Pharmacokinetics of Daprodustat and Metabolites in Individuals with Normal and Impaired Hepatic Function

Daprodustat is a hypoxia‐inducible factor‐prolyl hydroxylase inhibitor in development for treatment of anemia of chronic kidney disease. We evaluated the role of hepatic impairment on daprodustat pharmacokinetics, pharmacodynamics, and tolerability. Participants with mild (Child‐Pugh Class A, score...

Full description

Saved in:

Bibliographic Details
Published in	Clinical pharmacology in drug development Vol. 11; no. 5; pp. 562 - 575
Main Authors	Mahar, Kelly M., Shaddinger, Bonnie C., Ramanjineyulu, Bandi, Andrews, Susan, Caltabiano, Stephen, Lindsay, Alistair C., Cobitz, Alexander R.
Format	Journal Article
Language	English
Published	United States Wiley Subscription Services, Inc 01.05.2022 John Wiley and Sons Inc
Subjects	anemia Barbiturates daprodustat Female Glycine - adverse effects Glycine - analogs & derivatives Glycine - pharmacokinetics hepatic impairment Humans Liver Liver Diseases - metabolism Male Metabolites Original Pharmacodynamics Pharmacokinetics Prolyl-Hydroxylase Inhibitors - adverse effects Prolyl-Hydroxylase Inhibitors - pharmacokinetics hepatic impairment pharmacokinetics daprodustat pharmacodynamics anemia
Online Access	Get full text

Cover

Loading…

Abstract	Daprodustat is a hypoxia‐inducible factor‐prolyl hydroxylase inhibitor in development for treatment of anemia of chronic kidney disease. We evaluated the role of hepatic impairment on daprodustat pharmacokinetics, pharmacodynamics, and tolerability. Participants with mild (Child‐Pugh Class A, score 5‒6) and moderate (Child‐Pugh Class B, score 7‒9) hepatic impairment and matched healthy controls were administered single 6‐mg doses of daprodustat. Exposure parameters were determined for daprodustat and its six metabolites. Comparisons resulted in 1.5‐ and 2.0‐fold higher daprodustat Cmax and area under the curve (AUC) exposures in participants with mild and moderate hepatic impairment, respectively, versus controls; Cmax in mild hepatic impairment was comparable to controls. Similarly, aligned with parent drug, unbound daprodustat Cmax and AUC exposures increased 1.6‐ to 2.3‐fold in hepatic‐impaired participants versus controls, and metabolite exposures were 1.2‐ to 2.0‐fold higher in participants with hepatic impairment. Erythropoeitin (EPO) baseline‐corrected AUC exposures were between 0.3‐fold lower and 2.2‐fold higher in matched controls versus hepatic‐impaired participants. No serious or study drug‐related adverse events were reported. Daprodustat exposure was increased in participants with moderate and mild hepatic impairment compared with matched controls; however, no meaningful differences in EPO were observed and no new safety concerns were identified (ClinicalTrials.gov: NCT03223337).
AbstractList	Daprodustat is a hypoxia-inducible factor-prolyl hydroxylase inhibitor in development for treatment of anemia of chronic kidney disease. We evaluated the role of hepatic impairment on daprodustat pharmacokinetics, pharmacodynamics, and tolerability. Participants with mild (Child-Pugh Class A, score 5-6) and moderate (Child-Pugh Class B, score 7-9) hepatic impairment and matched healthy controls were administered single 6-mg doses of daprodustat. Exposure parameters were determined for daprodustat and its six metabolites. Comparisons resulted in 1.5- and 2.0-fold higher daprodustat C and area under the curve (AUC) exposures in participants with mild and moderate hepatic impairment, respectively, versus controls; C in mild hepatic impairment was comparable to controls. Similarly, aligned with parent drug, unbound daprodustat C and AUC exposures increased 1.6- to 2.3-fold in hepatic-impaired participants versus controls, and metabolite exposures were 1.2- to 2.0-fold higher in participants with hepatic impairment. Erythropoeitin (EPO) baseline-corrected AUC exposures were between 0.3-fold lower and 2.2-fold higher in matched controls versus hepatic-impaired participants. No serious or study drug-related adverse events were reported. Daprodustat exposure was increased in participants with moderate and mild hepatic impairment compared with matched controls; however, no meaningful differences in EPO were observed and no new safety concerns were identified (ClinicalTrials.gov: NCT03223337). Abstract Daprodustat is a hypoxia‐inducible factor‐prolyl hydroxylase inhibitor in development for treatment of anemia of chronic kidney disease. We evaluated the role of hepatic