Single ascending oral dose pharmacokinetics and pharmacodynamics study of EV-077: the specific inhibitor of prostanoid- and isoprostane-induced cellular activation
Purpose This study was performed to determine the oral pharmacokinetics (PK) of EV-077 and its effects on pharmacodynamic (PD) markers. EV-077 blocks prostanoid-induced and isoprostane-induced cellular activation, and is in development for the treatment of vascular inflammation and associated compli...
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| Veröffentlicht in: | European journal of clinical pharmacology 2013-03, Vol.69 (3), p.459-465 |
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| creator | Richardson, A. Sakariassen, K. S. Meyer, J.-P. Alberts, P. Sorensen, A. S. |
| description | Purpose
This study was performed to determine the oral pharmacokinetics (PK) of EV-077 and its effects on pharmacodynamic (PD) markers. EV-077 blocks prostanoid-induced and isoprostane-induced cellular activation, and is in development for the treatment of vascular inflammation and associated complications of type-2 diabetes..
Methods
This single-ascending-dose mono-centre study was randomised, placebo-controlled, and double-blinded within each dose group. Seven EV-077 doses were administered sequentially as an oral solution: 0.0125, 0.125, 0.375, 0.75, 1.25, 1.875 and 2.5 mg/kg body weight. PK, platelet aggregation, bleeding time and safety parameters were measured. Seven to eight healthy male subjects were dosed per group: five to six subjects received EV-077 and two subjects received placebo.
Results
Tmax was reached rapidly between 0.5 h and 1.0 h. Both Cmax and AUC increased linearly with the dose. The apparent terminal half-life (t½z) increased with the dose, most likely reflecting the increasing last quantifiable concentration with increasing dose; at 2.5 mg/kg, it was 2.7-6.9 h. Measurement of platelet aggregation showed no effect at 0.0125 mg/kg, and a full and reversible inhibition at doses of 0.125-2.5 mg/kg. The average bleeding time was dose-dependently prolonged, but was always below 9 min. The PK/PD profile showed that at plasma concentrations above 20 ng/ml, EV-077 platelet aggregation was completely inhibited (>90 %). All tested doses were well tolerated.
Conclusions
Orally administered EV-077 was well tolerated, readily absorbed, reached Cmax within 1 h, with a linear PK based on Cmax and AUC. The inhibition of platelet aggregation was complete and reversible at doses of 0.125 mg/kg and higher, and average bleeding time was below 9 min. |
| doi_str_mv | 10.1007/s00228-012-1348-9 |
| format | Article |
| fullrecord | <record><control><sourceid>proquest_cross</sourceid><recordid>TN_cdi_proquest_journals_1287354561</recordid><sourceformat>XML</sourceformat><sourcesystem>PC</sourcesystem><sourcerecordid>2891077381</sourcerecordid><originalsourceid>FETCH-LOGICAL-c402t-2c440a87047a750246c57a150fbd161de98658ed7f07e70653be50f87f5a3143</originalsourceid><addsrcrecordid>eNp1kcFu1DAQhi0EokvhAbggS4ijYZzYccINVaUgVeqhVa-W1550XbL2YjtI-zy8KE53KVx6sj3zzT8z_gl5y-EjB1CfMkDT9Ax4w3grejY8Iysu2voCwZ-TFUDLWTcoOCGvcr4H4HKA9iU5qVVcgoQV-X3tw92E1GSLwdU7jclM1MWMdLcxaWts_OEDFm8zNcE9Bt0-mO0SzGV2expHen7LQKnPtGyQ5h1aP3pLfdj4tS8xLcQuxVxMiN6xBy2f4zGEzAc3W3TU4jTNk0nU2OJ_meJjeE1ejGbK-OZ4npKbr-c3Z9_Y5dXF97Mvl8wKaAprrBBgegVCGSWhEZ2VytQ9x7XjHXc49J3s0akRFCroZLvGmuzVKE1bv-2UvD_I1pl-zpiLvo9zCrWj5k2vWilkxyvFD5Stk-eEo94lvzVprznoxRV9cEVXV_Tiih5qzbuj8rzeonus-GtDBT4cgeqDmcZkgvX5H6ekGlS7CDUHLtdUuMP034hPdv8D_NimdA</addsrcrecordid><sourcetype>Aggregation