Bioequivalence of Eslicarbazepine Acetate from Two Different Sources of its Active Product Ingredient in Healthy Subjects

Purpose To compare the bioavailability (BA) and pharmacokinetic (PK) properties and to demonstrate the bioequivalence (BE) between two active product ingredient (API) sources of eslicarbazepine acetate (ESL) in healthy volunteers. Design, subjects and methods Forty healthy male and female subjects a...

Full description

Saved in:
Bibliographic Details
Published inDrugs in R&D Vol. 13; no. 2; pp. 137 - 143
Main Authors Falcão, Amílcar, Lima, Ricardo, Sousa, Rui, Nunes, Teresa, Soares-da-Silva, Patrício
Format Journal Article
LanguageEnglish
Published Cham Springer International Publishing AG 01.06.2013
Springer Nature B.V
Subjects
Adolescent
Adult
Anticonvulsants
Bioavailability
Bioequivalence
Biological Availability
Chemistry, Pharmaceutical
Convulsions & seizures
Cross-Over Studies
Dibenzazepines - adverse effects
Dibenzazepines - pharmacokinetics
Drug dosages
Female
Healthy Volunteers
Humans
Internal Medicine
Laboratories
Male
Medicine
Medicine & Public Health
Oral administration
Original
Original Research Article
Pharmacokinetics
Pharmacology/Toxicology
Pharmacotherapy
Plasma
Tablets
Therapeutic Equivalency
Urinalysis
Variance analysis
Vital signs
United States > US
Geometric Mean Ratio
Dosage Strength
Active Pharmaceutical Ingredient
Maximum Observe Plasma Concentration
Eslicarbazepine Acetate
Online AccessGet full text
ISSN1174-5886
1179-6901
1179-6901
DOI10.1007/s40268-013-0016-6

Cover

Abstract Purpose To compare the bioavailability (BA) and pharmacokinetic (PK) properties and to demonstrate the bioequivalence (BE) between two active product ingredient (API) sources of eslicarbazepine acetate (ESL) in healthy volunteers. Design, subjects and methods Forty healthy male and female subjects aged 18–40 years were randomized to treatment with 400 or 800 mg ESL marketed (MF) formulation [current active pharmaceutical ingredient (API) source] and 400 or 800 mg ESL to-be-marketed (TBM) formulation (new API source) under a gender-balanced, two-period, two-sequence crossover open-label study design. Subjects were assigned to receive either 400 or 800 mg ESL dose strengths, and each was randomly administered on two occasions—either a single oral tablet of MF or a single oral tablet of TBM—separated by a washout period of at least 7 days. Formulations were to be considered bioequivalent if, for both 400 or 800 mg ESL dosage strengths, the test (TBM)/reference (MF) geometric mean ratios (GMR) and 90 % confidence intervals (90 % CI) of the area under the plasma concentration-time curve (AUC) and peak plasma concentration ( C max ) were within the predetermined range of 80–125 %. Results Test/reference GMR (90 % CI) for the C max and AUC was respectively 100 % (94–109 %) and 96 % (94–98 %) following 400 mg ESL and 100 % (95–105 %) and 100 % (97–103 %) following 800 mg ESL. Conclusion Oral tablet formulations of either 400 or 800 mg ESL from the new API source were found to be bioequivalent to the corresponding marketed Zebinix ® formulation according to the regulatory definition of bioequivalence.
AbstractList To compare the bioavailability (BA) and pharmacokinetic (PK) properties and to demonstrate the bioequivalence (BE) between two active product ingredient (API) sources of eslicarbazepine acetate (ESL) in healthy volunteers.PURPOSETo compare the bioavailability (BA) and pharmacokinetic (PK) properties and to demonstrate the bioequivalence (BE) between two active product ingredient (API) sources of eslicarbazepine acetate (ESL) in healthy volunteers.Forty healthy male and female subjects aged 18-40 years were randomized to treatment with 400 or 800 mg ESL marketed (MF) formulation [current active pharmaceutical ingredient (API) source] and 400 or 800 mg ESL to-be-marketed (TBM) formulation (new API source) under a gender-balanced, two-period, two-sequence crossover open-label study design. Subjects were assigned to receive either 400 or 800 mg ESL dose strengths, and each was randomly administered on two occasions--either a single oral tablet of MF or a single oral tablet of TBM--separated by a washout period of at least 7 days. Formulations were to be considered bioequivalent if, for both 400 or 800 mg ESL dosage strengths, the test (TBM)/reference (MF) geometric mean ratios (GMR) and 90% confidence intervals (90% CI) of the area under the plasma concentration-time curve (AUC) and peak plasma concentration (Cmax) were within the predetermined range of 80-125%.DESIGN, SUBJECTS AND METHODSForty healthy male and female subjects aged 18-40 years were randomized to treatment with 400 or 800 mg ESL marketed (MF) formulation [current active pharmaceutical ingredient (API) source] and 400 or 800 mg ESL to-be-marketed (TBM) formulation (new API source) under a gender-balanced, two-period, two-sequence crossover open-label study design. Subjects were assigned to receive either 400 or 800 mg ESL dose strengths, and each was randomly administered on two occasions--either a single oral tablet of MF or a single oral tablet of TBM--separated by a washout period of at least 7 days. Formulations were to be considered bioequivalent if, for both 400 or 800 mg ESL dosage strengths, the test (TBM)/reference (MF) geometric mean ratios (GMR) and 90% confidence intervals (90% CI) of the area under the plasma concentration-time curve (AUC) and peak plasma concentration (Cmax) were within the predetermined range of 80-125%.Test/reference GMR (90% CI) for the Cmax and AUC was respectively 100% (94-109%) and 96% (94-98%) following 400 mg ESL and 100% (95-105%) and 100% (97-103%) following 800 mg ESL.RESULTSTest/reference GMR (90% CI) for the Cmax and AUC was respectively 100% (94-109%) and 96% (94-98%) following 400 mg ESL and 100% (95-105%) and 100% (97-103%) following 800 mg ESL.Oral tablet formulations of either 400 or 800 mg ESL from the new API source were found to be bioequivalent to the corresponding marketed Zebinix® formulation according to the regulatory definition of bioequivalence.CONCLUSIONOral tablet formulations of either 400 or 800 mg ESL from the new API source were found to be bioequivalent to the corresponding marketed Zebinix® formulation according to the regulatory definition of bioequivalence.
