SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2129059670> ?p ?o ?g. }

Showing items 1 to 100 of ±146 with 100 items per page.

W2129059670 endingPage "730" @default.
W2129059670 startingPage "717" @default.
W2129059670 abstract "T cell epitope peptides derived from proteolipid protein (PLP139–151) or myelin basic protein (MBP86–100) induce experimental autoimmune encephalomyelitis (EAE) in “susceptible” strains of mice (e.g., SJL/J). In this study, we show that the encephalitogenic effect of these epitopes when injected subcutaneously in complete Freund's adjuvant was significantly enhanced if administered to the animal in a multimerized form as a T cell epitope oligomer (i.e., as multiple repeats of the peptide epitope, such as 16-mers). Oligomer-treated SJL/J mice developed EAE faster and showed a more severe progression of the disease than animals treated with peptide alone. In addition, haplotype-matched B10.S mice, “resistant” to EAE induction by peptide, on injection of 16-mers developed a severe form of EAE. Even more striking, however, was the dramatic suppression of incidence and severity of the disease, seen after single intravenous injections of only 50 μg of the PLP139–151 16-mer, administered to SJL/J mice 7 d after the induction of the disease. Although relapse occurred at about day 45, an additional injection several days before that maintained the suppression. Importantly, the specific suppressive effect of oligomer treatment was also evident if EAE was induced with spinal cord homogenate instead of the single peptide antigen. By contrast, the PLP139–151 peptide accelerated rather than retarded the progression of disease." @default.
W2129059670 created "2016-06-24" @default.
W2129059670 creator A5000314838 @default.
W2129059670 creator A5019713118 @default.
W2129059670 creator A5024159365 @default.
W2129059670 creator A5037605110 @default.
W2129059670 creator A5040129865 @default.
W2129059670 creator A5073296118 @default.
W2129059670 date "2000-02-21" @default.
W2129059670 modified "2023-10-14" @default.
W2129059670 title "Induction and Suppression of an Autoimmune Disease by Oligomerized T Cell Epitopes" @default.
W2129059670 cites W109817324 @default.
W2129059670 cites W1562022567 @default.
W2129059670 cites W1583354177 @default.
W2129059670 cites W1619327403 @default.
W2129059670 cites W1771941672 @default.
W2129059670 cites W1877895673 @default.
W2129059670 cites W1898802354 @default.
W2129059670 cites W1941317616 @default.
W2129059670 cites W1977658278 @default.
W2129059670 cites W1997157937 @default.
W2129059670 cites W2000048275 @default.
W2129059670 cites W2003691176 @default.
W2129059670 cites W2009660482 @default.
W2129059670 cites W2013642092 @default.
W2129059670 cites W2014954180 @default.
W2129059670 cites W2017243368 @default.
W2129059670 cites W2023561229 @default.
W2129059670 cites W2025001946 @default.
W2129059670 cites W2025445086 @default.
W2129059670 cites W2028852768 @default.
W2129059670 cites W2032747803 @default.
W2129059670 cites W2033919411 @default.
W2129059670 cites W2034160116 @default.
W2129059670 cites W2035488110 @default.
W2129059670 cites W2041404362 @default.
W2129059670 cites W2043837690 @default.
W2129059670 cites W2044316391 @default.
W2129059670 cites W2052502606 @default.
W2129059670 cites W2066016513 @default.
W2129059670 cites W2067069532 @default.
W2129059670 cites W2067071374 @default.
W2129059670 cites W2070530924 @default.
W2129059670 cites W2084916103 @default.
W2129059670 cites W2085414987 @default.
W2129059670 cites W2103858336 @default.
W2129059670 cites W2125595905 @default.
W2129059670 cites W2133621763 @default.
W2129059670 cites W2134453100 @default.
W2129059670 cites W2144818921 @default.
W2129059670 cites W2149497800 @default.
W2129059670 cites W2151475642 @default.
W2129059670 cites W2153544097 @default.
W2129059670 cites W2159756478 @default.
W2129059670 cites W2160659449 @default.
W2129059670 cites W2412319492 @default.
W2129059670 cites W48399004 @default.
W2129059670 doi "https://doi.org/10.1084/jem.191.4.717" @default.
W2129059670 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/2195838" @default.
W2129059670 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/10684863" @default.
W2129059670 hasPublicationYear "2000" @default.
W2129059670 type Work @default.
W2129059670 sameAs 2129059670 @default.
W2129059670 citedByCount "44" @default.
W2129059670 countsByYear W21290596702012 @default.
W2129059670 countsByYear W21290596702013 @default.
W2129059670 countsByYear W21290596702016 @default.
W2129059670 countsByYear W21290596702019 @default.
W2129059670 countsByYear W21290596702021 @default.
W2129059670 countsByYear W21290596702023 @default.
W2129059670 crossrefType "journal-article" @default.
W2129059670 hasAuthorship W2129059670A5000314838 @default.
W2129059670 hasAuthorship W2129059670A5019713118 @default.
W2129059670 hasAuthorship W2129059670A5024159365 @default.
W2129059670 hasAuthorship W2129059670A5037605110 @default.
W2129059670 hasAuthorship W2129059670A5040129865 @default.
W2129059670 hasAuthorship W2129059670A5073296118 @default.
W2129059670 hasBestOaLocation W21290596701 @default.
W2129059670 hasConcept C134018914 @default.
W2129059670 hasConcept C147483822 @default.
W2129059670 hasConcept C153911025 @default.
W2129059670 hasConcept C159654299 @default.
W2129059670 hasConcept C195616568 @default.
W2129059670 hasConcept C203014093 @default.
W2129059670 hasConcept C2776090121 @default.
W2129059670 hasConcept C2777426553 @default.
W2129059670 hasConcept C2777863537 @default.
W2129059670 hasConcept C2777899865 @default.
W2129059670 hasConcept C2778486448 @default.
W2129059670 hasConcept C2778609137 @default.
W2129059670 hasConcept C2779075594 @default.
W2129059670 hasConcept C2779281246 @default.
W2129059670 hasConcept C2780130043 @default.
W2129059670 hasConcept C2780640218 @default.
W2129059670 hasConcept C2780876595 @default.
W2129059670 hasConcept C529278444 @default.
W2129059670 hasConcept C55493867 @default.
W2129059670 hasConcept C7821365 @default.