impairment on daprodustat pharmacokinetics, pharmacodynamics, and tolerability. Participants with mild (Child‐Pugh Class A, score 5‒6) and moderate (Child‐Pugh Class B, score 7‒9) hepatic impairment and matched healthy controls were administered single 6‐mg doses of daprodustat. Exposure parameters were determined for daprodustat and its six metabolites. Comparisons resulted in 1.5‐ and 2.0‐fold higher daprodustat C max and area under the curve (AUC) exposures in participants with mild and moderate hepatic impairment, respectively, versus controls; C max in mild hepatic impairment was comparable to controls. Similarly, aligned with parent drug, unbound daprodustat C max and AUC exposures increased 1.6‐ to 2.3‐fold in hepatic‐impaired participants versus controls, and metabolite exposures were 1.2‐ to 2.0‐fold higher in participants with hepatic impairment. Erythropoeitin (EPO) baseline‐corrected AUC exposures were between 0.3‐fold lower and 2.2‐fold higher in matched controls versus hepatic‐impaired participants. No serious or study drug‐related adverse events were reported. Daprodustat exposure was increased in participants with moderate and mild hepatic impairment compared with matched controls; however, no meaningful differences in EPO were observed and no new safety concerns were identified (ClinicalTrials.gov: NCT03223337). Daprodustat is a hypoxia‐inducible factor‐prolyl hydroxylase inhibitor in development for treatment of anemia of chronic kidney disease. We evaluated the role of hepatic impairment on daprodustat pharmacokinetics, pharmacodynamics, and tolerability. Participants with mild (Child‐Pugh Class A, score 5‒6) and moderate (Child‐Pugh Class B, score 7‒9) hepatic impairment and matched healthy controls were administered single 6‐mg doses of daprodustat. Exposure parameters were determined for daprodustat and its six metabolites. Comparisons resulted in 1.5‐ and 2.0‐fold higher daprodustat C max and area under the curve (AUC) exposures in participants with mild and moderate hepatic impairment, respectively, versus controls; C max in mild hepatic impairment was comparable to controls. Similarly, aligned with parent drug, unbound daprodustat C max and AUC exposures increased 1.6‐ to 2.3‐fold in hepatic‐impaired participants versus controls, and metabolite exposures were 1.2‐ to 2.0‐fold higher in participants with hepatic impairment. Erythropoeitin (EPO) baseline‐corrected AUC exposures were between 0.3‐fold lower and 2.2‐fold higher in matched controls versus hepatic‐impaired participants. No serious or study drug‐related adverse events were reported. Daprodustat exposure was increased in participants with moderate and mild hepatic impairment compared with matched controls; however, no meaningful differences in EPO were observed and no new safety concerns were identified (ClinicalTrials.gov: NCT03223337). Daprodustat is a hypoxia‐inducible factor‐prolyl hydroxylase inhibitor in development for treatment of anemia of chronic kidney disease. We evaluated the role of hepatic impairment on daprodustat pharmacokinetics, pharmacodynamics, and tolerability. Participants with mild (Child‐Pugh Class A, score 5‒6) and moderate (Child‐Pugh Class B, score 7‒9) hepatic impairment and matched healthy controls were administered single 6‐mg doses of daprodustat. Exposure parameters were determined for daprodustat and its six metabolites. Comparisons resulted in 1.5‐ and 2.0‐fold higher daprodustat Cmax and area under the curve (AUC) exposures in participants with mild and moderate hepatic impairment, respectively, versus controls; Cmax in mild hepatic impairment was comparable to controls. Similarly, aligned with parent drug, unbound daprodustat Cmax and AUC exposures increased 1.6‐ to 2.3‐fold in hepatic‐impaired participants versus controls, and metabolite exposures were 1.2‐ to 2.0‐fold higher in participants with hepatic impairment. Erythropoeitin (EPO) baseline‐corrected AUC exposures were between 0.3‐fold lower and 2.2‐fold higher in matched controls versus hepatic‐impaired participants. No serious or study drug‐related adverse events were reported. Daprodustat exposure was increased in participants with moderate and mild hepatic impairment compared with matched controls; however, no meaningful differences in EPO were observed and no new safety concerns were identified (ClinicalTrials.gov: NCT03223337).
Author	Mahar, Kelly M. Shaddinger, Bonnie C. Cobitz, Alexander R. Caltabiano, Stephen Ramanjineyulu, Bandi Andrews, Susan Lindsay, Alistair C.
