FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2895864000> ?p ?o ?g. }

• W2895864000 endingPage "13" @default.
• W2895864000 startingPage "1" @default.
• W2895864000 abstract "Lymphocyte costimulation plays a central role in immunology, inflammation, and immunotherapy. The inducible T cell costimulator (ICOS) is expressed on T cells following peptide: MHC engagement with CD28 costimulation. The interaction of ICOS with its sole ligand, the inducible T cell costimulatory ligand (ICOSL; also known as B7-related protein-1), triggers a number of key activities of T cells including differentiation and cytokine production. Suppression of T cell activation can be achieved by blocking this interaction and has been shown to be an effective means of ameliorating disease in models of autoimmunity. In this study, we isolated specific anti-ICOSL new antigen receptor domains from a synthetic phage display library and demonstrated their ability to block the ICOS/ICOSL interaction and inhibit T cell proliferation. Anti-mouse ICOSL domains, considered here as surrogates for the use of anti-human ICOSL domains in patient therapy, were tested for efficacy in a collagen-induced mouse model of rheumatoid arthritis where they significantly decreased the inflammation of joints and delayed and reduced overall disease progression and severity." @default.
• W2895864000 created "2018-10-26" @default.
• W2895864000 creator A5011032790 @default.
• W2895864000 creator A5025162919 @default.
• W2895864000 creator A5030861371 @default.
• W2895864000 creator A5045641515 @default.
• W2895864000 creator A5047850773 @default.
• W2895864000 creator A5059583858 @default.
• W2895864000 creator A5060649824 @default.
• W2895864000 creator A5063499028 @default.
• W2895864000 creator A5079532494 @default.
• W2895864000 creator A5079932070 @default.
• W2895864000 creator A5091121185 @default.
• W2895864000 date "2018-10-17" @default.
• W2895864000 modified "2023-10-02" @default.
• W2895864000 title "Anti-ICOSL New Antigen Receptor Domains Inhibit T Cell Proliferation and Reduce the Development of Inflammation in the Collagen-Induced Mouse Model of Rheumatoid Arthritis" @default.
• W2895864000 cites W116895358 @default.
• W2895864000 cites W1542262758 @default.
• W2895864000 cites W1549578384 @default.
• W2895864000 cites W1609716101 @default.
• W2895864000 cites W1628992377 @default.
• W2895864000 cites W1661441964 @default.
• W2895864000 cites W1909853035 @default.
• W2895864000 cites W1937071194 @default.
• W2895864000 cites W1964538987 @default.
• W2895864000 cites W1964592316 @default.
• W2895864000 cites W1971219506 @default.
• W2895864000 cites W1971972971 @default.
• W2895864000 cites W1972394228 @default.
• W2895864000 cites W1979364075 @default.
• W2895864000 cites W1987720155 @default.
• W2895864000 cites W1996903105 @default.
• W2895864000 cites W200453334 @default.
• W2895864000 cites W2005855621 @default.
• W2895864000 cites W2009923660 @default.
• W2895864000 cites W2021256658 @default.
• W2895864000 cites W2024644107 @default.
• W2895864000 cites W2028279604 @default.
• W2895864000 cites W2028971378 @default.
• W2895864000 cites W2030889094 @default.
• W2895864000 cites W2032792840 @default.
• W2895864000 cites W2043397806 @default.
• W2895864000 cites W2052077392 @default.
• W2895864000 cites W2052503785 @default.
• W2895864000 cites W2063712078 @default.
• W2895864000 cites W2072902418 @default.
• W2895864000 cites W2073796343 @default.
• W2895864000 cites W2094656087 @default.
• W2895864000 cites W2101623377 @default.
• W2895864000 cites W2108556253 @default.
• W2895864000 cites W2114308202 @default.
• W2895864000 cites W2114738239 @default.
• W2895864000 cites W2115912680 @default.
• W2895864000 cites W2119103976 @default.
• W2895864000 cites W2123130879 @default.
• W2895864000 cites W2124670599 @default.
• W2895864000 cites W2130769674 @default.
• W2895864000 cites W2133866209 @default.
• W2895864000 cites W2133866843 @default.
• W2895864000 cites W2136866940 @default.
• W2895864000 cites W2140060739 @default.
• W2895864000 cites W2143660712 @default.
• W2895864000 cites W2154515402 @default.
• W2895864000 cites W2160529810 @default.
• W2895864000 cites W2170143249 @default.
• W2895864000 cites W2319957449 @default.
• W2895864000 cites W2339641503 @default.
• W2895864000 cites W2590315680 @default.
• W2895864000 cites W2758511152 @default.
• W2895864000 cites W2765708508 @default.
• W2895864000 cites W2768335405 @default.
• W2895864000 cites W2778983584 @default.
• W2895864000 cites W2794254410 @default.
• W2895864000 cites W3013838954 @default.
• W2895864000 cites W4211111012 @default.
• W2895864000 doi "https://doi.org/10.1155/2018/4089459" @default.
• W2895864000 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6207862" @default.
• W2895864000 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30417018" @default.
• W2895864000 hasPublicationYear "2018" @default.
• W2895864000 type Work @default.
• W2895864000 sameAs 2895864000 @default.
• W2895864000 citedByCount "9" @default.
• W2895864000 countsByYear W28958640002019 @default.
• W2895864000 countsByYear W28958640002020 @default.
• W2895864000 countsByYear W28958640002021 @default.
• W2895864000 countsByYear W28958640002022 @default.
• W2895864000 countsByYear W28958640002023 @default.
• W2895864000 crossrefType "journal-article" @default.
• W2895864000 hasAuthorship W2895864000A5011032790 @default.
• W2895864000 hasAuthorship W2895864000A5025162919 @default.
• W2895864000 hasAuthorship W2895864000A5030861371 @default.
• W2895864000 hasAuthorship W2895864000A5045641515 @default.
• W2895864000 hasAuthorship W2895864000A5047850773 @default.
• W2895864000 hasAuthorship W2895864000A5059583858 @default.
• W2895864000 hasAuthorship W2895864000A5060649824 @default.
• W2895864000 hasAuthorship W2895864000A5063499028 @default.
• W2895864000 hasAuthorship W2895864000A5079532494 @default.
• W2895864000 hasAuthorship W2895864000A5079932070 @default.

• next