Database</sourcetype><iscdi>true</iscdi><recordtype>article</recordtype><pqid>1287354561</pqid></control><display><type>article</type><title>Single ascending oral dose pharmacokinetics and pharmacodynamics study of EV-077: the specific inhibitor of prostanoid- and isoprostane-induced cellular activation</title><source>MEDLINE</source><source>Springer Nature - Complete Springer Journals</source><creator>Richardson, A. ; Sakariassen, K. S. ; Meyer, J.-P. ; Alberts, P. ; Sorensen, A. S.</creator><creatorcontrib>Richardson, A. ; Sakariassen, K. S. ; Meyer, J.-P. ; Alberts, P. ; Sorensen, A. S.</creatorcontrib><description>Purpose
This study was performed to determine the oral pharmacokinetics (PK) of EV-077 and its effects on pharmacodynamic (PD) markers. EV-077 blocks prostanoid-induced and isoprostane-induced cellular activation, and is in development for the treatment of vascular inflammation and associated complications of type-2 diabetes..
Methods
This single-ascending-dose mono-centre study was randomised, placebo-controlled, and double-blinded within each dose group. Seven EV-077 doses were administered sequentially as an oral solution: 0.0125, 0.125, 0.375, 0.75, 1.25, 1.875 and 2.5 mg/kg body weight. PK, platelet aggregation, bleeding time and safety parameters were measured. Seven to eight healthy male subjects were dosed per group: five to six subjects received EV-077 and two subjects received placebo.
Results
Tmax was reached rapidly between 0.5 h and 1.0 h. Both Cmax and AUC increased linearly with the dose. The apparent terminal half-life (t½z) increased with the dose, most likely reflecting the increasing last quantifiable concentration with increasing dose; at 2.5 mg/kg, it was 2.7-6.9 h. Measurement of platelet aggregation showed no effect at 0.0125 mg/kg, and a full and reversible inhibition at doses of 0.125-2.5 mg/kg. The average bleeding time was dose-dependently prolonged, but was always below 9 min. The PK/PD profile showed that at plasma concentrations above 20 ng/ml, EV-077 platelet aggregation was completely inhibited (>90 %). All tested doses were well tolerated.
Conclusions
Orally administered EV-077 was well tolerated, readily absorbed, reached Cmax within 1 h, with a linear PK based on Cmax and AUC. The inhibition of platelet aggregation was complete and reversible at doses of 0.125 mg/kg and higher, and average bleeding time was below 9 min.</description><identifier>ISSN: 0031-6970</identifier><identifier>EISSN: 1432-1041</identifier><identifier>DOI: 10.1007/s00228-012-1348-9</identifier><identifier>PMID: 22815050</identifier><language>eng</language><publisher>Berlin/Heidelberg: Springer-Verlag</publisher><subject>Administration, Oral ; Adult ; Area Under Curve ; Biological and medical sciences ; Biomedical and Life Sciences ; Biomedicine ; Bleeding Time ; Cellular biology ; Dose-Response Relationship, Drug ; Double-Blind Method ; Drug therapy ; Enzyme Inhibitors - administration & dosage ; Enzyme Inhibitors - adverse effects ; Enzyme Inhibitors - blood ; Enzyme Inhibitors - pharmacokinetics ; Half-Life ; Humans ; Kinetics ; Linear Models ; Male ; Medical sciences ; Metabolic Clearance Rate ; Middle Aged ; Pharmacokinetics and Disposition ; Pharmacology ; Pharmacology. Drug treatments ; Pharmacology/Toxicology ; Platelet Aggregation - drug effects ; Platelet Aggregation Inhibitors - administration & dosage ; Platelet