AuthorAffiliation	2 Medicine Delivery Unit GlaxoSmithKline Collegeville Pennsylvania USA 4 Clinical Science & Study Operations GlaxoSmithKline Collegeville Pennsylvania USA 3 Biostatistics GlaxoSmithKline Bangalore India 1 Clinical Pharmacology Modeling & Simulation GlaxoSmithKline Collegeville Pennsylvania USA
AuthorAffiliation_xml	– name: 4 Clinical Science & Study Operations GlaxoSmithKline Collegeville Pennsylvania USA – name: 1 Clinical Pharmacology Modeling & Simulation GlaxoSmithKline Collegeville Pennsylvania USA – name: 2 Medicine Delivery Unit GlaxoSmithKline Collegeville Pennsylvania USA – name: 3 Biostatistics GlaxoSmithKline Bangalore India
Author_xml	– sequence: 1 givenname: Kelly M. surname: Mahar fullname: Mahar, Kelly M. email: kelly.m.mahar@gsk.com organization: GlaxoSmithKline – sequence: 2 givenname: Bonnie C. surname: Shaddinger fullname: Shaddinger, Bonnie C. organization: GlaxoSmithKline – sequence: 3 givenname: Bandi surname: Ramanjineyulu fullname: Ramanjineyulu, Bandi organization: GlaxoSmithKline – sequence: 4 givenname: Susan surname: Andrews fullname: Andrews, Susan organization: GlaxoSmithKline – sequence: 5 givenname: Stephen surname: Caltabiano fullname: Caltabiano, Stephen organization: GlaxoSmithKline – sequence: 6 givenname: Alistair C. surname: Lindsay fullname: Lindsay, Alistair C. organization: GlaxoSmithKline – sequence: 7 givenname: Alexander R. surname: Cobitz fullname: Cobitz, Alexander R. organization: GlaxoSmithKline
BackLink	https://www.ncbi.nlm.nih.gov/pubmed/35355447$$D View this record in MEDLINE/PubMed
BookMark	eNp1kU9PFDEYhxsDEVw4-AVMEy94WOn_GS4mZhdkE1QOmHhr3mk7bnGmHdsZCN_eLosbNLGXvkmfPn37_l6hvRCDQ-g1Je8pIezUDNaW6oy8QIeMKjKvlKj3djX_foCOc74lZSlCKRUv0QGXXEohqkO0vl5D6sHEnz640ZuMY4uXMKRopzzCiCFY_NmN0MTOjy5jH_AqWH_n7QRdxvd-XOMvsSi6R3TVD-CTs_jSDVB8-GIKZvQxHKH9tlxwx0_7DH27OL9ZXM6vvn5aLT5ezY0QnMyt4cIoUlFZs1Zyxh2YltSCWkEMA-YqRW0DnDHCpW04MMNaAqqxpOaqEnyGPmy9w9T0zhoXxgSdHpLvIT3oCF7_fRL8Wv-Id_qMU6JYXQQnT4IUf00uj7r32biug-DilDVTQtayPFUV9O0_6G2cUijfK5Qs05a8THqG3m0pk2LOybW7ZijRmwj1JkK9ibCwb553vyP_BFaA0y1w7zv38H-TXlwvl4_K3ywfqGQ
CitedBy_id	crossref_primary_10_1002_cpdd_1257 crossref_primary_10_1002_cpt_3215 crossref_primary_10_1016_j_lfs_2024_122641 crossref_primary_10_1177_00185787231172382
Cites_doi	10.1007/s00228-008-0553-z 10.1056/NEJMoa0907845 10.1053/j.ajkd.2017.09.026 10.1016/j.jchromb.2015.11.057 10.1038/ki.2008.295 10.1002/hep.1840210121 10.1056/NEJMoa065485 10.1186/s12882-019-1547-z 10.1093/ckj/sfz013 10.1681/ASN.2014111139 10.3748/wjg.v22.i3.1260 10.1053/j.ajkd.2016.12.011 10.1002/cpdd.1029 10.1681/ASN.2011111078 10.1093/ckj/sfy014 10.1002/prp2.327 10.1177/0192623319880445 10.1093/ndt/gft443 10.2215/CJN.16011219 10.1002/cpdd.83 10.1056/NEJMoa1005109 10.1093/ckj/sfy013 10.1080/00365520310008340
ContentType	Journal Article
Copyright	2022 GlaxoSmithKline. published by Wiley Periodicals LLC on behalf of American College of Clinical Pharmacology 2022 GlaxoSmithKline. Clinical Pharmacology in Drug Development published by Wiley Periodicals LLC on behalf of American College of Clinical Pharmacology. 2022. This article is published under http://creativecommons.org/licenses/by/4.0/ (the “License”). Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.
Copyright_xml	– notice: 2022 GlaxoSmithKline. published by Wiley Periodicals LLC on behalf of American College of Clinical Pharmacology – notice: 2022 GlaxoSmithKline. Clinical Pharmacology in Drug Development published by Wiley Periodicals LLC on behalf of American College of Clinical Pharmacology. – notice: 2022. This article is published under http://creativecommons.org/licenses/by/4.0/ (the “License”). Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.
