FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2896421189> ?p ?o ?g. }

• W2896421189 endingPage "115" @default.
• W2896421189 startingPage "107" @default.
• W2896421189 abstract "Objective To characterize the phenotype and function of fibroblasts derived from airway scar in idiopathic subglottic stenosis (iSGS) and to explore scar fibroblast response to interleukin 17A (IL-17A). Study Design Basic science. Setting Laboratory. Subjects and Methods Primary fibroblast cell lines from iSGS subjects, idiopathic pulmonary fibrosis subjects, and normal control airways were utilized for analysis. Protein, molecular, and flow cytometric techniques were applied in vitro to assess the phenotype and functional response of disease fibroblasts to IL-17A. Results Mechanistically, IL-17A drives iSGS scar fibroblast proliferation ( P < .01), synergizes with transforming growth factor ß1 to promote extracellular matrix production (collagen and fibronectin; P = .04), and directly stimulates scar fibroblasts to produce chemokines (chemokine ligand 2) and cytokines (IL-6 and granulocyte-macrophage colony-stimulating factor) critical to the recruitment and differentiation of myeloid cells ( P < .01). Glucocorticoids abrogated IL-17A-dependent iSGS scar fibroblast production of granulocyte-macrophage colony-stimulating factor ( P = .02). Conclusion IL-17A directly drives iSGS scar fibroblast proliferation, synergizes with transforming growth factor ß1 to promote extracellular matrix production, and amplifies local inflammatory signaling. Glucocorticoids appear to partially abrogate fibroblast-dependent inflammatory signaling. These results offer mechanistic support for future translational study of clinical reagents for manipulation of the IL-17A pathway in iSGS patients." @default.
• W2896421189 created "2018-10-26" @default.
• W2896421189 creator A5021563941 @default.
• W2896421189 creator A5022299075 @default.
• W2896421189 creator A5035624344 @default.
• W2896421189 creator A5042606734 @default.
• W2896421189 creator A5045180601 @default.
• W2896421189 creator A5051812693 @default.
• W2896421189 creator A5063872240 @default.
• W2896421189 creator A5068181002 @default.
• W2896421189 creator A5075068837 @default.
• W2896421189 creator A5090398738 @default.
• W2896421189 creator A5091586329 @default.
• W2896421189 date "2018-10-16" @default.
• W2896421189 modified "2023-10-11" @default.
• W2896421189 title "Pathologic Fibroblasts in Idiopathic Subglottic Stenosis Amplify Local Inflammatory Signals" @default.
• W2896421189 cites W1505833426 @default.
• W2896421189 cites W1548753867 @default.
• W2896421189 cites W183636652 @default.
• W2896421189 cites W1875866852 @default.
• W2896421189 cites W1895601060 @default.
• W2896421189 cites W1925654693 @default.
• W2896421189 cites W1966608706 @default.
• W2896421189 cites W1977437151 @default.
• W2896421189 cites W1978695171 @default.
• W2896421189 cites W1983260461 @default.
• W2896421189 cites W1996997066 @default.
• W2896421189 cites W1997131908 @default.
• W2896421189 cites W1998905025 @default.
• W2896421189 cites W2015141049 @default.
• W2896421189 cites W2015912102 @default.
• W2896421189 cites W2031694374 @default.
• W2896421189 cites W2032788173 @default.
• W2896421189 cites W2033884349 @default.
• W2896421189 cites W2055348159 @default.
• W2896421189 cites W2055712900 @default.
• W2896421189 cites W2061047385 @default.
• W2896421189 cites W2065184077 @default.
• W2896421189 cites W2065949135 @default.
• W2896421189 cites W2067754406 @default.
• W2896421189 cites W2083467607 @default.
• W2896421189 cites W2085099489 @default.
• W2896421189 cites W2087180040 @default.
• W2896421189 cites W2095715691 @default.
• W2896421189 cites W2106341988 @default.
• W2896421189 cites W2107277218 @default.
• W2896421189 cites W2117559606 @default.
• W2896421189 cites W2124841074 @default.
• W2896421189 cites W2136808380 @default.
• W2896421189 cites W2141411192 @default.
• W2896421189 cites W2142249617 @default.
• W2896421189 cites W2145007867 @default.
• W2896421189 cites W2154733572 @default.
• W2896421189 cites W2263390674 @default.
• W2896421189 cites W2428301625 @default.
• W2896421189 cites W2436699703 @default.
• W2896421189 cites W2597638978 @default.
• W2896421189 cites W2610273044 @default.
• W2896421189 cites W2623528309 @default.
• W2896421189 cites W2757048625 @default.
• W2896421189 cites W2761253664 @default.
• W2896421189 cites W2784123747 @default.
• W2896421189 cites W1964184380 @default.
• W2896421189 doi "https://doi.org/10.1177/0194599818803584" @default.
• W2896421189 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6389372" @default.
• W2896421189 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30322354" @default.
• W2896421189 hasPublicationYear "2018" @default.
• W2896421189 type Work @default.
• W2896421189 sameAs 2896421189 @default.
• W2896421189 citedByCount "30" @default.
• W2896421189 countsByYear W28964211892019 @default.
• W2896421189 countsByYear W28964211892020 @default.
• W2896421189 countsByYear W28964211892021 @default.
• W2896421189 countsByYear W28964211892022 @default.
• W2896421189 countsByYear W28964211892023 @default.
• W2896421189 crossrefType "journal-article" @default.
• W2896421189 hasAuthorship W2896421189A5021563941 @default.
• W2896421189 hasAuthorship W2896421189A5022299075 @default.
• W2896421189 hasAuthorship W2896421189A5035624344 @default.
• W2896421189 hasAuthorship W2896421189A5042606734 @default.
• W2896421189 hasAuthorship W2896421189A5045180601 @default.
• W2896421189 hasAuthorship W2896421189A5051812693 @default.
• W2896421189 hasAuthorship W2896421189A5063872240 @default.
• W2896421189 hasAuthorship W2896421189A5068181002 @default.
• W2896421189 hasAuthorship W2896421189A5075068837 @default.
• W2896421189 hasAuthorship W2896421189A5090398738 @default.
• W2896421189 hasAuthorship W2896421189A5091586329 @default.
• W2896421189 hasBestOaLocation W28964211891 @default.
• W2896421189 hasConcept C13373296 @default.
• W2896421189 hasConcept C189165786 @default.
• W2896421189 hasConcept C203014093 @default.
• W2896421189 hasConcept C2776914184 @default.
• W2896421189 hasConcept C2780381497 @default.
• W2896421189 hasConcept C502942594 @default.
• W2896421189 hasConcept C54355233 @default.
• W2896421189 hasConcept C71924100 @default.
• W2896421189 hasConcept C81885089 @default.
• W2896421189 hasConcept C86492073 @default.

• next