Aggregation Inhibitors - adverse effects ; Platelet Aggregation Inhibitors - blood ; Platelet Aggregation Inhibitors - pharmacokinetics ; Receptors, Thromboxane - antagonists & inhibitors ; Thromboxane-A Synthase - antagonists & inhibitors ; Young Adult</subject><ispartof>European journal of clinical pharmacology, 2013-03, Vol.69 (3), p.459-465</ispartof><rights>Springer-Verlag 2012</rights><rights>2014 INIST-CNRS</rights><rights>Springer-Verlag Berlin Heidelberg 2013</rights><lds50>peer_reviewed</lds50><woscitedreferencessubscribed>false</woscitedreferencessubscribed><citedby>FETCH-LOGICAL-c402t-2c440a87047a750246c57a150fbd161de98658ed7f07e70653be50f87f5a3143</citedby><cites>FETCH-LOGICAL-c402t-2c440a87047a750246c57a150fbd161de98658ed7f07e70653be50f87f5a3143</cites></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><linktopdf>$$Uhttps://link.springer.com/content/pdf/10.1007/s00228-012-1348-9$$EPDF$$P50$$Gspringer$$H</linktopdf><linktohtml>$$Uhttps://link.springer.com/10.1007/s00228-012-1348-9$$EHTML$$P50$$Gspringer$$H</linktohtml><link.rule.ids>314,776,780,27903,27904,41467,42536,51298</link.rule.ids><backlink>$$Uhttp://pascal-francis.inist.fr/vibad/index.php?action=getRecordDetail&idt=27579739$$DView record in Pascal Francis$$Hfree_for_read</backlink><backlink>$$Uhttps://www.ncbi.nlm.nih.gov/pubmed/22815050$$D View this record in MEDLINE/PubMed$$Hfree_for_read</backlink></links><search><creatorcontrib>Richardson, A.</creatorcontrib><creatorcontrib>Sakariassen, K. S.</creatorcontrib><creatorcontrib>Meyer, J.-P.</creatorcontrib><creatorcontrib>Alberts, P.</creatorcontrib><creatorcontrib>Sorensen, A. S.</creatorcontrib><title>Single ascending oral dose pharmacokinetics and pharmacodynamics study of EV-077: the specific inhibitor of prostanoid- and isoprostane-induced cellular activation</title><title>European journal of clinical pharmacology</title><addtitle>Eur J Clin Pharmacol</addtitle><addtitle>Eur J Clin Pharmacol</addtitle><description>Purpose
This study was performed to determine the oral pharmacokinetics (PK) of EV-077 and its effects on pharmacodynamic (PD) markers. EV-077 blocks prostanoid-induced and isoprostane-induced cellular activation, and is in development for the treatment of vascular inflammation and associated complications of type-2 diabetes..
Methods
This single-ascending-dose mono-centre study was randomised, placebo-controlled, and double-blinded within each dose group. Seven EV-077 doses were administered sequentially as an oral solution: 0.0125, 0.125, 0.375, 0.75, 1.25, 1.875 and 2.5 mg/kg body weight. PK, platelet aggregation, bleeding time and safety parameters were measured. Seven to eight healthy male subjects were dosed per group: five to six subjects received EV-077 and two subjects received placebo.
Results
Tmax was reached rapidly between 0.5 h and 1.0 h. Both Cmax and AUC increased linearly with the dose. The apparent terminal half-life (t½z) increased with the dose, most likely reflecting the increasing last quantifiable concentration with increasing dose; at 2.5 mg/kg, it was 2.7-6.9 h. Measurement of platelet aggregation showed no effect at 0.0125 mg/kg, and a full and reversible inhibition at doses of 0.125-2.5 mg/kg. The average bleeding time was dose-dependently prolonged, but was always below 9 min. The PK/PD profile showed that at plasma concentrations above 20 ng/ml, EV-077 platelet aggregation was completely inhibited (>90 %). All tested doses were well tolerated.
