The Influence of Age on in vitro Plasmin Generation in the Presence of Fibrin Monomer

Parmar, Nagina; Mitchell, Lesley; Berry, Leslie R.; Andrew, Maureen; Chan, Anthony

doi:10.1159/000090927

Cited by 13 publications

(7 citation statements)

References 88 publications

(57 reference statements)

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“…The antifibrinolytic effect of lipoproteins is also less pronounced in newborns compared with adults, due to the presence of lower plasminogen concentration. 37 When compared with adult reference ranges, children aged 1 to 5 years might display significantly higher values of soluble thrombomodulin, thrombin-antithrombin complex, and D-dimer. 38 Finally, although platelet function might be reduced in newborns, 39 the global primary hemostasis system, as assessed by the platelet function analyzer (PFA-100; Dade Behring, Marburg, Germany), might be enhanced because of the increased VWF-mediated platelet adhesion.…”

Section: Hemostatic Abnormalities In the Newbornmentioning

confidence: 99%

Coagulation Testing in Pediatric Patients: The Young Are Not Just Miniature Adults

Lippi

Franchini

Montagnana

et al. 2007

Semin Thromb Hemost

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During the past few decades, great progress has been made toward a better understanding of the development of the hemostatic system. It is now clear that the physiology of hemostasis in pediatric patients differs widely from that in adults, supporting the hypothesis that children might have natural protective mechanisms that justify such variations. However, the correct interpretation of hemostasis test results in young patients, along with a deep understanding of the normal postnatal development in the human coagulation system, are essential prerequisites to the proper investigation of thrombotic and hemorrhagic problems in pediatric patients. Because the hemostatic system is not fully mature by 3 to 6 months of age, it is important to recognize that interpretation of laboratory data in pediatric patients must be accompanied by appropriate age-dependent reference ranges, which should also be specific for the testing system used, to prevent misclassification of children as having defects of factors and inhibitors of the coagulation system.

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Section: Hemostatic Abnormalities In the Newbornmentioning

confidence: 99%

Coagulation Testing in Pediatric Patients: The Young Are Not Just Miniature Adults

Lippi

Franchini

Montagnana

et al. 2007

Semin Thromb Hemost

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“…Serine proteases possessing a trypsin fold are involved in many biological processes, including blood coagulation [1], metastasis of cancer cells [2], fibrinolysis [3], mammary gland involution [4], and the envenomation process [5]. These enzymes may be inhibited by ecotin, a periplasmic Escherichia coli-derived protein and a "fold-specific" inhibitor that has an unusually broad specificity to proteases such as trypsin, chymotrypsin, elastase, factor Xa, kallikrein, and factor XIIa [6,7].…”

Section: Introductionmentioning

confidence: 99%

Engineering Ecotin for Identifying Proteins with a Trypsin Fold

Sathler

Craik

Takeuchi

et al. 2009

Appl Biochem Biotechnol

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Ecotin is a bidentate, fold-specific inhibitor of mammalian serine-proteases produced by Escherichia coli. This molecule may be engineered to increase and/or change its affinity and specificity providing significant biotechnological potential. Since ecotin binds tightly to serine proteases of the trypsin fold, it may help to identify the role of these enzymes in different biological processes. In this work, we tested ecotin variants as an affinity purification reagent for identifying enzymes in samples of tumor progression and mammary gland involution. Initially, we used a commercial source of urokinase-type plasminogen activator (u-PA) that remained fully active after elution from an affinity column of the ecotin variant (M84R, M85R). We then successfully identified u-PA from more complex mixtures including lysates from a prostate cancer cell line and involuting mouse mammary glands. Interestingly, a membrane-type serine protease 1 was isolated from the Triton X-100-solubilized PC-3 cell lysates, and surprisingly, haptoglobin, a serine-protease homolog protein, was also identified in mammary gland lysates and in blood. Haptoglobin does not prevent ecotin inhibition of u-PA, but it may act as a carrier within blood when ecotin is used in vivo. Finally, this affinity purification matrix was also able to identify a thrombin-like enzyme from snake venom using an ecotin variant directed against thrombin. Overall, the ecotin variants acted as robust tools for the isolation and characterization of proteins with a trypsin fold. Thus, they may assist in the understanding of the role of these serine proteases and homologous proteins in different biological processes.

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“…8 Recently, it was shown that plasmin generation induced by r-tPA in vitro was lower in newborn than in adult plasma, which could explain the clinical finding that the elimination of thrombi in newborns is more challenging than in adults. 5 During the neonatal period, thrombin formation, endothelial activation, and procoagulant activity are increased. In our patients, catheter usage was 76.4%, but pathologies that increase the risk of thrombosis and lead to clinical deterioration, such as sepsis, hypoxia, polycythemia, and mutations in thrombosis markers, were also present.…”

Section: Discussionmentioning

confidence: 99%

“…In children, these systems exhibit agedependent differences, including a lower plasminogen concentration than in adults and thus reduced plasmin generation. 5 The varying risks of thrombus formation resulting from the above-described situations highlight the requirement for a patient-specific thrombolytic therapy in neonates and infants.…”

Section: Introductionmentioning

confidence: 99%