DBID	24P WIN CGR CUY CVF ECM EIF NPM AAYXX CITATION K9. 7X8 5PM
DOI	10.1002/cpdd.1090
DatabaseName	Wiley_OA刊 Wiley-Blackwell Backfiles (Open access) Medline MEDLINE MEDLINE (Ovid) MEDLINE MEDLINE PubMed CrossRef ProQuest Health & Medical Complete (Alumni) MEDLINE - Academic PubMed Central (Full Participant titles)
DatabaseTitle	MEDLINE Medline Complete MEDLINE with Full Text PubMed MEDLINE (Ovid) CrossRef ProQuest Health & Medical Complete (Alumni) MEDLINE - Academic
DatabaseTitleList	MEDLINE CrossRef ProQuest Health & Medical Complete (Alumni)
Database_xml	– sequence: 1 dbid: 24P name: Wiley-Blackwell Titles (Open access) url: https://authorservices.wiley.com/open-science/open-access/browse-journals.html sourceTypes: Publisher – sequence: 2 dbid: NPM name: PubMed url: https://proxy.k.utb.cz/login?url=http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed sourceTypes: Index Database – sequence: 3 dbid: EIF name: MEDLINE url: https://proxy.k.utb.cz/login?url=https://www.webofscience.com/wos/medline/basic-search sourceTypes: Index Database
DeliveryMethod	fulltext_linktorsrc
Discipline	Pharmacy, Therapeutics, & Pharmacology
DocumentTitleAlternate	Mahar et al
EISSN	2160-7648
EndPage	575
ExternalDocumentID	10_1002_cpdd_1090 35355447 CPDD1090
Genre	article Clinical Study Research Support, Non-U.S. Gov't Journal Article
GroupedDBID	-MK 05W 0R~ 1OC 24P 33P 3SF 52U 52V 53G 8-1 AAESR AAEVG AAHHS AANLZ AAONW AAXRX AAZKR ABCUV ABDBF ABJNI ABQWH ABXGK ACAHQ ACBWZ ACCFJ ACCZN ACGFS ACGOF ACMXC ACPOU ACXBN ACXQS ADBBV ADBTR ADEOM ADIZJ ADKYN ADMGS ADOZA ADXAS ADZMN ADZOD AEEZP AEIGN AEIMD AENEX AEQDE AEUYR AFBPY AFFPM AFGKR AFPWT AHBTC AIACR AITYG AIURR AIWBW AJBDE ALMA_UNASSIGNED_HOLDINGS ALUQN AMBMR AMYDB ASPBG ATUGU AVWKF AZFZN AZVAB BDRZF BFHJK BHBCM BMXJE BNHUX BOGZA BRXPI C45 DCZOG DPXWK DRFUL DRMAN DRSTM EBS EJD FUBAC G-S GODZA H13 HGLYW KBYEO LATKE LEEKS LH4 LITHE LOXES LSO LUTES LW6 LYRES MEWTI MRFUL MRMAN MRSTM MSFUL MSMAN MSSTM MXFUL MXMAN MXSTM MY~ O66 O9- OVD P2W PQQKQ R.K ROL SUPJJ TEORI TUS WBKPD WIH WIJ WIK WIN WOHZO WOIKV WPGGZ WXSBR WYJ ZZTAW CGR CUY CVF ECM EIF NPM AAYXX CITATION K9. 7X8 5PM
ID	FETCH-LOGICAL-c4430-dc34c6071582f5323eacf0841d40c2a2e761dba322035db3a2c2f0a6bd0836743
IEDL.DBID	24P
ISSN	2160-763X
IngestDate	Tue Sep 17 21:22:36 EDT 2024 Sat Aug 17 02:35:53 EDT 2024 Thu Oct 10 17:59:39 EDT 2024 Fri Aug 23 03:35:51 EDT 2024 Wed Oct 16 00:41:10 EDT 2024 Sat Aug 24 01:03:11 EDT 2024
IsDoiOpenAccess	true
IsOpenAccess	true
IsPeerReviewed	true
IsScholarly	true
Issue	5
Keywords	hepatic impairment pharmacokinetics daprodustat pharmacodynamics anemia
Language	English
License	Attribution 2022 GlaxoSmithKline. Clinical Pharmacology in Drug Development published by Wiley Periodicals LLC on behalf of American College of Clinical Pharmacology. This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
LinkModel	DirectLink
MergedId	FETCHMERGED-LOGICAL-c4430-dc34c6071582f5323eacf0841d40c2a2e761dba322035db3a2c2f0a6bd0836743
Notes	CSL Behring, King of Prussia, Pennsylvania, USA ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23
OpenAccessLink	https://onlinelibrary.wiley.com/doi/abs/10.1002%2Fcpdd.1090
PMID	35355447
PQID	2656015335
PQPubID	2034576
PageCount	14
ParticipantIDs	pubmedcentral_primary_oai_pubmedcentral_nih_gov_9310628 proquest_miscellaneous_2645856747 proquest_journals_2656015335 crossref_primary_10_1002_cpdd_1090 pubmed_primary_35355447 wiley_primary_10_1002_cpdd_1090_CPDD1090