To compare the bioavailability (BA) and pharmacokinetic (PK) properties and to demonstrate the bioequivalence (BE) between two active product ingredient (API) sources of eslicarbazepine acetate (ESL) in healthy volunteers. Forty healthy male and female subjects aged 18-40 years were randomized to treatment with 400 or 800 mg ESL marketed (MF) formulation [current active pharmaceutical ingredient (API) source] and 400 or 800 mg ESL to-be-marketed (TBM) formulation (new API source) under a gender-balanced, two-period, two-sequence crossover open-label study design. Subjects were assigned to receive either 400 or 800 mg ESL dose strengths, and each was randomly administered on two occasions--either a single oral tablet of MF or a single oral tablet of TBM--separated by a washout period of at least 7 days. Formulations were to be considered bioequivalent if, for both 400 or 800 mg ESL dosage strengths, the test (TBM)/reference (MF) geometric mean ratios (GMR) and 90% confidence intervals (90% CI) of the area under the plasma concentration-time curve (AUC) and peak plasma concentration (Cmax) were within the predetermined range of 80-125%. Test/reference GMR (90% CI) for the Cmax and AUC was respectively 100% (94-109%) and 96% (94-98%) following 400 mg ESL and 100% (95-105%) and 100% (97-103%) following 800 mg ESL. Oral tablet formulations of either 400 or 800 mg ESL from the new API source were found to be bioequivalent to the corresponding marketed Zebinix® formulation according to the regulatory definition of bioequivalence.
To compare the bioavailability (BA) and pharmacokinetic (PK) properties and to demonstrate the bioequivalence (BE) between two active product ingredient (API) sources of eslicarbazepine acetate (ESL) in healthy volunteers. Forty healthy male and female subjects aged 18-40 years were randomized to treatment with 400 or 800 mg ESL marketed (MF) formulation [current active pharmaceutical ingredient (API) source] and 400 or 800 mg ESL to-be-marketed (TBM) formulation (new API source) under a gender-balanced, two-period, two-sequence crossover open-label study design. Subjects were assigned to receive either 400 or 800 mg ESL dose strengths, and each was randomly administered on two occasions--either a single oral tablet of MF or a single oral tablet of TBM--separated by a washout period of at least 7 days. Formulations were to be considered bioequivalent if, for both 400 or 800 mg ESL dosage strengths, the test (TBM)/reference (MF) geometric mean ratios (GMR) and 90% confidence intervals (90% CI) of the area under the plasma concentration-time curve (AUC) and peak plasma concentration (Cmax) were within the predetermined range of 80-125%. Test/reference GMR (90% CI) for the Cmax and AUC was respectively 100% (94-109%) and 96% (94-98%) following 400 mg ESL and 100% (95-105%) and 100% (97-103%) following 800 mg ESL. Oral tablet formulations of either 400 or 800 mg ESL from the new API source were found to be bioequivalent to the corresponding marketed Zebinix® formulation according to the regulatory definition of bioequivalence.
Purpose To compare the bioavailability (BA) and pharmacokinetic (PK) properties and to demonstrate the bioequivalence (BE) between two active product ingredient (API) sources of eslicarbazepine acetate (ESL) in healthy volunteers. Design, subjects and methods Forty healthy male and female subjects aged 18–40 years were randomized to treatment with 400 or 800 mg ESL marketed (MF) formulation [current active pharmaceutical ingredient (API) source] and 400 or 800 mg ESL to-be-marketed (TBM) formulation (new API source) under a gender-balanced, two-period, two-sequence crossover open-label study design. Subjects were assigned to receive either 400 or 800 mg ESL dose strengths, and each was randomly administered on two occasions—either a single oral tablet of MF or a single oral tablet of TBM—separated by a washout period of at least 7 days. Formulations were to be considered bioequivalent if, for both 400 or 800 mg ESL dosage strengths, the test (TBM)/reference (MF) geometric mean ratios (GMR) and 90 % confidence intervals (90 % CI) of the area under the plasma concentration-time curve (AUC) and peak plasma concentration ( C max ) were within the predetermined range of 80–125 %. Results Test/reference GMR (90 % CI) for the C max and AUC was respectively 100 % (94–109 %) and 96 % (94–98 %) following 400 mg ESL and 100 % (95–105 %) and 100 % (97–103 %) following 800 mg ESL. Conclusion Oral tablet formulations of either 400 or 800 mg ESL from the new API source were found to be bioequivalent to the corresponding marketed Zebinix ® formulation according to the regulatory definition of bioequivalence.
PurposeTo compare the bioavailability (BA) and pharmacokinetic (PK) properties and to demonstrate the bioequivalence (BE) between two active product ingredient (API) sources of eslicarbazepine acetate (ESL) in healthy volunteers.Design, subjects and methodsForty healthy male and female subjects aged 18–40 years were randomized to treatment with 400 or 800 mg ESL marketed (MF) formulation [current active pharmaceutical ingredient (API) source] and 400 or 800 mg ESL to-be-marketed (TBM) formulation (new API source) under a gender-balanced, two-period, two-sequence crossover open-label study design. Subjects were assigned to receive either 400 or 800 mg ESL dose strengths, and each was randomly administered on two occasions—either a single oral tablet of MF or a single oral tablet of TBM—separated by a washout period of at least 7 days. Formulations were to be considered bioequivalent if, for both 400 or 800 mg ESL dosage strengths, the test (TBM)/reference (MF) geometric mean ratios (GMR) and 90 % confidence intervals (90 % CI) of the area under the plasma concentration-time curve (AUC) and peak plasma concentration (Cmax) were within the predetermined range of 80–125 %.ResultsTest/reference GMR (90 % CI) for the Cmax and AUC was respectively 100 % (94–109 %) and 96 % (94–98 %) following 400 mg ESL and 100 % (95–105 %) and 100 % (97–103 %) following 800 mg ESL.ConclusionOral tablet formulations of either 400 or 800 mg ESL from the new API source were found to be bioequivalent to the corresponding marketed Zebinix® formulation according to the regulatory definition of bioequivalence.