Conclusions
Orally administered EV-077 was well tolerated, readily absorbed, reached Cmax within 1 h, with a linear PK based on Cmax and AUC. The inhibition of platelet aggregation was complete and reversible at doses of 0.125 mg/kg and higher, and average bleeding time was below 9 min.</description><subject>Administration, Oral</subject><subject>Adult</subject><subject>Area Under Curve</subject><subject>Biological and medical sciences</subject><subject>Biomedical and Life Sciences</subject><subject>Biomedicine</subject><subject>Bleeding Time</subject><subject>Cellular biology</subject><subject>Dose-Response Relationship, Drug</subject><subject>Double-Blind Method</subject><subject>Drug therapy</subject><subject>Enzyme Inhibitors - administration & dosage</subject><subject>Enzyme Inhibitors - adverse effects</subject><subject>Enzyme Inhibitors - blood</subject><subject>Enzyme Inhibitors - pharmacokinetics</subject><subject>Half-Life</subject><subject>Humans</subject><subject>Kinetics</subject><subject>Linear Models</subject><subject>Male</subject><subject>Medical sciences</subject><subject>Metabolic Clearance Rate</subject><subject>Middle Aged</subject><subject>Pharmacokinetics and Disposition</subject><subject>Pharmacology</subject><subject>Pharmacology. Drug treatments</subject><subject>Pharmacology/Toxicology</subject><subject>Platelet Aggregation - drug effects</subject><subject>Platelet Aggregation Inhibitors - administration & dosage</subject><subject>Platelet Aggregation Inhibitors - adverse effects</subject><subject>Platelet Aggregation Inhibitors - blood</subject><subject>Platelet Aggregation Inhibitors - pharmacokinetics</subject><subject>Receptors, Thromboxane - antagonists & inhibitors</subject><subject>Thromboxane-A Synthase - antagonists & inhibitors</subject><subject>Young Adult</subject><issn>0031-6970</issn><issn>1432-1041</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2013</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><sourceid>ABUWG</sourceid><sourceid>AFKRA</sourceid><sourceid>BENPR</sourceid><sourceid>CCPQU</sourceid><recordid>eNp1kcFu1DAQhi0EokvhAbggS4ijYZzYccINVaUgVeqhVa-W1550XbL2YjtI-zy8KE53KVx6sj3zzT8z_gl5y-EjB1CfMkDT9Ax4w3grejY8Iysu2voCwZ-TFUDLWTcoOCGvcr4H4HKA9iU5qVVcgoQV-X3tw92E1GSLwdU7jclM1MWMdLcxaWts_OEDFm8zNcE9Bt0-mO0SzGV2expHen7LQKnPtGyQ5h1aP3pLfdj4tS8xLcQuxVxMiN6xBy2f4zGEzAc3W3TU4jTNk0nU2OJ_meJjeE1ejGbK-OZ4npKbr-c3Z9_Y5dXF97Mvl8wKaAprrBBgegVCGSWhEZ2VytQ9x7XjHXc49J3s0akRFCroZLvGmuzVKE1bv-2UvD_I1pl-zpiLvo9zCrWj5k2vWilkxyvFD5Stk-eEo94lvzVprznoxRV9cEVXV_Tiih5qzbuj8rzeonus-GtDBT4cgeqDmcZkgvX5H6ekGlS7CDUHLtdUuMP034hPdv8D_NimdA</recordid><startdate>20130301</startdate><enddate>20130301</enddate><creator>Richardson, A.</creator><creator>Sakariassen, K. S.</creator><creator>Meyer, J.-P.</creator><creator>Alberts, P.</creator><creator>Sorensen, A. S.</creator><general>Springer-Verlag</general><general>Springer</general><general>Springer Nature B.V</general><scope>IQODW</scope><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>3V.</scope><scope>7RV</scope><scope>7TK</scope><scope>7U9</scope><scope>7X7</scope><scope>7XB</scope><scope>88E</scope><scope>8AO</scope><scope>8FI</scope><scope>8FJ</scope><scope>8FK</scope><scope>ABUWG</scope><scope>AFKRA</scope><scope>BENPR</scope><scope>CCPQU</scope><scope>FYUFA</scope><scope>GHDGH</scope><scope>H94</scope><scope>K9.</scope><scope>KB0</scope><scope>M0S</scope><scope>M1P</scope><scope>NAPCQ</scope><scope>PQEST</scope><scope>PQQKQ</scope><scope>PQUKI</scope></search><sort><creationdate>20130301</creationdate><title>Single ascending oral dose pharmacokinetics and pharmacodynamics study of EV-077: the specific inhibitor of prostanoid- and isoprostane-induced cellular activation</title><author>Richardson, A. ; Sakariassen, K. S. ; Meyer, J.-P. ; Alberts, P. ; Sorensen, A. S.