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Please use this identifier to cite or link to this item: https://repository.monashhealth.org/monashhealthjspui/handle/1/46762
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dc.contributor.authorTam C.S.-
dc.contributor.authorOu Y.C.-
dc.contributor.authorTrotman J.-
dc.contributor.authorOpat S.-
dc.date.accessioned2022-03-31T22:46:51Z-
dc.date.available2022-03-31T22:46:51Z-
dc.date.copyright2021-
dc.date.issued2022-02-13en
dc.identifier.citationExpert Review of Clinical Pharmacology. 14(11) (pp 1329-1344), 2021. Date of Publication: 2021.-
dc.identifier.urihttps://repository.monashhealth.org/monashhealthjspui/handle/1/46762-
dc.description.abstractIntroduction: Bruton's tyrosine kinase (BTK) inhibitors have revolutionized the treatment of B-cell lymphomas. Zanubrutinib was designed to achieve improved therapeutic concentrations and minimize off-target activities putatively accounting, in part, for the adverse effects seen with other BTK inhibitors. Areas covered: This drug profile covers zanubrutinib clinical pharmacology and the translation of pharmacokinetics (PK) and pharmacodynamics (PD) to clinical efficacy and safety profiles, by highlighting key differences between zanubrutinib and other BTK inhibitors. We discuss PK, sustained BTK occupancy, and potential factors affecting PK of zanubrutinib, including food effects, hepatic impairment, and drug-drug interactions. These data, along with exposure-response analyses, were used to support the recommended dose of 320 mg, either once daily or as 160 mg twice daily. Translation of PK/PD attributes into clinical effects was demonstrated in a randomized, phase 3 head-to-head study comparing it with ibrutinib in patients with Waldenstrom macroglobulinemia. Expert opinion: Among the approved BTK inhibitors, zanubrutinib is less prone to PK modulation by intrinsic and extrinsic factors, leading to more consistent, sustained therapeutic exposures and improved dosing convenience. Zanubrutinib PK/PD has translated into durable responses and improved safety, representing an important new treatment option for patients who benefit from BTK therapy.Copyright © 2021 The Author(s). Published by Informa UK Limited, trading as Taylor & Francis Group.-
dc.publisherTaylor and Francis Ltd.-
dc.relation.ispartofExpert Review of Clinical Pharmacology-
dc.subject.meshclinical pharmacology-
dc.subject.meshdrug absorption-
dc.subject.meshdrug distribution-
dc.subject.meshdrug efficacy-
dc.subject.meshdrug excretion-
dc.subject.meshdrug exposure-
dc.subject.meshdrug indication-
dc.subject.meshdrug interaction-
dc.subject.meshdrug metabolism-
dc.subject.meshdrug potency-
dc.subject.meshdrug safety-
dc.subject.meshdrug selectivity-
dc.subject.meshfood drug interaction-
dc.subject.meshpharmacodynamic parameters-
dc.subject.meshpharmacokinetic parameters-
dc.subject.meshphase 3 (topic)-
dc.subject.mesh(topic)-
dc.subject.meshrecommended drug dose-
dc.subject.meshWaldenstroem macroglobulinemia/dt []-
dc.subject.meshacalabrutinib/cr [Drug Concentration]-
dc.subject.meshacalabrutinib/it [Drug Interaction]-
dc.subject.meshacalabrutinib/pk [Pharmacokinetics]-
dc.subject.meshacalabrutinib/pd [Pharmacology]-
dc.subject.meshacalabrutinib/pv [Special Situation for Pharmacovigilance]-
dc.subject.meshBruton tyrosine kinase/ec [Endogenous Compound]-
dc.subject.meshcytochrome P450 3A/ec [Endogenous Compound]-
dc.subject.meshibrutinib/cr [Drug Concentration]-
dc.subject.meshibrutinib/it [Drug Interaction]-
dc.subject.meshibrutinib/pk [Pharmacokinetics]-
dc.subject.meshibrutinib/pd [Pharmacology]-
dc.subject.meshibrutinib/pv [Special Situation for Pharmacovigilance]-
dc.subject.meshitraconazole/it [Drug Interaction]-
dc.subject.meshketoconazole/it [Drug Interaction]-
dc.subject.meshvoriconazole/it [Drug Interaction]-
dc.subject.meshzanubrutinib/cr [Drug Concentration]-
dc.subject.meshzanubrutinib/do [Drug Dose]-
dc.subject.meshzanubrutinib/it [Drug Interaction]-
dc.subject.meshzanubrutinib/dt []-
dc.subject.meshzanubrutinib/pk [Pharmacokinetics]-
dc.subject.meshzanubrutinib/pd [Pharmacology]-
dc.subject.meshzanubrutinib/pv [Special Situation for Pharmacovigilance]-
dc.titleClinical pharmacology and PK/PD translation of the second-generation Bruton's tyrosine kinase inhibitor, zanubrutinib.-
dc.typeArticle-
dc.identifier.affiliationHaematology-
dc.identifier.doihttp://monash.idm.oclc.org/login?url=https://dx.doi.org/10.1080/17512433.2021.1978288-
dc.publisher.placeUnited Kingdom-
dc.identifier.pubmedid34491123 [https://www.ncbi.nlm.nih.gov/pubmed/?term=34491123]-
dc.identifier.institution(Tam) Department of Haematology, Peter MacCallum Cancer Centre, Melbourne, VIC, Australia-
dc.identifier.institution(Tam) Department of Haematology, St Vincent's Hospital, Fitzroy, Vic, Australia-
dc.identifier.institution(Tam) Department of Haematology, University of Melbourne, Parkville, VIC, Australia-
dc.identifier.institution(Tam) Department of Haematology, Royal Melbourne Hospital, Parkville, Vic, Australia-
dc.identifier.institution(Ou) Clinical Pharmacology, BeiGene USA Inc, San Mateo, CA, United States-
dc.identifier.institution(Trotman) Department of Haematology, Concord Repatriation Hospital, Concord, NSW, Australia-
dc.identifier.institution(Trotman) Department of Haematology, The University of Sydney, Concord, Nsw, Australia-
dc.identifier.institution(Opat) Director, Clinical Haematology, Monash Health, Clayton, Vic, Australia-
dc.identifier.institution(Opat) Director, Clinical Haematology, Monash University, Clayton, VIC, Australia-
dc.identifier.affiliationmh(Opat) Director, Clinical Haematology, Monash Health, Clayton, Vic, Australia-
item.openairecristypehttp://purl.org/coar/resource_type/c_18cf-
item.fulltextNo Fulltext-
item.grantfulltextnone-
item.openairetypeArticle-
item.cerifentitytypePublications-
crisitem.author.deptHaematology-
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