A. de Boer scite author profile

A. de Boer

5Publications

99Citation Statements Received

92Citation Statements Given

How they've been cited

195

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Affiliations

Centre for Human Drug Research, Leiden University

Publications

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Liver Blood Flow as a Major Determinant of the Clearance of Recombinant Human Tissue-Type Plasminogen Activator

Boer

Kluft²,

Kroon

et al. 1992

Thromb Haemost

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SummaryThe influence of changes in liver blood flow on the clearance of rt-PA was studied both in healthy subjects and in a perfused rat liver model. Liver blood flow in healthy subjects was documented indirectly by the clearance of indocyanine green (ICG). Exercise reduced liver blood flow on average by 57% with a 95% confidence interval (95% Cl) ranging from 51% to 62% (n = 5) and increased plasma levels of rt-PA activity (after an i. v. infusion of 18 mg of rt-PA over 120 min) by 119% (95% Cl, 58% - 203%) and rt-PA antigen by 91% (95% Cl, 30% - 140%). In the perfused rat liver model it was shown that halving or doubling of the physiological flow rate of a perfusate, containing rt-PA caused a proportional change in the clearance of rt-PA, while the extraction of rt-PA by the liver remained similar. In conclusion, liver blood flow is a major determinant of the clearance of rt-PA. This may have important implications for dosage of rt-PA in patients with myocardial infarction.

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Are Atypical Nevi a Risk Factor for Uveal Melanoma? A Case-Control Study

Hees

Boer

Jager

et al. 1994

Journal of Investigative Dermatology

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Oral absorption profile of nitrendipine in healthy subjects: a kinetic and dynamic study.

Soons

Boer

Brummelen

et al. 1989

Brit J Clinical Pharma

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1 In nine healthy male subjects the kinetics of nitrendipine were assessed after i.v. administration and its absorption profile was studied when given by a tablet formulation and by an osmotic pumping device (Osmet) with a zero-order in vitro release of 2.62 ± 0.19 mg h-' for 13 h.2 Plasma concentrations of nitrendipine and its pyridine metabolite, heart rate and blood pressure were determined at regular intervals after drug administration. 3 After i.v. nitrendipine, the plasma concentration declined triexponentially with a mean terminal elimination half-life of 11.7 ± 5.4 h. The mean systemic plasma clearance was 1.47 ± 0.22 1 min-1. 4 Administration of the Osmet resulted in a relatively smooth plasma concentrationtime profile in comparison with the tablet. The mean plateau concentration was 2.63 + 1.31 ng ml-1 and the duration of this plateau was 10.7 ± 3.2 h. The intake of food gave rise to a transient increase of the plasma concentration of both nitrendipine and its pyridine metabolite.5 The mean bioavailability of nitrendipine from the Osmet (8.2 ± 1.6%) was lower than from the tablet (11.1 ± 4.5%), which is probably due to release of nitrendipine in lower parts of the G.I. tract where absorption is not or less possible. 6 Intravenous administration caused a transient decrease in DBP of 26 ± 4%, accompanied by a maximal reflex tachycardia of 46 ± 17%. No clear haemodynamic effects were observed after oral administration. The Osmet produced less side-effects (headache) than the tablet.

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Plasminogen Activator Inhibitor (PA-lnhibitor) Activity in the Blood of Patients with Deep Vein Thrombosis

Paramo

Boer²,

Colucci

et al. 1985

Thromb Haemost

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Diurnal Rhythm in Anticoagulant Effect of Heparin during a Low Dose Constant Rate Infusion

et al. 1992

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SummaryThe objective of the study was to investigate possible diurnal rhythms in coagulation tests during a continuous intravenous infusion of unfractionated heparin. Six volunteers participated in the study, which was divided in a treatment (500 U heparin/h for 30 h) and a control experiment. Under basal conditions, no rhythm was found in coagulation tests. During heparin treatment, APTT, thrombin clotting time and anti-Xa activity showed a greater anticoagulant effect at night, with a striking decrease in the morning.In a search for the explanation of this phenomenon we looked for diurnal variations in the urinary excretion of heparin, in the plasma concentrations of antithrombin III and platelet factor 4, and in the effect of heparin added to the plasma samples in vitro. None of these studies provided the explanation.

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A. de Boer

Liver Blood Flow as a Major Determinant of the Clearance of Recombinant Human Tissue-Type Plasminogen Activator

Are Atypical Nevi a Risk Factor for Uveal Melanoma? A Case-Control Study

Oral absorption profile of nitrendipine in healthy subjects: a kinetic and dynamic study.

Plasminogen Activator Inhibitor (PA-lnhibitor) Activity in the Blood of Patients with Deep Vein Thrombosis

Diurnal Rhythm in Anticoagulant Effect of Heparin during a Low Dose Constant Rate Infusion

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