Author Sousa, Rui
Nunes, Teresa
Falcão, Amílcar
Soares-da-Silva, Patrício
Lima, Ricardo
Author_xml – sequence: 1
  givenname: Amílcar
  surname: Falcão
  fullname: Falcão, Amílcar
  organization: Faculty of Pharmacy, University of Coimbra
– sequence: 2
  givenname: Ricardo
  surname: Lima
  fullname: Lima, Ricardo
  organization: Department of Research and Development, BIAL-Portela & Cª-S A
– sequence: 3
  givenname: Rui
  surname: Sousa
  fullname: Sousa, Rui
  organization: Department of Research and Development, BIAL-Portela & Cª-S A
– sequence: 4
  givenname: Teresa
  surname: Nunes
  fullname: Nunes, Teresa
  organization: Department of Research and Development, BIAL-Portela & Cª-S A
– sequence: 5
  givenname: Patrício
  surname: Soares-da-Silva
  fullname: Soares-da-Silva, Patrício
  email: psoares.silva@bial.com
  organization: Department of Research and Development, BIAL-Portela & Cª-S A, Department of Pharmacology and Therapeutics, Faculty of Medicine, University of Porto
BackLink https://www.ncbi.nlm.nih.gov/pubmed/23677811$$D View this record in MEDLINE/PubMed
BookMark eNp9kktv1DAUhSNURB_wA9ggS2zYBPyIH9kglVJopUogtawtx7meepSxp3YyaPrr6zClKpWoN7bk7xyf63sPq70QA1TVW4I_Eozlp9xgKlSNCasxJqIWL6oDQmRbixaTvT_npuZKif3qMOclLhAT6lW1T5mQUhFyUG2_-Ag3k9-YAYIFFB06zYO3JnXmFtY-ADq2MJoRkEtxha5-R_TVOwcJwogu45Qs5Fnlx1zI0W8A_Uyxn-yIzsMiQe9n0Ad0BmYYr7focuqWYMf8unrpzJDhzf1-VP36dnp1clZf_Ph-fnJ8UdumVWPdCMwbyXrlqAJnsWp50yuCqeXMUqI63knKhXRlGcEId9hx3jrGcNMyLtlR9Xnnu566FfS2xElm0OvkVyZtdTRe_3sT_LVexI0uX9W2mBeDD_cGKd5MkEe98tnCMJgAccqaMEmoxITQgr5_gi7LD4VSnmaUslbJphHPUaQRxQ4LPFPvHud-CPy3dwUgO8CmmHMC94AQrOf50Lv50KXrep4PPZvKJxrrS3N9nEv3w7NKulPm8kpYQHoU-r-iO_A4zgg
CitedBy_id crossref_primary_10_1007_s10928_018_9596_7
crossref_primary_10_1016_j_jchromb_2019_02_027
Cites_doi 10.1177/0091270008319706
10.1007/s00228-007-0414-1
10.1177/0091270004267591
10.1002/9781444316667.ch38
10.2165/0126839-200809060-00007
10.1016/S0920-1211(01)00231-5
10.1177/0091270005279364
10.1208/s12248-009-9142-z
10.1021/jm980627g
10.1111/j.1528-1167.2012.03519.x
10.1016/j.eplepsyres.2011.05.013
10.1002/bdd.549
10.1023/A:1011503032353
10.5414/CPP46119
10.25004/IJPSDR.2011.030206
ContentType Journal Article
Copyright The Author(s) 2013
Copyright Wolters Kluwer Health Adis International Jun 2013
Copyright Springer Nature B.V. Jun 2013
Copyright_xml – notice: The Author(s) 2013
– notice: Copyright Wolters Kluwer Health Adis International Jun 2013
– notice: Copyright Springer Nature B.V. Jun 2013
DBID C6C
AAYXX
CITATION
CGR
CUY
CVF
ECM
EIF
NPM
3V.
7X7
7XB
88E
8FI
8FJ
8FK
ABUWG
AFKRA
BENPR
CCPQU
FYUFA
GHDGH
K9.
M0S
M1P
PHGZM
PHGZT
PJZUB
PKEHL
PPXIY
PQEST
PQQKQ
PQUKI
PRINS
7X8
5PM
DOI 10.1007/s40268-013-0016-6
DatabaseName Springer Nature OA Free Journals
CrossRef
Medline
MEDLINE
MEDLINE (Ovid)
MEDLINE
MEDLINE
PubMed
ProQuest Central (Corporate)
Health & Medical Collection (ProQuest)
ProQuest Central (purchase pre-March 2016)
Medical Database (Alumni Edition)
Hospital Premium Collection
Hospital Premium Collection (Alumni Edition)
ProQuest Central (Alumni) (purchase pre-March 2016)
ProQuest Central (Alumni)
ProQuest Central UK/Ireland
ProQuest Central
ProQuest One Community College
Proquest Health Research Premium Collection
Health Research Premium Collection (Alumni)
ProQuest Health & Medical Complete (Alumni)
ProQuest Health & Medical Collection
Medical Database
ProQuest Central Premium
ProQuest One Academic (New)
ProQuest Health & Medical Research Collection
ProQuest One Academic Middle East (New)
ProQuest One Health & Nursing
ProQuest One Academic Eastern Edition (DO NOT USE)
ProQuest One Academic
ProQuest One Academic UKI Edition
ProQuest Central China
MEDLINE - Academic
PubMed Central (Full Participant titles)
DatabaseTitle CrossRef
MEDLINE
Medline Complete
MEDLINE with Full Text
PubMed
MEDLINE (Ovid)
ProQuest One Academic Middle East (New)
ProQuest One Academic Eastern Edition
ProQuest Health & Medical Complete (Alumni)
ProQuest Central (Alumni Edition)
ProQuest One Community College
ProQuest One Health & Nursing
ProQuest Hospital Collection
Health Research Premium Collection (Alumni)
ProQuest Central China
ProQuest Hospital Collection (Alumni)
ProQuest Central
ProQuest Health & Medical Complete
Health Research Premium Collection
ProQuest Medical Library
ProQuest One Academic UKI Edition
Health and Medicine Complete (Alumni Edition)
Health & Medical Research Collection
ProQuest Central (New)
ProQuest One Academic
ProQuest One Academic (New)
ProQuest Medical Library (Alumni)
ProQuest Central (Alumni)
ProQuest Health & Medical Research Collection
MEDLINE - Academic
DatabaseTitleList MEDLINE - Academic
MEDLINE
ProQuest One Academic Middle East (New)

ProQuest One Academic Middle East (New)
Database_xml – sequence: 1
  dbid: C6C
  name: SpringerOpen Free (Free internet resource, activated by CARLI)
  url: http://www.springeropen.com/
  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
– sequence: 4
  dbid: BENPR
  name: ProQuest Central
  url: https://www.proquest.com/central
  sourceTypes: Aggregation Database
DeliveryMethod fulltext_linktorsrc
Discipline Medicine
Pharmacy, Therapeutics, & Pharmacology
EISSN 1179-6901
EndPage 143
ExternalDocumentID PMC3689905
3136456051
23677811
10_1007_s40268_013_0016_6
Genre Randomized Controlled Trial
Research Support, Non-U.S. Gov't
Journal Article
GeographicLocations United States--US
GeographicLocations_xml – name: United States--US
GroupedDBID ---
-A0
.XZ
0R~
29G
2JY
36B
3V.
