FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2176071570> ?p ?o ?g. }

• W2176071570 endingPage "334" @default.
• W2176071570 startingPage "327" @default.
• W2176071570 abstract "Objective We measured serum levels of proinflammatory/prothrombotic markers P-selectin, CD40L, matrix metalloproteinase 9 (MMP-9), intracellular adhesion molecule 1 (ICAM-1), and interleukin (IL)-6 in ischemic stroke patients, correlating their levels with the results of aspirin (ASA) and clopidogrel antiplatelet responses, using 3 “point of care” platelet function instruments, thromboelastograph (TEG), Accumetrics (ACU), and impedance aggregometer (IMP). Methods Patients on chronic ASA regimen at the time of stroke were switched to 300 mg clopidogrel loading dose and 75 mg clopidogrel maintenance dose. Serum levels of the aforementioned inflammatory mediators were measured in 51 patients at baseline (on ASA regimen), and at 26 ± 5 hours and 64 ± 18 hours postclopidogrel administration by enzyme-linked immunosorbent assay. Results P-selectin, CD40L, and MMP-9 serum levels were reduced; ICAM-1 and IL-6 serum levels showed no difference postclopidogrel administration relative to baseline. Patients' stratification based on ASA dose showed more significant reductions in P-selectin, CD40L, and MMP-9 serum levels postclopidogrel administration in patients who were on baseline 81 mg ASA, as compared to patients on 325 mg ASA. Measurement with TEG was sensitive for correlating ASA antiplatelet responses to serum levels of inflammatory markers, whereas measurements with ACU and IMP were sensitive for correlating clopidogrel antiplatelet responses to serum levels of inflammatory markers. Conclusion Clopidogrel exerts both platelet-dependent and platelet-independent anti-inflammatory effects. The association between platelet function and inflammation depends on the platelet function analyzer, the type of antiplatelet agent, the nature of the inflammatory marker, and the time of measurement relative to the time of drug administration. We measured serum levels of proinflammatory/prothrombotic markers P-selectin, CD40L, matrix metalloproteinase 9 (MMP-9), intracellular adhesion molecule 1 (ICAM-1), and interleukin (IL)-6 in ischemic stroke patients, correlating their levels with the results of aspirin (ASA) and clopidogrel antiplatelet responses, using 3 “point of care” platelet function instruments, thromboelastograph (TEG), Accumetrics (ACU), and impedance aggregometer (IMP). Patients on chronic ASA regimen at the time of stroke were switched to 300 mg clopidogrel loading dose and 75 mg clopidogrel maintenance dose. Serum levels of the aforementioned inflammatory mediators were measured in 51 patients at baseline (on ASA regimen), and at 26 ± 5 hours and 64 ± 18 hours postclopidogrel administration by enzyme-linked immunosorbent assay. P-selectin, CD40L, and MMP-9 serum levels were reduced; ICAM-1 and IL-6 serum levels showed no difference postclopidogrel administration relative to baseline. Patients' stratification based on ASA dose showed more significant reductions in P-selectin, CD40L, and MMP-9 serum levels postclopidogrel administration in patients who were on baseline 81 mg ASA, as compared to patients on 325 mg ASA. Measurement with TEG was sensitive for correlating ASA antiplatelet responses to serum levels of inflammatory markers, whereas measurements with ACU and IMP were sensitive for correlating clopidogrel antiplatelet responses to serum levels of inflammatory markers. Clopidogrel exerts both platelet-dependent and platelet-independent anti-inflammatory effects. The association between platelet function and inflammation depends on the platelet function analyzer, the type of antiplatelet agent, the nature of the inflammatory marker, and the time of measurement relative to the time of drug administration." @default.
• W2176071570 created "2016-06-24" @default.
• W2176071570 creator A5003998107 @default.
• W2176071570 creator A5052345788 @default.
• W2176071570 creator A5054281421 @default.
• W2176071570 creator A5063224353 @default.
• W2176071570 creator A5072490641 @default.
• W2176071570 creator A5082811870 @default.
• W2176071570 creator A5082820535 @default.
• W2176071570 creator A5083002276 @default.
• W2176071570 creator A5088401832 @default.
• W2176071570 date "2016-02-01" @default.
• W2176071570 modified "2023-10-14" @default.
• W2176071570 title "Relationship between Inflammation and Aspirin and Clopidogrel Antiplatelet Responses in Acute Ischemic Stroke" @default.
• W2176071570 cites W1534620902 @default.
• W2176071570 cites W1905017519 @default.
• W2176071570 cites W1976018233 @default.
• W2176071570 cites W1979853906 @default.
• W2176071570 cites W1984019856 @default.
