FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2201114920> ?p ?o ?g. }

• W2201114920 endingPage "213" @default.
• W2201114920 startingPage "209" @default.
• W2201114920 abstract "PurposeVascular lesions of the orbit, although not malignant, can cause morbidity because of their location near critical structures in the orbit. For the same reason, they can be challenging to remove surgically. Anti-vascular endothelial growth factor (VEGF) drugs are increasingly being used to treat diseases with prominent angiogenesis. Our study aimed to determine to what extent VEGF receptors and their subtypes are expressed on selected vascular lesions of the orbit.DesignRetrospective case series of all orbital vascular lesions removed by one of the authors (JAG) at the Mayo Clinic.ParticipantsA total of 52 patients who underwent removal of vascular orbital lesions.MethodsThe pathology specimens from the patients were retrieved, their pathologic diagnosis was confirmed, demographic and clinical information were gathered, and sections from vascular tumors were stained with vascular endothelial growth factor receptor (VEGFR), vascular endothelial growth factor receptor type 1 (VEGFR1), vascular endothelial growth factor receptor type 2 (VEGFR2), and vascular endothelial growth factor receptor type 3 (VEGFR3).Main Outcome MeasuresThe existence and pattern of staining with VEGF and its subtypes on these lesions.ResultsThere were 28 specimens of venous malformations, 4 capillary hemangiomas, 7 lymphatic malformations, and 6 lymphaticovenous malformations. All samples stained with VEGF, 55% stained with VEGFR1, 98% stained with VEGFR2, and 96% stained with VEGFR3. Most (94%) of the VEGFR2 staining was diffuse.ConclusionsMost orbital vascular lesions express VEGF receptors, which may suggest a future target for nonsurgical treatment. Vascular lesions of the orbit, although not malignant, can cause morbidity because of their location near critical structures in the orbit. For the same reason, they can be challenging to remove surgically. Anti-vascular endothelial growth factor (VEGF) drugs are increasingly being used to treat diseases with prominent angiogenesis. Our study aimed to determine to what extent VEGF receptors and their subtypes are expressed on selected vascular lesions of the orbit. Retrospective case series of all orbital vascular lesions removed by one of the authors (JAG) at the Mayo Clinic. A total of 52 patients who underwent removal of vascular orbital lesions. The pathology specimens from the patients were retrieved, their pathologic diagnosis was confirmed, demographic and clinical information were gathered, and sections from vascular tumors were stained with vascular endothelial growth factor receptor (VEGFR), vascular endothelial growth factor receptor type 1 (VEGFR1), vascular endothelial growth factor receptor type 2 (VEGFR2), and vascular endothelial growth factor receptor type 3 (VEGFR3). The existence and pattern of staining with VEGF and its subtypes on these lesions. There were 28 specimens of venous malformations, 4 capillary hemangiomas, 7 lymphatic malformations, and 6 lymphaticovenous malformations. All samples stained with VEGF, 55% stained with VEGFR1, 98% stained with VEGFR2, and 96% stained with VEGFR3. Most (94%) of the VEGFR2 staining was diffuse. Most orbital vascular lesions express VEGF receptors, which may suggest a future target for nonsurgical treatment." @default.
• W2201114920 created "2016-06-24" @default.
• W2201114920 creator A5004000972 @default.
• W2201114920 creator A5049186993 @default.
• W2201114920 creator A5070990965 @default.
• W2201114920 creator A5081888516 @default.
• W2201114920 creator A5084861549 @default.
• W2201114920 creator A5089768754 @default.
• W2201114920 date "2016-01-01" @default.
• W2201114920 modified "2023-10-11" @default.
• W2201114920 title "Expression of Vascular Endothelial Growth Factor Receptors in Benign Vascular Lesions of the Orbit" @default.
• W2201114920 cites W1970028203 @default.
• W2201114920 cites W1982964633 @default.
• W2201114920 cites W2000292756 @default.
• W2201114920 cites W2012063336 @default.
• W2201114920 cites W2023959682 @default.
• W2201114920 cites W2026996188 @default.
• W2201114920 cites W2030537668 @default.
• W2201114920 cites W2037834317 @default.
• W2201114920 cites W2043651574 @default.
• W2201114920 cites W2053359352 @default.
• W2201114920 cites W2058046310 @default.
• W2201114920 cites W2070178377 @default.
• W2201114920 cites W2085010530 @default.
• W2201114920 cites W2103388828 @default.