4.4
53G
5GY
6I2
7X7
88E
8FI
8FJ
8R4
8R5
AAKAS
AAKKN
ABDBF
ABEEZ
ABUWG
ABWHX
ACACY
ACGFS
ACUHS
ACULB
ADBBV
ADRAZ
ADZCM
AEYRQ
AFGXO
AFKRA
AHMBA
AHSBF
AHYZX
ALIPV
ALMA_UNASSIGNED_HOLDINGS
AMKLP
AOIJS
ASPBG
AVWKF
A~4
BAPOH
BAWUL
BCNDV
BENPR
BPHCQ
BVXVI
BYPQX
C24
C6C
CAG
CCPQU
COF
CS3
DIK
DU5
EAP
EBC
EBS
EJD
EMB
EMK
EMOBN
EPL
ESX
F5P
FYUFA
GROUPED_DOAJ
HMCUK
HYE
IAO
IEA
IHR
INH
INR
ITC
KQ8
M1P
M48
MK0
O9-
OAC
OB2
OK1
OVD
PQQKQ
PROAC
PSQYO
Q2X
R2J
RNS
RPM
RSV
RZALA
SISQX
SOJ
SV3
TEORI
TUS
UKHRP
W1D
YFH
~JE
AAYXX
ADGHP
CITATION
PHGZM
PHGZT
CGR
CUY
CVF
ECM
EIF
NPM
PJZUB
PPXIY
7XB
8FK
K9.
PKEHL
PQEST
PQUKI
PRINS
7X8
5PM
ID FETCH-LOGICAL-c498t-4605473d8f28efc08954d8102c53c218b5b72567ffffa6315f0f559f330493573
IEDL.DBID 7X7
ISSN 1174-5886
1179-6901
IngestDate Thu Aug 21 14:06:13 EDT 2025
Tue Aug 05 10:07:42 EDT 2025
Fri Jul 25 09:24:04 EDT 2025
Fri Jul 25 05:57:50 EDT 2025
Mon Jul 21 05:44:08 EDT 2025
Thu Apr 24 22:56:45 EDT 2025
Sun Jul 06 05:06:40 EDT 2025
Fri Feb 21 02:37:02 EST 2025
IsDoiOpenAccess true
IsOpenAccess true
IsPeerReviewed true
IsScholarly true
Issue 2
Keywords Geometric Mean Ratio
Dosage Strength
Active Pharmaceutical Ingredient
Maximum Observe Plasma Concentration
Eslicarbazepine Acetate
Language English
License http://creativecommons.org/licenses/by-nc/2.5
Open AccessThis article is distributed under the terms of the Creative Commons Attribution Noncommercial License which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and the source are credited.
LinkModel DirectLink
MergedId FETCHMERGED-LOGICAL-c498t-4605473d8f28efc08954d8102c53c218b5b72567ffffa6315f0f559f330493573
Notes ObjectType-Article-2
SourceType-Scholarly Journals-1
ObjectType-General Information-1
content type line 14
ObjectType-Feature-3
ObjectType-Article-1
ObjectType-Feature-2
content type line 23
ObjectType-Undefined-3
OpenAccessLink https://link.springer.com/10.1007/s40268-013-0016-6
PMID 23677811
PQID 1461370606
PQPubID 2034452
PageCount 7
ParticipantIDs pubmedcentral_primary_oai_pubmedcentral_nih_gov_3689905
proquest_miscellaneous_1371270112
proquest_journals_3223987446
proquest_journals_1461370606
pubmed_primary_23677811
crossref_primary_10_1007_s40268_013_0016_6
crossref_citationtrail_10_1007_s40268_013_0016_6
springer_journals_10_1007_s40268_013_0016_6
PublicationCentury 2000
PublicationDate 2013-06-01
PublicationDateYYYYMMDD 2013-06-01
PublicationDate_xml – month: 06
  year: 2013
  text: 2013-06-01
  day: 01
PublicationDecade 2010
PublicationPlace Cham
PublicationPlace_xml – name: Cham
– name: New Zealand
– name: Auckland
PublicationTitle Drugs in R&D
PublicationTitleAbbrev Drugs R D
PublicationTitleAlternate Drugs R D
PublicationYear 2013
Publisher Springer International Publishing AG
Springer Nature B.V
Publisher_xml – name: Springer International Publishing AG
– name: Springer Nature B.V
References Chow, Wang (CR21) 2001; 28
Soerensen, Pekcec, Potschka, Soares-da-Silva (CR13) 2011; 52
Midha, McKay (CR24) 2009; 11
Almeida, Falcao, Maia, Mazur, Gellert, Soares-da-Silva (CR28) 2005; 45
Pekcec, Potschka, Soares-da-Silva (CR12) 2011; 52
Almeida, Bialer, Soares-da-Silva, Shorvon, Perucca, Engel (CR3) 2009
Falcao, Maia, Almeida, Mazur, Gellert, Soares-da-Silva (CR5) 2007; 28
CR17
Almeida, Soares-da-Silva (CR19) 2004; 44
Hassan, Alfadly, Azmin, Peh, Tan, Noorizan (CR23) 2007; 48
Steinijans, Sauter, Hauschke, Diletti, Schall, Luus (CR22) 1995; 33
Rani, Pargal (CR25) 2004; 36
Almeida, Potgieter, Maia, Potgieter, Mota, Soares-da-Silva (CR6) 2008; 64
Almeida, Minciu, Nunes, Butoianu, Falcao, Magureanu (CR7) 2008; 48
Perucca, Elger, Halasz, Falcao, Almeida, Soares-da-Silva (CR9) 2011; 96
Torrao, Machado, Pires, Palma, Bonifacio, Wright (CR11) 2011; 52
CR27
CR26
Maia, Almeida, Falcão, Soares, Mota, Potgieter (CR8) 2008; 46
Sierra-Paredes, Sierra-Marcuno, Loureiro, Wright, Soares-da-Silva (CR14) 2011; 52
Hebeisen, Brady, Konrad, Soares-da-Silva (CR15) 2011; 52
Brady, Hebeisen, Konrad, Soares-da-Silva (CR16) 2011; 52
Fontes-Ribeiro, Macedo, Nunes, Neta, Vasconcelos, Cerdeira (CR20) 2008; 9
Benes, Parada, Figueiredo, Alves, Freitas, Learmonth (CR1) 1999; 42
Pires, Palma, Loureiro, Bonifacio, Wright, Soares-da-Silva (CR10) 2011; 52
Hainzl, Parada, Soares-da-Silva (CR2) 2001; 44
Shep, Nimkar, Shah, Jaiswal (CR18) 2011; 3
Bialer, Soares-da-Silva (CR4) 2012; 53
N Pires (16_CR10) 2011; 52
C Fontes-Ribeiro (16_CR20) 2008; 9
L Torrao (16_CR11) 2011; 52
J Maia (16_CR8) 2008; 46
Y Hassan (16_CR23) 2007; 48
G Sierra-Paredes (16_CR14) 2011; 52
VW Steinijans (16_CR22) 1995; 33
L Almeida (16_CR6) 2008; 64
SC Chow (16_CR21) 2001; 28
S Rani (16_CR25) 2004; 36
S Hebeisen (16_CR15) 2011; 52
D Shep (16_CR18) 2011; 3
A Pekcec (16_CR12) 2011; 52
16_CR26
D Hainzl (16_CR2) 2001; 44
16_CR27
K Brady (16_CR16) 2011; 52
L Almeida (16_CR19) 2004; 44
L Almeida (16_CR3) 2009
L Almeida (16_CR28) 2005; 45
M Bialer (16_CR4) 2012; 53
J Soerensen (16_CR13) 2011; 52
A Falcao (16_CR5) 2007; 28
L Almeida (16_CR7) 2008; 48
K Midha (16_CR24) 2009; 11
J Benes (16_CR1) 1999; 42
