FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W1529537962> ?p ?o ?g. }

• W1529537962 endingPage "8432" @default.
• W1529537962 startingPage "8427" @default.
• W1529537962 abstract "The use of receptor-ligand interactions to direct toxins to kill diseased cells selectively has shown considerable promise for treatment of a number of cancers and, more recently, autoimmune disease. Here we move the fusion toxin protein (FTP) technology beyond cancer/autoimmune therapeutics to target the human viral pathogen, human cytomegalovirus (HCMV), on the basis of its expression of the 7TM G protein-coupled chemokine receptor US28. The virus origin of US28 provides an exceptional chemokine-binding profile with high selectivity and improved binding for the CX3C chemokine, CX3CL1. Moreover, US28 is constitutively internalizing by nature, providing highly effective FTP delivery. We designed a synthetic CX3CL1 variant engineered to have ultra-high affinity for US28 and greater specificity for US28 than the natural sole receptor for CX3CL1, CX3CR1, and we fused the synthetic variant with the cytotoxic domain of Pseudomonas Exotoxin A. This novel strategy of a rationally designed FTP provided unparalleled anti-HCMV efficacy and potency in vitro and in vivo." @default.
• W1529537962 created "2016-06-24" @default.
• W1529537962 creator A5005540598 @default.
• W1529537962 creator A5017426114 @default.
• W1529537962 creator A5021248446 @default.
• W1529537962 creator A5034044681 @default.
• W1529537962 creator A5035872776 @default.
• W1529537962 creator A5046607220 @default.
• W1529537962 creator A5051522561 @default.
• W1529537962 creator A5057973675 @default.
• W1529537962 creator A5071806328 @default.
• W1529537962 creator A5074060343 @default.
• W1529537962 creator A5082778488 @default.
• W1529537962 creator A5086284188 @default.
• W1529537962 creator A5089252187 @default.
• W1529537962 creator A5023176439 @default.
• W1529537962 date "2015-06-15" @default.
• W1529537962 modified "2023-10-12" @default.
• W1529537962 title "Rationally designed chemokine-based toxin targeting the viral G protein-coupled receptor US28 potently inhibits cytomegalovirus infection in vivo" @default.
• W1529537962 cites W1566903555 @default.
• W1529537962 cites W1589088345 @default.
• W1529537962 cites W1968206013 @default.
• W1529537962 cites W1970291943 @default.
• W1529537962 cites W1972809208 @default.
• W1529537962 cites W1973323812 @default.
• W1529537962 cites W1974624016 @default.
• W1529537962 cites W1981593721 @default.
• W1529537962 cites W1984007340 @default.
• W1529537962 cites W1984115097 @default.
• W1529537962 cites W1987061694 @default.
• W1529537962 cites W1987888973 @default.
• W1529537962 cites W1988778953 @default.
• W1529537962 cites W1996558200 @default.
• W1529537962 cites W2001385539 @default.
• W1529537962 cites W2006973742 @default.
• W1529537962 cites W2009013652 @default.
• W1529537962 cites W2014608550 @default.
• W1529537962 cites W2017214646 @default.
• W1529537962 cites W2018624173 @default.
• W1529537962 cites W2025338891 @default.
• W1529537962 cites W2027331988 @default.
• W1529537962 cites W2030261483 @default.
• W1529537962 cites W2032612463 @default.
• W1529537962 cites W2057623646 @default.
• W1529537962 cites W2064841628 @default.
• W1529537962 cites W2068392260 @default.
• W1529537962 cites W2073357767 @default.
• W1529537962 cites W2083483697 @default.
• W1529537962 cites W2102598864 @default.
• W1529537962 cites W2107003632 @default.
• W1529537962 cites W2127354313 @default.
• W1529537962 cites W2128119454 @default.
• W1529537962 cites W2129285015 @default.
• W1529537962 cites W2129743309 @default.
• W1529537962 cites W2132025920 @default.
• W1529537962 cites W2139214028 @default.
• W1529537962 cites W2147120870 @default.
• W1529537962 cites W2149690064 @default.
• W1529537962 cites W2150427022 @default.
• W1529537962 cites W2157329817 @default.
• W1529537962 cites W2160000072 @default.
• W1529537962 cites W2168046861 @default.
• W1529537962 cites W2314406250 @default.
• W1529537962 cites W2317862388 @default.
• W1529537962 cites W4246519760 @default.
• W1529537962 doi "https://doi.org/10.1073/pnas.1509392112" @default.
• W1529537962 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/4500259" @default.
• W1529537962 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/26080445" @default.
• W1529537962 hasPublicationYear "2015" @default.
• W1529537962 type Work @default.
• W1529537962 sameAs 1529537962 @default.
• W1529537962 citedByCount "43" @default.
• W1529537962 countsByYear W15295379622015 @default.
• W1529537962 countsByYear W15295379622016 @default.
• W1529537962 countsByYear W15295379622017 @default.
• W1529537962 countsByYear W15295379622018 @default.
• W1529537962 countsByYear W15295379622019 @default.
• W1529537962 countsByYear W15295379622020 @default.
• W1529537962 countsByYear W15295379622021 @default.
• W1529537962 countsByYear W15295379622022 @default.
• W1529537962 countsByYear W15295379622023 @default.
• W1529537962 crossrefType "journal-article" @default.
• W1529537962 hasAuthorship W1529537962A5005540598 @default.
• W1529537962 hasAuthorship W1529537962A5017426114 @default.
• W1529537962 hasAuthorship W1529537962A5021248446 @default.
• W1529537962 hasAuthorship W1529537962A5023176439 @default.
• W1529537962 hasAuthorship W1529537962A5034044681 @default.
• W1529537962 hasAuthorship W1529537962A5035872776 @default.
• W1529537962 hasAuthorship W1529537962A5046607220 @default.
• W1529537962 hasAuthorship W1529537962A5051522561 @default.
• W1529537962 hasAuthorship W1529537962A5057973675 @default.
• W1529537962 hasAuthorship W1529537962A5071806328 @default.
• W1529537962 hasAuthorship W1529537962A5074060343 @default.
• W1529537962 hasAuthorship W1529537962A5082778488 @default.
• W1529537962 hasAuthorship W1529537962A5086284188 @default.
• W1529537962 hasAuthorship W1529537962A5089252187 @default.
• W1529537962 hasBestOaLocation W15295379621 @default.
• W1529537962 hasConcept C104317684 @default.

• next