• W2201114920 cites W2104774124 @default.
• W2201114920 cites W2115378043 @default.
• W2201114920 cites W2121704563 @default.
• W2201114920 cites W2123903372 @default.
• W2201114920 cites W2124772324 @default.
• W2201114920 cites W2136593003 @default.
• W2201114920 cites W2153484787 @default.
• W2201114920 cites W2171086580 @default.
• W2201114920 cites W4236614851 @default.
• W2201114920 cites W4365918917 @default.
• W2201114920 doi "https://doi.org/10.1016/j.ophtha.2015.09.009" @default.
• W2201114920 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/26481818" @default.
• W2201114920 hasPublicationYear "2016" @default.
• W2201114920 type Work @default.
• W2201114920 sameAs 2201114920 @default.
• W2201114920 citedByCount "11" @default.
• W2201114920 countsByYear W22011149202016 @default.
• W2201114920 countsByYear W22011149202017 @default.
• W2201114920 countsByYear W22011149202018 @default.
• W2201114920 countsByYear W22011149202019 @default.
• W2201114920 countsByYear W22011149202020 @default.
• W2201114920 countsByYear W22011149202021 @default.
• W2201114920 countsByYear W22011149202022 @default.
• W2201114920 crossrefType "journal-article" @default.
• W2201114920 hasAuthorship W2201114920A5004000972 @default.
• W2201114920 hasAuthorship W2201114920A5049186993 @default.
• W2201114920 hasAuthorship W2201114920A5070990965 @default.
• W2201114920 hasAuthorship W2201114920A5081888516 @default.
• W2201114920 hasAuthorship W2201114920A5084861549 @default.
• W2201114920 hasAuthorship W2201114920A5089768754 @default.
• W2201114920 hasBestOaLocation W22011149201 @default.
• W2201114920 hasConcept C103041312 @default.
• W2201114920 hasConcept C126322002 @default.
• W2201114920 hasConcept C126838900 @default.
• W2201114920 hasConcept C127413603 @default.
• W2201114920 hasConcept C142724271 @default.
• W2201114920 hasConcept C146285616 @default.
• W2201114920 hasConcept C146978453 @default.
• W2201114920 hasConcept C14858245 @default.
• W2201114920 hasConcept C167734588 @default.
• W2201114920 hasConcept C170493617 @default.
• W2201114920 hasConcept C196644772 @default.
• W2201114920 hasConcept C2777025900 @default.
• W2201114920 hasConcept C2777507709 @default.
• W2201114920 hasConcept C2780394083 @default.
• W2201114920 hasConcept C71924100 @default.
• W2201114920 hasConceptScore W2201114920C103041312 @default.
• W2201114920 hasConceptScore W2201114920C126322002 @default.
• W2201114920 hasConceptScore W2201114920C126838900 @default.
• W2201114920 hasConceptScore W2201114920C127413603 @default.
• W2201114920 hasConceptScore W2201114920C142724271 @default.
• W2201114920 hasConceptScore W2201114920C146285616 @default.
• W2201114920 hasConceptScore W2201114920C146978453 @default.
• W2201114920 hasConceptScore W2201114920C14858245 @default.
• W2201114920 hasConceptScore W2201114920C167734588 @default.
• W2201114920 hasConceptScore W2201114920C170493617 @default.
• W2201114920 hasConceptScore W2201114920C196644772 @default.
• W2201114920 hasConceptScore W2201114920C2777025900 @default.
• W2201114920 hasConceptScore W2201114920C2777507709 @default.
• W2201114920 hasConceptScore W2201114920C2780394083 @default.
• W2201114920 hasConceptScore W2201114920C71924100 @default.
• W2201114920 hasIssue "1" @default.
• W2201114920 hasLocation W22011149201 @default.
• W2201114920 hasLocation W22011149202 @default.
• W2201114920 hasOpenAccess W2201114920 @default.
• W2201114920 hasPrimaryLocation W22011149201 @default.
• W2201114920 hasRelatedWork W2009081283 @default.
• W2201114920 hasRelatedWork W2029619231 @default.
• W2201114920 hasRelatedWork W2034393061 @default.
• W2201114920 hasRelatedWork W2118989983 @default.
• W2201114920 hasRelatedWork W2151772280 @default.
• W2201114920 hasRelatedWork W2161808292 @default.
• W2201114920 hasRelatedWork W2318497614 @default.

• next