16_CR17
E Perucca (16_CR9) 2011; 96
References_xml – volume: 48
  start-page: 966
  issue: 8
  year: 2008
  end-page: 977
  ident: CR7
  article-title: Pharmacokinetics, efficacy, and tolerability of eslicarbazepine acetate in children and adolescents with epilepsy
  publication-title: J Clin Pharmacol
  doi: 10.1177/0091270008319706
– volume: 52
  start-page: 119
  issue: Suppl. 6
  year: 2011
  ident: CR14
  article-title: Effects of eslicarbazepine acetate on acute and chronic latrunculin A-induced seizures and extracellular amino acid levels in the mouse hippocampus
  publication-title: Epilepsia
– volume: 52
  start-page: 260
  issue: Suppl. 6
  year: 2011
  ident: CR16
  article-title: The effects of eslicarbazepine, -licarbazepine, oxcarbazepine and carbamazepine on ion transmission Ca 3.2 channels
  publication-title: Epilepsia
– volume: 52
  start-page: 257
  issue: Suppl. 6
  year: 2011
  ident: CR13
  article-title: The effects of eslicarbazepine acetate in the amygdala kindling model of temporal lobe epilepsy
  publication-title: Epilepsia
– volume: 64
  start-page: 267
  issue: 3
  year: 2008
  end-page: 273
  ident: CR6
  article-title: Pharmacokinetics of eslicarbazepine acetate in patients with moderate hepatic impairment
  publication-title: Eur J Clin Pharmacol
  doi: 10.1007/s00228-007-0414-1
– volume: 44
  start-page: 906
  issue: 8
  year: 2004
  end-page: 918
  ident: CR19
  article-title: Safety, tolerability, and pharmacokinetic profile of BIA 2-093, a novel putative antiepileptic, in a rising multiple-dose study in young healthy humans
  publication-title: J Clin Pharmacol
  doi: 10.1177/0091270004267591
– volume: 52
  start-page: 257
  issue: Suppl. 6
  year: 2011
  ident: CR12
  article-title: Effects of eslicarbazepine acetate and its metabolites in the corneal kindling model of epilepsy
  publication-title: Epilepsia
– volume: 46
  start-page: 119
  issue: 3
  year: 2008
  end-page: 130
  ident: CR8
  article-title: Effect of renal impairment on the pharmacokinetics of eslicarbazepine acetate
  publication-title: Int J Clin Pharmacol Ther
– start-page: 485
  year: 2009
  end-page: 498
  ident: CR3
  article-title: Eslicarbazepine acetate
  publication-title: The treatment of epilepsy
  doi: 10.1002/9781444316667.ch38
– volume: 9
  start-page: 447
  issue: 6
  year: 2008
  end-page: 454
  ident: CR20
  article-title: Dosage form proportionality and food effect of the final tablet formulation of eslicarbazepine acetate: randomized, open-label, crossover, single-centre study in healthy volunteers
  publication-title: Drugs R D
  doi: 10.2165/0126839-200809060-00007
– ident: CR27
– volume: 44
  start-page: 197
  issue: 2–3
  year: 2001
  end-page: 206
  ident: CR2
  article-title: Metabolism of two new antiepileptic drugs and their principal metabolites (+)- and (−)-10,11-dihydro-10-hydroxy carbamazepine
  publication-title: Epilepsy Res
  doi: 10.1016/S0920-1211(01)00231-5
– volume: 45
  start-page: 1062
  issue: 9
  year: 2005
  end-page: 1066
  ident: CR28
  article-title: Single-dose and steady-state pharmacokinetics of eslicarbazepine acetate (BIA 2-093) in healthy elderly and young subjects
  publication-title: J Clin Pharmacol
  doi: 10.1177/0091270005279364
– volume: 52
  start-page: 257
  issue: Suppl. 6
  year: 2011
  end-page: 258
  ident: CR15
  article-title: Inhibitory effects of eslicarbazepine acetate and its metabolites against neuronal voltage-gated sodium channels
  publication-title: Epilepsia
– volume: 3
  start-page: 101
  issue: 2
  year: 2011
  end-page: 103
  ident: CR18
  article-title: Comparative bioavailability study with two sodium valproate tablet formulations in healthy subjects
  publication-title: Int J Pharma Sci Drug Res
– volume: 52
  start-page: 118
  issue: Suppl. 6
  year: 2011
  ident: CR10
  article-title: Effects of eslicarbazepine acetate, eslicarbazepine, carbamazepine and oxcarbazepine in the maximal electroconvulsive shock test in the mice
  publication-title: Epilepsia
– volume: 11
  start-page: 664
  issue: 4
  year: 2009
  end-page: 670
  ident: CR24
  article-title: Bioequivalence; its history, practice, and future
  publication-title: AAPS J
  doi: 10.1208/s12248-009-9142-z
– volume: 42
  start-page: 2582
  issue: 14
  year: 1999
  end-page: 2587
  ident: CR1
  article-title: Anticonvulsant and sodium channel-blocking properties of novel 10,11-dihydro-5H-dibenz[b,f]azepine-5-carboxamide derivatives
  publication-title: J Med Chem
  doi: 10.1021/jm980627g
– volume: 52
  start-page: 118
  issue: Suppl. 6
  year: 2011
  end-page: 119
  ident: CR11
  article-title: Effects of eslicarbazepine acetate, eslicarbazepine, carbamazepine and oxcarbazepine in the 6-HZ psychomotor seizure model in the mice
  publication-title: Epilepsia
– ident: CR17
– volume: 53
  start-page: 935
  issue: 6
  year: 2012
  end-page: 946
  ident: CR4
  article-title: Pharmacokinetics and drug interactions of eslicarbazepine acetate
  publication-title: Epilepsia