• W2176071570 cites W1998250344 @default.
• W2176071570 cites W2004690434 @default.
• W2176071570 cites W2019399894 @default.
• W2176071570 cites W2023684680 @default.
• W2176071570 cites W2026222911 @default.
• W2176071570 cites W2029888572 @default.
• W2176071570 cites W2031881965 @default.
• W2176071570 cites W2041182922 @default.
• W2176071570 cites W2048278363 @default.
• W2176071570 cites W2059950477 @default.
• W2176071570 cites W2064293654 @default.
• W2176071570 cites W2085190889 @default.
• W2176071570 cites W2096976767 @default.
• W2176071570 cites W2105642801 @default.
• W2176071570 cites W2108431750 @default.
• W2176071570 cites W2112476056 @default.
• W2176071570 cites W2114744626 @default.
• W2176071570 cites W2117327095 @default.
• W2176071570 cites W2122822332 @default.
• W2176071570 cites W2133236250 @default.
• W2176071570 cites W2140392018 @default.
• W2176071570 cites W2335674947 @default.
• W2176071570 doi "https://doi.org/10.1016/j.jstrokecerebrovasdis.2015.10.001" @default.
• W2176071570 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/26586373" @default.
• W2176071570 hasPublicationYear "2016" @default.
• W2176071570 type Work @default.
• W2176071570 sameAs 2176071570 @default.
• W2176071570 citedByCount "15" @default.
• W2176071570 countsByYear W21760715702016 @default.
• W2176071570 countsByYear W21760715702017 @default.
• W2176071570 countsByYear W21760715702018 @default.
• W2176071570 countsByYear W21760715702019 @default.
• W2176071570 countsByYear W21760715702020 @default.
• W2176071570 countsByYear W21760715702021 @default.
• W2176071570 countsByYear W21760715702022 @default.
• W2176071570 crossrefType "journal-article" @default.
• W2176071570 hasAuthorship W2176071570A5003998107 @default.
• W2176071570 hasAuthorship W2176071570A5052345788 @default.
• W2176071570 hasAuthorship W2176071570A5054281421 @default.
• W2176071570 hasAuthorship W2176071570A5063224353 @default.
• W2176071570 hasAuthorship W2176071570A5072490641 @default.
• W2176071570 hasAuthorship W2176071570A5082811870 @default.
• W2176071570 hasAuthorship W2176071570A5082820535 @default.
• W2176071570 hasAuthorship W2176071570A5083002276 @default.
• W2176071570 hasAuthorship W2176071570A5088401832 @default.
• W2176071570 hasConcept C126322002 @default.
• W2176071570 hasConcept C164027704 @default.
• W2176071570 hasConcept C2776914184 @default.
• W2176071570 hasConcept C2777265216 @default.
• W2176071570 hasConcept C2777628954 @default.
• W2176071570 hasConcept C2777849778 @default.
• W2176071570 hasConcept C3018697912 @default.
• W2176071570 hasConcept C71924100 @default.
• W2176071570 hasConcept C89560881 @default.
• W2176071570 hasConcept C98274493 @default.
• W2176071570 hasConceptScore W2176071570C126322002 @default.
• W2176071570 hasConceptScore W2176071570C164027704 @default.
• W2176071570 hasConceptScore W2176071570C2776914184 @default.
• W2176071570 hasConceptScore W2176071570C2777265216 @default.
• W2176071570 hasConceptScore W2176071570C2777628954 @default.
• W2176071570 hasConceptScore W2176071570C2777849778 @default.
• W2176071570 hasConceptScore W2176071570C3018697912 @default.
• W2176071570 hasConceptScore W2176071570C71924100 @default.
• W2176071570 hasConceptScore W2176071570C89560881 @default.
• W2176071570 hasConceptScore W2176071570C98274493 @default.
• W2176071570 hasIssue "2" @default.
• W2176071570 hasLocation W21760715701 @default.
• W2176071570 hasLocation W21760715702 @default.
• W2176071570 hasOpenAccess W2176071570 @default.
• W2176071570 hasPrimaryLocation W21760715701 @default.
• W2176071570 hasRelatedWork W1975904564 @default.
• W2176071570 hasRelatedWork W1995832396 @default.
• W2176071570 hasRelatedWork W2042706070 @default.
• W2176071570 hasRelatedWork W2059334533 @default.
• W2176071570 hasRelatedWork W2075941057 @default.
• W2176071570 hasRelatedWork W2118793783 @default.
• W2176071570 hasRelatedWork W2143333244 @default.
• W2176071570 hasRelatedWork W2171282819 @default.
• W2176071570 hasRelatedWork W2408263356 @default.

• next