PublicationCentury	2000
PublicationDate	May 2022
PublicationDateYYYYMMDD	2022-05-01
PublicationDate_xml	– month: 05 year: 2022 text: May 2022
PublicationDecade	2020
PublicationPlace	United States
PublicationPlace_xml	– name: United States – name: Oxford – name: Hoboken
PublicationTitle	Clinical pharmacology in drug development
PublicationTitleAlternate	Clin Pharmacol Drug Dev
PublicationYear	2022
Publisher	Wiley Subscription Services, Inc John Wiley and Sons Inc
Publisher_xml	– name: Wiley Subscription Services, Inc – name: John Wiley and Sons Inc
References	2018; 6 2021; 109 2012; 2 2021; 10 2014; 3 2019; 20 2017; 69 2004; 39 2019; 12 1995; 21 2010; 363 2020; 15 2020; 48 2018 2016; 1009‐1010 2014; 29 2009; 361 2008; 74 2018; 71 2008; 64 2012; 23 2016; 27 2006; 355 2016; 22 e_1_2_8_24_1 e_1_2_8_25_1 e_1_2_8_26_1 e_1_2_8_27_1 e_1_2_8_3_1 e_1_2_8_2_1 e_1_2_8_5_1 e_1_2_8_7_1 e_1_2_8_6_1 Kidney Disease: Improving Global Outcomes (KDIGO) Anemia Work Group (e_1_2_8_4_1) 2012; 2 e_1_2_8_9_1 e_1_2_8_8_1 e_1_2_8_20_1 e_1_2_8_22_1 Chen L (e_1_2_8_21_1) 2021; 109 e_1_2_8_17_1 e_1_2_8_18_1 e_1_2_8_19_1 e_1_2_8_13_1 e_1_2_8_14_1 e_1_2_8_15_1 e_1_2_8_16_1 Food and Drug Administration (e_1_2_8_23_1) 2018 e_1_2_8_10_1 e_1_2_8_11_1 e_1_2_8_12_1
References_xml	– volume: 12 start-page: 139 issue: 1 year: 2019 end-page: 148 article-title: Daprodustat for anemia: a 24‐week, open‐label, randomized controlled trial in participants on hemodialysis publication-title: Clin Kidney J – volume: 12 start-page: 693 issue: 5 year: 2019 end-page: 701 article-title: Effect of renal function and dialysis modality on daprodustat and predominant metabolite exposure publication-title: Clin Kidney J – volume: 10 start-page: 1419 issue: 12 year: 2021 end-page: 1431 article-title: Clinical pharmacokinetics of daprodustat: results of an absorption, distribution, and excretion study with IV microtracer and concomitant oral doses for bioavailability determination publication-title: Clin Pharmacol Drug Dev – volume: 22 start-page: 1260 year: 2016 end-page: 1278 article-title: Pharmacokinetic drug interactions in liver disease: an update publication-title: World J Gastroenterol – volume: 361 start-page: 2019 issue: 21 year: 2009 end-page: 2032 article-title: A trial of darbepoetin alfa in type 2 diabetes and chronic kidney disease publication-title: N Engl J Med – volume: 74 start-page: 791 issue: 6 year: 2008 end-page: 798 article-title: Secondary analysis of the CHOIR trial epoetin‐alpha dose and achieved hemoglobin outcomes publication-title: Kidney Int – volume: 21 start-page: 120 year: 1995 end-page: 128 article-title: Differential alterations of cytochrome P450 proteins in livers from patients with severe chronic liver disease publication-title: Hepatology – volume: 1009‐1010 start-page: 7 year: 2016 end-page: 16 article-title: Overcoming bioanalytical challenges associated with the separation and quantitation of GSK1278863, a HIF‐prolyl hydroxylase inhibitor, and its 14 stereoisomeric metabolites publication-title: J Chromatogr B Analyt Technol Biomed Life Sci – volume: 109 start-page: S54 year: 2021 article-title: Human Metabolism and disposition of daprodustat: a prolyl hydroxylase inhibitor to treat anemia in chronic kidney