  doi: 10.1111/j.1528-1167.2012.03519.x
– volume: 48
  start-page: 819
  year: 2007
  end-page: 823
  ident: CR23
  article-title: Bioequivalence evaluation of two different formulations of ciprofloxacin tablets in healthy volunteers
  publication-title: Singap Med J
– volume: 96
  start-page: 132
  issue: 1–2
  year: 2011
  end-page: 139
  ident: CR9
  article-title: Pharmacokinetics of eslicarbazepine acetate at steady-state in adults with partial-onset seizures
  publication-title: Epilepsy Res
  doi: 10.1016/j.eplepsyres.2011.05.013
– volume: 36
  start-page: 209
  issue: 4
  year: 2004
  end-page: 216
  ident: CR25
  article-title: Bioequivalence: an overview of statistical concepts
  publication-title: Indian J Pharmacol
– volume: 28
  start-page: 249
  issue: 5
  year: 2007
  end-page: 256
  ident: CR5
  article-title: Effect of gender on the pharmacokinetics of eslicarbazepine acetate (BIA 2–093), a new voltage-gated sodium channel blocker
  publication-title: Biopharm Drug Dispos
  doi: 10.1002/bdd.549
– volume: 33
  start-page: 427
  issue: 8
  year: 1995
  end-page: 430
  ident: CR22
  article-title: Reference tables for the intrasubject coefficient of variation in bioequivalence studies
  publication-title: Int J Clin Pharmacol Therapeut
– ident: CR26
– volume: 28
  start-page: 155
  issue: 2
  year: 2001
  end-page: 169
  ident: CR21
  article-title: On sample size calculation in bioequivalence trials
  publication-title: J Pharmacokinet Pharmacodyn
  doi: 10.1023/A:1011503032353
– volume: 52
  start-page: 260
  issue: Suppl. 6
  year: 2011
  ident: 16_CR16
  publication-title: Epilepsia
– volume: 48
  start-page: 966
  issue: 8
  year: 2008
  ident: 16_CR7
  publication-title: J Clin Pharmacol
  doi: 10.1177/0091270008319706
– volume: 52
  start-page: 118
  issue: Suppl. 6
  year: 2011
  ident: 16_CR10
  publication-title: Epilepsia
– volume: 52
  start-page: 118
  issue: Suppl. 6
  year: 2011
  ident: 16_CR11
  publication-title: Epilepsia
– ident: 16_CR17
– volume: 28
  start-page: 155
  issue: 2
  year: 2001
  ident: 16_CR21
  publication-title: J Pharmacokinet Pharmacodyn
  doi: 10.1023/A:1011503032353
– volume: 46
  start-page: 119
  issue: 3
  year: 2008
  ident: 16_CR8
  publication-title: Int J Clin Pharmacol Ther
  doi: 10.5414/CPP46119
– volume: 44
  start-page: 906
  issue: 8
  year: 2004
  ident: 16_CR19
  publication-title: J Clin Pharmacol
  doi: 10.1177/0091270004267591
– volume: 28
  start-page: 249
  issue: 5
  year: 2007
  ident: 16_CR5
  publication-title: Biopharm Drug Dispos
  doi: 10.1002/bdd.549
– ident: 16_CR27
– volume: 52
  start-page: 257
  issue: Suppl. 6
  year: 2011
  ident: 16_CR15
  publication-title: Epilepsia
– volume: 44
  start-page: 197
  issue: 2–3
  year: 2001
  ident: 16_CR2
  publication-title: Epilepsy Res
  doi: 10.1016/S0920-1211(01)00231-5
– volume: 11
  start-page: 664
  issue: 4
  year: 2009
  ident: 16_CR24
  publication-title: AAPS J
  doi: 10.1208/s12248-009-9142-z
– volume: 36
  start-page: 209
  issue: 4
  year: 2004
  ident: 16_CR25
  publication-title: Indian J Pharmacol
– volume: 52
  start-page: 257
  issue: Suppl. 6
  year: 2011
  ident: 16_CR13
  publication-title: Epilepsia
– volume: 45
  start-page: 1062
  issue: 9
  year: 2005
  ident: 16_CR28
  publication-title: J Clin Pharmacol
  doi: 10.1177/0091270005279364
– volume: 52
  start-page: 119
  issue: Suppl. 6
  year: 2011
  ident: 16_CR14
  publication-title: Epilepsia
– volume: 52
  start-page: 257
  issue: Suppl. 6
  year: 2011
  ident: 16_CR12
  publication-title: Epilepsia
– volume: 33
  start-page: 427
  issue: 8
  year: 1995
  ident: 16_CR22
  publication-title: Int J Clin Pharmacol Therapeut
– volume: 42
  start-page: 2582
  issue: 14
  year: 1999
  ident: 16_CR1
  publication-title: J Med Chem
  doi: 10.1021/jm980627g
– start-page: 485
  volume-title: The treatment of epilepsy
  year: 2009
  ident: 16_CR3
  doi: 10.1002/9781444316667.ch38
– ident: 16_CR26
– volume: 53
  start-page: 935
  issue: 6
  year: 2012
  ident: 16_CR4
  publication-title: Epilepsia
  doi: 10.1111/j.1528-1167.2012.03519.x
– volume: 9
  start-page: 447
  issue: 6
  year: 2008
  ident: 16_CR20
  publication-title: Drugs R D
  doi: 10.2165/0126839-200809060-00007
– volume: 48
  start-page: 819
  year: 2007
  ident: 16_CR23
  publication-title: Singap Med J
– volume: 64
  start-page: 267
  issue: 3
  year: 2008
  ident: 16_CR6
  publication-title: Eur J Clin Pharmacol
  doi: 10.1007/s00228-007-0414-1
– volume: 3
  start-page: 101
  issue: 2
  year: 2011
  ident: 16_CR18
  publication-title: Int J Pharma Sci Drug Res
  doi: 10.25004/IJPSDR.2011.030206
– volume: 96
  start-page: 132
  issue: 1–2
  year: 2011
  ident: 16_CR9
  publication-title: Epilepsy Res
  doi: 10.1016/j.eplepsyres.2011.05.013
SSID ssj0001368
Score 1.9401809
Snippet Purpose To compare the bioavailability (BA) and pharmacokinetic (PK) properties and to demonstrate the bioequivalence (BE) between two active product...
