FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2051237683> ?p ?o ?g. }

• W2051237683 endingPage "237" @default.
• W2051237683 startingPage "234" @default.
• W2051237683 abstract "Based on more than a decade of evidence, high-sensitivity C-reactive protein (hsCRP)1 is in clinical use as an inexpensive adjunct to global cardiovascular risk prediction, as a tool to determine risk of future diabetes and metabolic syndrome, and as a method for monitoring efficacy of statin therapy. In the last decade, more than 20 prospective cohort studies have indicated that hsCRP concentrations independently associate with future risk of myocardial infarction, stroke, metabolic syndrome, and type 2 diabetes, and most studies of adequate sample size have found that hsCRP adds prognostic information to global risk prediction scores. On this basis, guidelines for use of hsCRP in clinical practice have been issued by the Centers for Disease Control and Prevention (1), and novel algorithms for risk prediction that incorporate hsCRP, such as the Reynolds Risk Score (www.reynoldsriskscore.com), have been shown to improve risk classification, particularly for “intermediate risk” patients who account for more than 70% of all vascular events (2). Further, as statins lower hsCRP in an LDL cholesterol–independent manner and as best clinical outcomes occur among statin-treated patients who not only reduce LDL cholesterol below 700 mg/L (70 mg/dL) but also reduce hsCRP below 2 mg/L, the concept of “dual goals” has been introduced into cardiovascular clinical practice (3)(4). Because of its relationships with insulin resistance, leptin, and cytokine function (5), as well as its role in endothelial dysfunction and inhibition of fibrinolysis (6)(7), CRP has also been of pathophysiologic interest as an intellectual bridge linking low-grade systemic inflammation to both diabetogenesis and atherogenesis.Given the consistency and generalizability of these data, it is …" @default.
• W2051237683 created "2016-06-24" @default.
• W2051237683 creator A5091595592 @default.
• W2051237683 date "2008-02-01" @default.
• W2051237683 modified "2023-09-23" @default.
• W2051237683 title "High-Sensitivity C-Reactive Protein as a Predictor of All-Cause Mortality: Implications for Research and Patient Care" @default.
• W2051237683 cites W143292899 @default.
• W2051237683 cites W1972171203 @default.
• W2051237683 cites W1985967126 @default.
• W2051237683 cites W2000869225 @default.
• W2051237683 cites W2012689879 @default.
• W2051237683 cites W2021753308 @default.
• W2051237683 cites W2039420330 @default.
• W2051237683 cites W2054893928 @default.
• W2051237683 cites W2058591384 @default.
• W2051237683 cites W2058610272 @default.
• W2051237683 cites W2066294435 @default.
• W2051237683 cites W2080883999 @default.
• W2051237683 cites W2099408048 @default.
• W2051237683 cites W2101603352 @default.
• W2051237683 cites W2104657159 @default.
• W2051237683 cites W2118154631 @default.
• W2051237683 cites W2119475547 @default.
• W2051237683 cites W2132814978 @default.
• W2051237683 cites W2146456234 @default.
• W2051237683 cites W2149104133 @default.
• W2051237683 cites W2149844486 @default.
• W2051237683 cites W2159871913 @default.
• W2051237683 cites W2160560551 @default.
• W2051237683 cites W2161465441 @default.
• W2051237683 cites W2163092745 @default.
• W2051237683 doi "https://doi.org/10.1373/clinchem.2007.099465" @default.
• W2051237683 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/18223130" @default.
• W2051237683 hasPublicationYear "2008" @default.
• W2051237683 type Work @default.
• W2051237683 sameAs 2051237683 @default.
• W2051237683 citedByCount "47" @default.
• W2051237683 countsByYear W20512376832012 @default.
• W2051237683 countsByYear W20512376832013 @default.
• W2051237683 countsByYear W20512376832014 @default.
• W2051237683 countsByYear W20512376832015 @default.
• W2051237683 countsByYear W20512376832016 @default.
• W2051237683 countsByYear W20512376832017 @default.
• W2051237683 countsByYear W20512376832018 @default.
• W2051237683 countsByYear W20512376832019 @default.
• W2051237683 countsByYear W20512376832020 @default.
• W2051237683 countsByYear W20512376832021 @default.
• W2051237683 crossrefType "journal-article" @default.
• W2051237683 hasAuthorship W2051237683A5091595592 @default.
• W2051237683 hasBestOaLocation W20512376831 @default.
• W2051237683 hasConcept C126322002 @default.
• W2051237683 hasConcept C177713679 @default.
• W2051237683 hasConcept C2776914184 @default.
• W2051237683 hasConcept C2781195455 @default.
• W2051237683 hasConcept C71924100 @default.
• W2051237683 hasConceptScore W2051237683C126322002 @default.
• W2051237683 hasConceptScore W2051237683C177713679 @default.
• W2051237683 hasConceptScore W2051237683C2776914184 @default.
• W2051237683 hasConceptScore W2051237683C2781195455 @default.
• W2051237683 hasConceptScore W2051237683C71924100 @default.
• W2051237683 hasIssue "2" @default.
• W2051237683 hasLocation W20512376831 @default.
• W2051237683 hasLocation W20512376832 @default.
• W2051237683 hasOpenAccess W2051237683 @default.
• W2051237683 hasPrimaryLocation W20512376831 @default.
• W2051237683 hasRelatedWork W1996673535 @default.
• W2051237683 hasRelatedWork W2016602574 @default.
• W2051237683 hasRelatedWork W2081220240 @default.
• W2051237683 hasRelatedWork W2114669833 @default.
• W2051237683 hasRelatedWork W2128199946 @default.
• W2051237683 hasRelatedWork W2388442319 @default.
• W2051237683 hasRelatedWork W2748952813 @default.
• W2051237683 hasRelatedWork W2766231742 @default.
• W2051237683 hasRelatedWork W2899084033 @default.
• W2051237683 hasRelatedWork W3031052312 @default.
• W2051237683 hasVolume "54" @default.
• W2051237683 isParatext "false" @default.
• W2051237683 isRetracted "false" @default.
• W2051237683 magId "2051237683" @default.
• W2051237683 workType "article" @default.