disease (CKD) publication-title: Clin Pharmacol Ther – volume: 71 start-page: 423 issue: 3 year: 2018 end-page: 435 article-title: Update on anemia in ESRD and earlier stages of CKD: core curriculum 2018 publication-title: Am J Kidney Dis – volume: 39 start-page: 259 year: 2004 end-page: 266 article-title: Analysis of factors contributing to higher erythropoietin levels in patients with chronic liver disease publication-title: Scand J Gastroenterol – year: 2018 – volume: 64 start-page: 1147 year: 2008 end-page: 1161 article-title: Pharmacokinetics and dosage adjustment in patients with hepatic dysfunction publication-title: Eur J Clin Pharmacol – volume: 363 start-page: 1146 issue: 12 year: 2010 end-page: 1155 article-title: Erythropoietic response and outcomes in kidney disease and type 2 diabetes publication-title: N Engl J Med – volume: 27 start-page: 1234 issue: 4 year: 2016 end-page: 1244 article-title: Four‐week studies of oral hypoxia‐inducible factor‐prolyl hydroxylase inhibitor GSK1278863 for treatment of anemia publication-title: J Am Soc Nephrol – volume: 355 start-page: 2085 issue: 20 year: 2006 end-page: 2098 article-title: Correction of anemia with epoetin alfa in chronic kidney disease publication-title: N Engl J Med – volume: 6 issue: 2 year: 2018 article-title: The drug interaction potential of daprodustat when coadministered with pioglitazone, rosuvastatin, or trimethoprim in healthy subjects publication-title: Pharmacol Res Perspect – volume: 23 start-page: 1631 issue: 10 year: 2012 end-page: 1634 article-title: Mechanisms of anemia in CKD publication-title: J Am Soc Nephrol – volume: 48 start-page: 362 issue: 2 year: 2020 end-page: 378 article-title: Carcinogenicity assessment of daprodustat (GSK1278863), a hypoxia‐inducible factor (HIF)‐prolyl hydroxylase inhibitor publication-title: Toxicol Pathol – volume: 69 start-page: 815 issue: 6 year: 2017 end-page: 826 article-title: Hypoxia‐inducible factor prolyl hydroxylase inhibitors: a potential new treatment for anemia in patients with CKD publication-title: Am J Kidney Dis – volume: 2 start-page: 279 issue: 4 year: 2012 end-page: 335 article-title: KDIGO clinical practice guideline for anemia in chronic kidney disease publication-title: Kidney Int Suppl – volume: 15 start-page: 1155 issue: 8 year: 2020 end-page: 1165 article-title: Efficacy and Safety of daprodustat compared with darbepoetin alfa in Japanese hemodialysis patients with anemia: a randomized, double‐blind, phase 3 trial publication-title: Clin J Am Soc Nephrol – volume: 12 start-page: 129 issue: 1 year: 2019 end-page: 138 article-title: Daprodustat for anemia: a 24‐week, open‐label, randomized controlled trial in participants with chronic kidney disease publication-title: Clin Kidney J – volume: 3 start-page: 109 issue: 2 year: 2014 end-page: 117 article-title: Effect of food and gemfibrozil on the pharmacokinetics of the novel prolyl hydroxylase inhibitor GSK1278863 publication-title: Clin Pharmacol Drug Dev – volume: 20 start-page: 372 issue: 1 year: 2019 article-title: A randomized, 29‐day, dose‐ranging, efficacy and safety study of daprodustat, administered three times weekly in patients with anemia on hemodialysis publication-title: BMC Nephrol – volume: 29 start-page: 263 issue: 2 year: 2014 end-page: 273 article-title: The iron cycle in Chronic Kidney Disease (CKD): from genetics and experimental models to CKD patients publication-title: Nephrol Dial Transplant – ident: e_1_2_8_26_1 doi: 10.1007/s00228-008-0553-z – ident: e_1_2_8_6_1 doi: 10.1056/NEJMoa0907845 – ident: e_1_2_8_5_1 doi: 10.1053/j.ajkd.2017.09.026 – ident: e_1_2_8_19_1 doi: 10.1016/j.jchromb.2015.11.057 – ident: e_1_2_8_9_1 doi: 10.1038/ki.2008.295 – volume: 109 start-page: S54 year: 2021 ident: e_1_2_8_21_1 article-title: Human Metabolism and disposition of daprodustat: a prolyl hydroxylase inhibitor to treat anemia in chronic kidney disease (CKD) publication-title: Clin Pharmacol Ther contributor: fullname: Chen L – volume: 2 start-page: 279 issue: 4 year: 2012 ident: e_1_2_8_4_1 article-title: KDIGO clinical practice guideline for anemia in chronic kidney disease publication-title: Kidney Int Suppl contributor: fullname: Kidney Disease: Improving Global Outcomes (KDIGO) Anemia Work Group – ident: e_1_2_8_25_1 doi: 10.1002/hep.1840210121 – ident: e_1_2_8_7_1 doi: 10.1056/NEJMoa065485 – ident: e_1_2_8_11_1 doi: 10.1186/s12882-019-1547-z – ident: e_1_2_8_18_1 doi: 10.1093/ckj/sfz013 – ident: e_1_2_8_13_1 doi: 10.1681/ASN.2014111139 – ident: e_1_2_8_24_1 doi: 10.3748/wjg.v22.i3.1260 – ident: e_1_2_8_15_1 doi: 10.1053/j.ajkd.2016.12.011 – ident: e_1_2_8_22_1 doi: 10.1002/cpdd.1029 – ident: e_1_2_8_2_1 doi: 10.1681/ASN.2011111078 – ident: e_1_2_8_14_1 doi: 10.1093/ckj/sfy014 – ident: e_1_2_8_17_1 doi: 10.1002/prp2.327 – ident: e_1_2_8_20_1 doi: 10.1177/0192623319880445 – volume-title: Bioanalytic Method Validation Guidance for Industry year: 2018 ident: e_1_2_8_23_1 contributor: fullname: Food and Drug Administration – ident: e_1_2_8_3_1 doi: 10.1093/ndt/gft443 – ident: e_1_2_8_10_1 doi: 10.2215/CJN.16011219 – ident: e_1_2_8_16_1 doi: 10.1002/cpdd.83 – ident: e_1_2_8_8_1 doi: 10.1056/NEJMoa1005109 – ident: e_1_2_8_12_1 doi: 10.1093/ckj/sfy013 – ident: e_1_2_8_27_1 doi: 10.1080/00365520310008340
SSID	ssj0000601114
Score	2.3049393
Snippet	Daprodustat is a hypoxia‐inducible factor‐prolyl hydroxylase inhibitor in development for treatment of anemia of chronic kidney disease. We evaluated the role... Daprodustat is a hypoxia-inducible factor-prolyl hydroxylase inhibitor in development for treatment of anemia of chronic kidney disease. We evaluated the role... Abstract Daprodustat is a hypoxia‐inducible factor‐prolyl hydroxylase inhibitor in development for treatment of anemia of chronic kidney disease. We evaluated...
SourceID	pubmedcentral proquest crossref pubmed wiley
SourceType	Open Access Repository Aggregation Database Index Database Publisher
StartPage	562
SubjectTerms	anemia Barbiturates daprodustat Female Glycine - adverse effects Glycine - analogs & derivatives Glycine - pharmacokinetics hepatic impairment Humans Liver Liver Diseases - metabolism Male Metabolites Original Pharmacodynamics Pharmacokinetics Prolyl-Hydroxylase Inhibitors - adverse effects Prolyl-Hydroxylase Inhibitors - pharmacokinetics
Title	Pharmacokinetics of Daprodustat and Metabolites in Individuals with Normal and Impaired Hepatic Function
URI	https://onlinelibrary.wiley.com/doi/abs/10.1002%2Fcpdd.1090 https://www.ncbi.nlm.nih.gov/pubmed/35355447 https://www.proquest.com/docview/2656015335 https://search.proquest.com/docview/2645856747 https://pubmed.ncbi.nlm.nih.gov/PMC9310628
Volume	11
hasFullText	1