To compare the bioavailability (BA) and pharmacokinetic (PK) properties and to demonstrate the bioequivalence (BE) between two active product ingredient (API)...
PurposeTo compare the bioavailability (BA) and pharmacokinetic (PK) properties and to demonstrate the bioequivalence (BE) between two active product ingredient...
SourceID pubmedcentral
proquest
pubmed
crossref
springer
SourceType Open Access Repository
Aggregation Database
Index Database
Enrichment Source
Publisher
StartPage 137
SubjectTerms Adolescent
Adult
Anticonvulsants
Bioavailability
Bioequivalence
Biological Availability
Chemistry, Pharmaceutical
Convulsions & seizures
Cross-Over Studies
Dibenzazepines - adverse effects
Dibenzazepines - pharmacokinetics
Drug dosages
Female
Healthy Volunteers
Humans
Internal Medicine
Laboratories
Male
Medicine
Medicine & Public Health
Oral administration
Original
Original Research Article
Pharmacokinetics
Pharmacology/Toxicology
Pharmacotherapy
Plasma
Tablets
Therapeutic Equivalency
Urinalysis
Variance analysis
Vital signs
SummonAdditionalLinks – databaseName: Scholars Portal Journals: Open Access
  dbid: M48
  link: http://utb.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwfV1LT9wwEB5Reuml6oO2KVC5UsWB4mo3juP4gCpaQLQSaKXuStyiPGwRCSWwyYqmv74zeW23LORqO3IyY_sbz8w3AJ-skIkWRnLEGoJ749TwGGE3d2Wk3FQjiDZNtMWFfzbzfl7Kyw3oy1t1P7Bca9pRPanZ_PrL79v6Ky74wyENDm0gn0KyBCcEw_0n8BQPJkWVHM69JXn4WPhB79hcN2z1aLqHN--HTf7nO22OpNMX8LzDkuyoFf5L2DD5K9ibtGTU9QGbLnOrygO2xyZLmur6NdTfssLcLjJUNVrdrLDspKQrvHkc_TE3iD7ZUULBiIZRDgqb3hXsuCunUrFfzaV_SaOyqsSetG2yScsfy37kaMZTLFnFspy1qU41w02Kbn3KLZidnky_n_GuEANPPB1UnHynnhJpYN3A2GQUaOmlAUKTRIoEMUIsY4XQSVl8Il-MpR1ZtFQs3ZVoIZV4A5t5kZt3wGQirZKkIVI3LtlIKa1t6sYIHbxIOTDqZRAmHUs5Fcu4Dgd-5UZsIYqN4vH80Hdgfxhy01J0PNZ5pxds2CsbmT9jQTRC65txzxOaygRg88ehGZch-Vai3BQLfIVQ5MNH9OrA21ZNhskQSR4l9DqgVhRo6EAU36steXbVUH2jxiJckA587lXtn1k_9I3vH_-IbXjmtjU9UPd3YLOaL8wuIqsq_tCsl78NXR6j
  priority: 102
  providerName: Scholars Portal
– databaseName: SpringerLINK
  dbid: C24
  link: http://utb.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwlV3dS9xAEB-shdIXqfYrVssUig-tC3fZbDb7aK2ihZaDnuBbyMcuBkqiJoecf70z-bJXbaH3upslx3zkNzszvwH46KTKjLRKENaQIpjmVqQEu4WvEu3nhkC0bastfoQnZ8G3c3Xe93HXQ7X7kJJsPfXY7EaRTsiFV1IwThHhE3iqKHTnOr5DbnHo3e9Udv1vBLWFiqJwSGU-dsTqx-gBwnxYKPlHtrT9CB2_gI0ePeJBJ-5NWLPlFjz73ufHt2Bv1jFRL_dxft9YVe_jHs7uOaqXL2H5pajs1aIgPWPTxsrhUc33d9dpcmsv6TA8yLgS0SI3oOD8psKv_SyVBn-2N_41P1U0Ne1kn4mzjjwWT0uK4bmQrMGixK7PaYnkofjKp34FZ8dH88MT0U9hEFlgokZw4jTQMo-cH1mXTSKjgjwiXJIpmRFASFWqCTdpR78klFPlJo7CFMcXJUYqLV_DelmV9i2gypTTitVDmTYfm2htjMv9lHBDkGgPJoM44qynKOdJGb_ikVy5lWBMEuRivDAOPfg0PnLZ8XP8a_POIOO4N9WaY5-pZA6hx5fJ4UnDMwJo-cO4TDbIiZWktNWCjpCaE_gEXT1402nM-DLMkMfdvB7oFV0aNzC_9-pKWVy0PN-kyIQVlAefB6377a3_9h-3_2v3O3jud_M9yCp2YL25XthdQllN-r61qjtz7B0K
  priority: 102
  providerName: Springer Nature
Title Bioequivalence of Eslicarbazepine Acetate from Two Different Sources of its Active Product Ingredient in Healthy Subjects
URI https://link.springer.com/article/10.1007/s40268-013-0016-6
https://www.ncbi.nlm.nih.gov/pubmed/23677811
https://www.proquest.com/docview/1461370606
https://www.proquest.com/docview/3223987446
https://www.proquest.com/docview/1371270112
https://pubmed.ncbi.nlm.nih.gov/PMC3689905
Volume 13
hasFullText 1
inHoldings 1
isFullTextHit
isPrint