</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-c402t-2c440a87047a750246c57a150fbd161de98658ed7f07e70653be50f87f5a3143</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2013</creationdate><topic>Administration, Oral</topic><topic>Adult</topic><topic>Area Under Curve</topic><topic>Biological and medical sciences</topic><topic>Biomedical and Life Sciences</topic><topic>Biomedicine</topic><topic>Bleeding Time</topic><topic>Cellular biology</topic><topic>Dose-Response Relationship, Drug</topic><topic>Double-Blind Method</topic><topic>Drug therapy</topic><topic>Enzyme Inhibitors - administration & dosage</topic><topic>Enzyme Inhibitors - adverse effects</topic><topic>Enzyme Inhibitors - blood</topic><topic>Enzyme Inhibitors - pharmacokinetics</topic><topic>Half-Life</topic><topic>Humans</topic><topic>Kinetics</topic><topic>Linear Models</topic><topic>Male</topic><topic>Medical sciences</topic><topic>Metabolic Clearance Rate</topic><topic>Middle Aged</topic><topic>Pharmacokinetics and Disposition</topic><topic>Pharmacology</topic><topic>Pharmacology. Drug treatments</topic><topic>Pharmacology/Toxicology</topic><topic>Platelet Aggregation - drug effects</topic><topic>Platelet Aggregation Inhibitors - administration & dosage</topic><topic>Platelet Aggregation Inhibitors - adverse effects</topic><topic>Platelet Aggregation Inhibitors - blood</topic><topic>Platelet Aggregation Inhibitors - pharmacokinetics</topic><topic>Receptors, Thromboxane - antagonists & inhibitors</topic><topic>Thromboxane-A Synthase - antagonists & inhibitors</topic><topic>Young Adult</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Richardson, A.</creatorcontrib><creatorcontrib>Sakariassen, K. S.</creatorcontrib><creatorcontrib>Meyer, J.-P.</creatorcontrib><creatorcontrib>Alberts, P.</creatorcontrib><creatorcontrib>Sorensen, A. S.</creatorcontrib><collection>Pascal-Francis</collection><collection>Medline</collection><collection>MEDLINE</collection><collection>MEDLINE (Ovid)</collection><collection>MEDLINE</collection><collection>MEDLINE</collection><collection>PubMed</collection><collection>CrossRef</collection><collection>ProQuest Central (Corporate)</collection><collection>Nursing & Allied Health Database</collection><collection>Neurosciences Abstracts</collection><collection>Virology and AIDS Abstracts</collection><collection>Health & Medical Collection</collection><collection>ProQuest Central (purchase pre-March 2016)</collection><collection>Medical Database (Alumni Edition)</collection><collection>ProQuest Pharma Collection</collection><collection>Hospital Premium Collection</collection><collection>Hospital Premium Collection (Alumni Edition)</collection><collection>ProQuest Central (Alumni) (purchase pre-March 2016)</collection><collection>ProQuest Central (Alumni Edition)</collection><collection>ProQuest Central UK/Ireland</collection><collection>ProQuest Central</collection><collection>ProQuest One Community College</collection><collection>Health Research Premium Collection</collection><collection>Health Research Premium Collection (Alumni)</collection><collection>AIDS and Cancer Research Abstracts</collection><collection>ProQuest Health & Medical Complete (Alumni)</collection><collection>Nursing & Allied Health Database (Alumni Edition)</collection><collection>Health & Medical Collection (Alumni Edition)</collection><collection>Medical Database</collection><collection>Nursing & Allied Health Premium</collection><collection>ProQuest One Academic Eastern Edition (DO NOT USE)</collection><collection>ProQuest One Academic</collection><collection>ProQuest One Academic UKI Edition</collection><jtitle>European journal of clinical pharmacology</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Richardson, A.</au><au>Sakariassen, K. S.</au><au>Meyer, J.-P.</au><au>Alberts, P.</au><au>Sorensen, A. S.</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Single ascending oral dose pharmacokinetics and pharmacodynamics study of EV-077: the specific inhibitor of prostanoid- and isoprostane-induced cellular activation</atitle><jtitle>European journal of clinical pharmacology</jtitle><stitle>Eur J Clin Pharmacol</stitle><addtitle>Eur J Clin Pharmacol</addtitle><date>2013-03-01</date><risdate>2013</risdate><volume>69</volume><issue>3</issue><spage>459</spage><epage>465</epage><pages>459-465</pages><issn>0031-6970</issn><eissn>1432-1041</eissn><abstract>Purpose
This study was performed to determine the oral pharmacokinetics (PK) of EV-077 and its effects on pharmacodynamic (PD) markers. EV-077 blocks prostanoid-induced and isoprostane-induced cellular activation, and is in development for the treatment of vascular inflammation and associated complications of type-2 diabetes..