inHoldings	1
isFullTextHit
isPrint
link	http://utb.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwjZ3LT9tAEIdHCC69VH3XLUULqlAPWKz3YcfqCQhRqATKAaTcrH1ZICoH1eHAf9-Zdew0QpW4OdpJvM54Zn-73vkM8L2QnpeG8zQrCp0qHIJSO6qLNHeFId6X1PHVCZdX-fRG_Zrr-Rb87GthOj7EsOBGkRHzNQW4se3xGhrqHrwnGBLO13eIGEPgfKFmwwILgUayyPYWWc5TjKN5Txbi4nj49uZ49ExkPt8r-a-GjYPQ5A28XqlHdtK5-y1sheYdHM46_PTTEbteV1O1R-yQzdZg6qf3cNt_vMeLJxO2qNnYUA6lMqolM41nl2GJ9wVVJrfsrmEXQ8FWy2jNll2RyP0dTS8wlWDG9GwaaF-2YxMcJMnRH-Bmcn59Nk1Xb1pInVKSp95J5Yg0p0ei1lJITMc1H6nMK-6EEaHIM28NBj-X2ltphBM1N7n1BLdGEfIRtptFEz4DK5XDn8GJZvC5crYslQ7W15k03FptfQIH_f9dPXRAjapDJ4uKnEKPxHkCu70nqlVMtZUgThDJU53A_tCM0UCPOEwTFo9ko3D-gz0qEvjUOW44i9Skrail2HDpYECk7c2W5u42ErdLFMG5GCXwIzr__x2vzmbjMR18ebnpV3glqKYi7qLche3ln8fwDZXO0u7FO3oPdk5Ox6eTvzgW_Dc
link.rule.ids	230,315,783,787,888,11574,27936,27937,46064,46488
linkProvider	Wiley-Blackwell
linkToHtml	http://utb.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwjZ3Lb9NAEIdHVTnABfHGUGBBqOJQq-t92LHEBTVECTRRDqmUm7Uvq1WRU5H00P-emXXsEFVI3GLtxLEzO7O_Xe98BvhcSM9Lw3maFYVOFQ5BqR3URZq7whDvS-r46oTpLB9fqB9LvTyAr10tTMuH6BfcKDJivqYApwXp0x011N14TzQknLA_UDl2ROI6q3m_wkKkkSzCvUWW8xQDadmhhbg47b-9PyDdU5n3N0v-LWLjKDR6Ao-38pF9a_39FA5C8wyO5y1_-u6ELXblVOsTdszmOzL13XO47A6v8e7JhK1qNjSURKmOasNM49k0bLBjUGnyml01bNJXbK0ZLdqyGancX9F0grkEU6Zn40Absx0b4ShJnn4BF6Pvi7Nxun3VQuqUkjz1TipHqDk9ELWWQmI-rvlAZV5xJ4wIRZ55azD6udTeSiOcqLnJrSe6NaqQl3DYrJrwGlipHJ4GZ5rB58rZslQ6WF9n0nBrtfUJfOr-7-qmJWpULTtZVOQUeibOEzjqPFFtg2pdCQIFkT7VCXzsmzEc6BmHacLqlmwUToDwiooEXrWO639FahJX1FLsubQ3INT2fktzdRmR2yWq4FwMEvgSnf_vC6_O5sMhfXjz_6Yf4OF4MT2vziezn2_hkaACi7il8ggON79vwzuUPRv7PvbuP_ln_jk
linkToPdf	http://utb.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwjZ3Lb9NAEIdHVZEQF8QbQ4EFoYpDra73YcfihBqiBGjkQyvlZu3LagVyIpIe-t8zs44dogqJm6OdxOuMZ_a3653PAB8L6XlpOE-zotCpwiEotaOmSHNXGOJ9SR1fnXA-z6eX6ttCLw7gc18L0_EhhgU3ioyYrynAV7453UFD3cp7giHhfP2eQhlO4HyhqmGBhUAjWWR7iyznKcbRoicLcXE6fHt_PLojMu_ulfxbw8ZBaPIIHm7VI_vSufsxHIT2CRxXHX769oRd7Kqp1ifsmFU7MPXtU7jqP_7EiycTtmzY2FAOpTKqDTOtZ-dhg_cFVSav2XXLZkPB1prRmi2bk8j9FU1nmEowY3o2DbQv27EJDpLk6GdwOfl6cTZNt29aSJ1SkqfeSeWINKdHotFSSEzHDR-pzCvuhBGhyDNvDQY_l9pbaYQTDTe59QS3RhHyHA7bZRteAiuVw5_BiWbwuXK2LJUO1jeZNNxabX0CH_r_u151QI26QyeLmpxCj8R5Ake9J-ptTK1rQZwgkqc6gfdDM0YDPeIwbVjekI3C-Q_2qEjgRee44SxSk7ailmLPpYMBkbb3W9rrq0jcLlEE52KUwKfo_H93vD6rxmM6ePX_pu_gfjWe1D9m8--v4YGg8oq4ofIIDje_b8IbFD0b-zbe3H8AT9T9WQ
openUrl	ctx_ver=Z39.88-2004&ctx_enc=info%3Aofi%2Fenc%3AUTF-8&rfr_id=info%3Asid%2Fsummon.serialssolutions.com&rft_val_fmt=info%3Aofi%2Ffmt%3Akev%3Amtx%3Ajournal&rft.genre=article&rft.atitle=Pharmacokinetics+of+Daprodustat+and+Metabolites+in+Individuals+with+Normal+and+Impaired+Hepatic+Function&rft.jtitle=Clinical+pharmacology+in+drug+development&rft.au=Mahar%2C+Kelly+M&rft.au=Shaddinger%2C+Bonnie+C&rft.au=Bandi+Ramanjineyulu&rft.au=Andrews%2C+Susan&rft.date=2022-05-01&rft.pub=Wiley+Subscription+Services%2C+Inc&rft.issn=2160-763X&rft.eissn=2160-7648&rft.volume=11&rft.issue=5&rft.spage=562&rft.epage=575&rft_id=info:doi/10.1002%2Fcpdd.1090&rft.externalDBID=NO_FULL_TEXT
thumbnail_l	http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/lc.gif&issn=2160-763X&client=summon
thumbnail_m	http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/mc.gif&issn=2160-763X&client=summon
thumbnail_s	http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/sc.gif&issn=2160-763X&client=summon