticoagulation. Data interpretation is based on age-dependent reference ranges or the identification of causative gene mutations/polymorphisms with respect to individual ethnic backgrounds.Zusammenfassung: Hintergrund: Erworbene und heredita Ère prothrombotische Risikofaktoren erho Èhen das Thromboserisiko im Neugeborenen-, Sa Èuglings-und Kindesalter. Das Ziel der vorliegenden U È bersicht war es, die Bedeutung erworbener und heredita Èrer Risikofaktoren, sowie den Zeitpunkt eines Screenings unter Beru Ècksichtigung der klinischen Situation zu evaluieren. Methoden: Die Untersuchung basiert auf aktuellen Daten der Literatur zu erworbenen und angeborenen prothrombotischen Risikofaktoren bei pa Èdiatrischen Patien-ten mit Thromboembolien. Schlussfolgerung: Nach Manifestation einer Thrombose sollten pa Èdiatrische Patienten auf das Vorliegen ha Èufiger Genmutationen (Faktor V G1691A, Prothrombin G20 210A und MTHFR C677T Genotypen) sowie seltener angeborener prothrombotischer Risikofaktoren (Protein C-, Protein S-, Antithrombin-und Plasminogenmangel), auf vermutlich genetisch bedingte Risikofaktoren (Dys-/Afibrinogena Èmien, Faktor-VIII-Erho Èhung und Faktor-XII-Mangel) und zusa Ètzlich auf neu beschriebene Risikofaktoren (Lipoprotein(a)-Erho Èhung) und Nu Èchtern-Homocysteinkonzentrationen untersucht werden. Risikofaktoren die mittels plasmabasierter Assays nachgewiesen werden, sollten 3±6 Monate nach einem thromboembolischen Ereigniss sowie nach Absetzen der oralen Antikoagulation erneut getestet werden. Screeningdaten mu Èssen auf der Grundlage altersabha Èngiger Normwerte oder der Identifikation von zugrundeliegenden Genmutationen/Polymorphismen unter Beru Ècksichtigung des ethischen Hintergrundes interpretiert werden.

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Use of a Reference Material Proposed by the International Federation of Clinical Chemistry and Laboratory Medicine to Evaluate Analytical Methods for the Determination of Plasma Lipoprotein(a)

Cited by 264 publications

References 17 publications

Functional approach to investigate Lp(a) in ischaemic heart and cerebral diseases

Functional approach to investigate Lp(a) in ischaemic heart and cerebral diseases

Lipoprotein(a), polymorphisms in the LPA gene, and incident venous thromboembolism among 21 483 women

DNA- and Plasma-based Screening for Risk Factors in Infants and Children with Symptomatic Thromboembolism/DNA- und plasmabasiertes Screening von Risikofaktoren bei Säuglingen und Kindern mit symptomatischen thromboembolischen Ereignissen

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