Methods
This single-ascending-dose mono-centre study was randomised, placebo-controlled, and double-blinded within each dose group. Seven EV-077 doses were administered sequentially as an oral solution: 0.0125, 0.125, 0.375, 0.75, 1.25, 1.875 and 2.5 mg/kg body weight. PK, platelet aggregation, bleeding time and safety parameters were measured. Seven to eight healthy male subjects were dosed per group: five to six subjects received EV-077 and two subjects received placebo.
Results
Tmax was reached rapidly between 0.5 h and 1.0 h. Both Cmax and AUC increased linearly with the dose. The apparent terminal half-life (t½z) increased with the dose, most likely reflecting the increasing last quantifiable concentration with increasing dose; at 2.5 mg/kg, it was 2.7-6.9 h. Measurement of platelet aggregation showed no effect at 0.0125 mg/kg, and a full and reversible inhibition at doses of 0.125-2.5 mg/kg. The average bleeding time was dose-dependently prolonged, but was always below 9 min. The PK/PD profile showed that at plasma concentrations above 20 ng/ml, EV-077 platelet aggregation was completely inhibited (>90 %). All tested doses were well tolerated.
Conclusions
Orally administered EV-077 was well tolerated, readily absorbed, reached Cmax within 1 h, with a linear PK based on Cmax and AUC. The inhibition of platelet aggregation was complete and reversible at doses of 0.125 mg/kg and higher, and average bleeding time was below 9 min.</abstract><cop>Berlin/Heidelberg</cop><pub>Springer-Verlag</pub><pmid>22815050</pmid><doi>10.1007/s00228-012-1348-9</doi><tpages>7</tpages></addata></record> |
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| ispartof | European journal of clinical pharmacology, 2013-03, Vol.69 (3), p.459-465 |
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| subjects | Administration, Oral Adult Area Under Curve Biological and medical sciences Biomedical and Life Sciences Biomedicine Bleeding Time Cellular biology Dose-Response Relationship, Drug Double-Blind Method Drug therapy Enzyme Inhibitors - administration & dosage Enzyme Inhibitors - adverse effects Enzyme Inhibitors - blood Enzyme Inhibitors - pharmacokinetics Half-Life Humans Kinetics Linear Models Male Medical sciences Metabolic Clearance Rate Middle Aged Pharmacokinetics and Disposition Pharmacology Pharmacology. Drug treatments Pharmacology/Toxicology Platelet Aggregation - drug effects Platelet Aggregation Inhibitors - administration & dosage Platelet Aggregation Inhibitors - adverse effects Platelet Aggregation Inhibitors - blood Platelet Aggregation Inhibitors - pharmacokinetics Receptors, Thromboxane - antagonists & inhibitors Thromboxane-A Synthase - antagonists & inhibitors Young Adult |
| title | Single ascending oral dose pharmacokinetics and pharmacodynamics study of EV-077: the specific inhibitor of prostanoid- and isoprostane-induced cellular activation |
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