link http://utb.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwfV3da9RAEB-0ffFF_Da2HitIH7SLd9lsNnmS9rxSBcuhV7i3kGx2MSDJtclRzr_emc3HeVabh0DYTUiY2c1vvn4D8NYKqWNhJEesIXgwyQ3PEHZzX6bKz2ME0cZlW1yE55fBl6Vcdg63ukur7PdEt1HnlSYf-QdUPBETV3v4cXXFqWsURVe7Fhr3YZ-oy8j4UsvB4CI6sqiPZFK5HNpKIaVuCU5Ih4e7_6JbAPN2nuRfwVL3Dzp7BA878MhOWmk_hnumfAJH85Z9enPMFttiqvqYHbH5lpd68xQ2p0VlrtYF6hYtZ1ZZNqvJZ3edpb_MCuEmO9GUfWgYFZ2wxU3FPnX9Uxr23Xn5a7qraGqcSfskm7eEsexziXY7JY81rChZW9u0YbgrkZunfgaXZ7PF9Jx3nRe4DuKo4RQsDZTII-tHxupxFMsgjxCLaCk0goJMZgqxkrJ4pKGYSDu2aJpYco7EQirxHPbKqjQvgUktrZKkEjJ2MdhUqTi2uZ8hVghS5cG4l0GiO1py6o7xMxkIlZ3YEhQbJeCFSejBu-GWVcvJcdfkw16wSbc8a7J3JoJ4g_49vNU1D94Mw7juKJiSlqZa4yOEoqA9wlUPXrRqMrwMseJRBa8HakeBhgnE6b07UhY_HLc3aiziA-nB-17V_njr_33jq7s_4gAe-G0TD9T9Q9hrrtfmNUKpJhu59TKC_dPZxfwbXk39gM7hdOScE3j-GkS_ARFOINM
linkProvider ProQuest
linkToHtml http://utb.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwtV1Lb9NAEB6V9AAXxBuXAosEPUBXJF6v1z4g1NJUCS1RBKnUm-vHmlpCdho7qsyP4jcy41cIhd7q69qWrfl29tudmW8AXsdChq7QkiPXENwaRJoHSLu5KX1lRi6SaF1lW0zs0Yn1-VSebsCvthaG0ipbn1g56igL6Yz8PQJPuKTVbn-cX3DqGkXR1baFRg2LI11e4pYt_zA-QPu-Mc3D4ezTiDddBXhouU7BKRBoKRE5senoOOw7rrQiB9fZUIoQF7xABgp5gIrx8m0xkHE_Rtod08bfFVIJfO8t2LQEUoUebO4PJ9Ovne8fCNtpY6dUoIe7M5uSxQQnbsXt9dXvCqW9mpn5V3i2WvUO78Hdhq6yvRpf92FDpw9gZ1rrXZe7bLYq38p32Q6brpSwy4dQ7ieZvlgmiGZyICyL2TCnU8JF4P_UcyS4bC-kfEfNqMyFzS4zdtB0bCnYtyqukNNTSZHjneSZ2bSWqGXj9PtCU7pawZKU1dVUJUM_SAdL-SM4uRGrPIZemqX6KTAZylhJAqF0q6ivr5TrxpEZIDuxfGVAv7WBFzZC6NSP44fXSThXZvPQbJTyZ3u2AW-7R-a1Csh1N2-3hvUah5DTDmsgSKno38MrdBvwqhvGmU7hGz_V2RJfIRSlCSBBNuBJDZPuY0iHj2qGDVBrAOpuIBXx9ZE0Oa_UxBGxyEikAe9aqP3x1f_7x63rf-Il3B7Nvhx7x-PJ0TO4Y9YtRHAebEOvWCz1cyRyRfCimT0Mzm56wv4GUNJXyA
linkToPdf http://utb.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwtV1Lb9QwEB6VIiEuiDeBAkaCHqBWd-M4Tg4IFbarLkXVSmylvaV52BAJJdtNVlX4afw6ZvJalkJvzdV2lGge_uyZ-QbgtREy9oWWHLGG4M4w0TxC2M1tGSo78RFE6zrb4sQ9OnU-z-V8C351tTCUVtn5xNpRJ3lMd-T7qHjCJ652d9-0aRHT0fjD4pxTBymKtHbtNBoVOdbVBR7fiveTEcr6jW2PD2efjnjbYYDHju-VnIKCjhKJZ2xPm3jg-dJJPNxzYyli3PwiGSnEBMrgE7piKM3AIAQ3dAngC6kEvvcG3FQCt020JTXvD3tEheZ1UVQq1cNzmktpY4ITyuLu5j54CdxeztH8K1Bb73_ju3CnBa7soNG0e7Cls_uwO22Yr6s9NlsXchV7bJdN15zY1QOoPqa5Pl-lqNfkSlhu2GFB94XLKPypFwh12UFMmY-aUcELm13kbNT2binZ1zrCUNCqtCxwJvloNm3Iatkk-7bUlLhWsjRjTV1VxdAj0hVT8RBOr0Umj2A7yzP9BJiMpVGS1FH6dfw3VMr3TWJHiFOcUFkw6GQQxC0lOnXm-BH0ZM612AIUGyX_uYFrwdt-yaLhA7lq8k4n2KB1DQWdtYaCOIv-PbzWcwte9cNo8xTICTOdr_AVQlHCAEJlCx43atJ_DDHyUfWwBWpDgfoJxCe-OZKl32tecdRYxCbSgnedqv3x1f_7x6dX_8RLuIVmGnyZnBw_g9t200sEzWAHtsvlSj9HRFdGL2rTYXB23bb6G5v4Wpg
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=Bioequivalence+of+Eslicarbazepine+Acetate+from+Two+Different+Sources+of+its+Active+Product+Ingredient+in+Healthy+Subjects&rft.jtitle=Drugs+in+R%26D&rft.au=Falc%C3%A3o%2C+Am%C3%ADlcar&rft.au=Lima%2C+Ricardo&rft.au=Sousa%2C+Rui&rft.au=Nunes%2C+Teresa&rft.date=2013-06-01&rft.pub=Springer+Nature+B.V&rft.eissn=1179-6901&rft.volume=13&rft.issue=2&rft.spage=137&rft.epage=143&rft_id=info:doi/10.1007%2Fs40268-013-0016-6&rft.externalDBID=HAS_PDF_LINK
thumbnail_l http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/lc.gif&issn=1174-5886&client=summon
thumbnail_m http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/mc.gif&issn=1174-5886&client=summon
thumbnail_s http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/sc.gif&issn=1174-5886&client=summon