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importance of measuring pharmacologically active metabolites of edoxaban: development and validation of an ultra-high-performance liquid chromatography coupled with a tandem mass spectrometry method
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نویسنده
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siriez romain ,alpan lütfiye ,elasaad kossay ,devel philippe ,laloy julie ,dogné jean-michel ,douxfils jonathan
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منبع
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journal of thrombosis and thrombolysis - 2020 - دوره : 49 - شماره : 3 - صفحه:395 -403
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چکیده
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Although doacs do not require regular measurements of their blood concentrations, clinical situations require an assessment of their concentration. among the factor xa inhibitors, edoxaban is the only compound for which some metabolites (e.g. edoxaban-m4) are reported to be pharmacologically active. therefore, their contribution could interfere with assays used for the estimation of edoxaban concentration. in addition, drug interactions alter the metabolite/parent compound ratio making the sole estimation of edoxaban concentration, a poor assessment of the overall anticoagulation. to develop a validated uhplc–ms/ms method to quantify simultaneously edoxaban and its more relevant m4-metabolite in human plasma. electrospray ionization and chromatographic separation were optimized for the simultaneous dosage of edoxaban and edoxaban-m4. the method was validated according to regulatory guidelines for bioanalytical method validation. the total run time was 6 min. the method was validated for calibration curves, precision, accuracy, carry-over, selectivity, matrix effect and short-time stability. this method permits quantification of edoxaban and edoxaban-m4 providing complementary information about the inhibitory effect of this active metabolite in chronometric or chromogenic assays. although patients treated with edoxaban exhibits usually low concentrations of active metabolites, the measurement of edoxaban-m4 is interesting; especially in case of drug interactions. indeed, concomitant prescriptions of edoxaban and carbamazepine or rifampicin is frequent and lead to disturbance of the estimations of edoxaban concentration by chromogenic anti-xa assays. therefore, patients are at risk of having inadequate control of anticoagulation supporting the need of measuring the most representative edoxaban metabolite concomitantly to the parent compound.
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کلیدواژه
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edoxaban ,edoxaban-m4 ,ultra-high-performance liquid chromatography/tandem mass spectrometry ,metabolite ,direct oral anticoagulant
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آدرس
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university of namur, namur thrombosis and hemostasis center (nthc), namur research institute for life sciences (narilis), department of pharmacy, belgium, university of namur, namur thrombosis and hemostasis center (nthc), namur research institute for life sciences (narilis), department of pharmacy, belgium, university of namur, namur thrombosis and hemostasis center (nthc), namur research institute for life sciences (narilis), department of pharmacy, belgium, university of namur, namur thrombosis and hemostasis center (nthc), namur research institute for life sciences (narilis), department of pharmacy, belgium, university of namur, namur nanosafety center (nnc), namur research institute for life sciences (narilis), department of pharmacy, belgium, university of namur, namur thrombosis and hemostasis center (nthc), namur research institute for life sciences (narilis), department of pharmacy, belgium, university of namur, namur thrombosis and hemostasis center (nthc), namur research institute for life sciences (narilis), department of pharmacy, belgium. qualiblood s.a, belgium
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Authors
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