FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W1997577538> ?p ?o ?g. }

• W1997577538 endingPage "2138" @default.
• W1997577538 startingPage "2129" @default.
• W1997577538 abstract "CD103 (alphaEbeta7) has been shown to be an excellent marker for identifying in vivo-activated FoxP3(+)CD4(+) regulatory T (Treg) cells. It is unknown whether reinfusion of in vivo-activated donor-type CD103(+) Treg cells from recipient can ameliorate ongoing chronic graft-versus-host disease (GVHD). Here, we showed that, in a chronic GVHD model of DBA/2 (H-2(d)) donor to BALB/c (H-2(d)) recipient, donor-type CD103(+) Treg cells from recipients were much more potent than CD25(hi) natural Treg cells from donors in reversing clinical signs of GVHD and tissue damage. Furthermore, in contrast to CD25(hi) natural Treg cells, CD103(+) Treg cells expressed high levels of CCR5 but low levels of CD62L and directly migrated to GVHD target tissues. In addition, the CD103(+) Treg cells strongly suppressed donor CD4(+) T-cell proliferation; they also induced apoptosis of in vivo-activated CD4(+) T and B cells and significantly reduced pathogenic T and B cells in GVHD target tissues. These results indicate that CD103(+) Treg cells from chronic GVHD recipients are functional, and reinfusion of the CD103(+) Treg cells can shift the balance between Treg cells and pathogenic T cells in chronic GVHD recipients and ameliorate ongoing disease." @default.
• W1997577538 created "2016-06-24" @default.
• W1997577538 creator A5000015397 @default.
• W1997577538 creator A5006842293 @default.
• W1997577538 creator A5009269974 @default.
• W1997577538 creator A5021119678 @default.
• W1997577538 creator A5039374832 @default.
• W1997577538 creator A5077212585 @default.
• W1997577538 creator A5081864075 @default.
• W1997577538 creator A5087227188 @default.
• W1997577538 date "2008-09-01" @default.
• W1997577538 modified "2023-10-02" @default.
• W1997577538 title "In vivo–activated CD103+CD4+ regulatory T cells ameliorate ongoing chronic graft-versus-host disease" @default.
• W1997577538 cites W1525863788 @default.
• W1997577538 cites W1527630965 @default.
• W1997577538 cites W1626051903 @default.
• W1997577538 cites W1661359408 @default.
• W1997577538 cites W1828603026 @default.
• W1997577538 cites W1964616348 @default.
• W1997577538 cites W1966073503 @default.
• W1997577538 cites W1966738123 @default.
• W1997577538 cites W1988361537 @default.
• W1997577538 cites W1991344211 @default.
• W1997577538 cites W2003407014 @default.
• W1997577538 cites W2004708987 @default.
• W1997577538 cites W2006249161 @default.
• W1997577538 cites W2018815039 @default.
• W1997577538 cites W2025694570 @default.
• W1997577538 cites W2031398803 @default.
• W1997577538 cites W2036872637 @default.
• W1997577538 cites W2037259928 @default.
• W1997577538 cites W2039817295 @default.
• W1997577538 cites W2042952613 @default.
• W1997577538 cites W2047762573 @default.
• W1997577538 cites W2063491568 @default.
• W1997577538 cites W2063966481 @default.
• W1997577538 cites W2066197042 @default.
• W1997577538 cites W2074181748 @default.
• W1997577538 cites W2075010539 @default.
• W1997577538 cites W2085704445 @default.
• W1997577538 cites W2100088787 @default.
• W1997577538 cites W2105970563 @default.
• W1997577538 cites W2107631420 @default.
• W1997577538 cites W2108639843 @default.
• W1997577538 cites W2110957620 @default.
• W1997577538 cites W2119173517 @default.
• W1997577538 cites W2119624288 @default.
• W1997577538 cites W2133765154 @default.
• W1997577538 cites W2135280067 @default.
• W1997577538 cites W2141812411 @default.
• W1997577538 cites W2144836936 @default.
• W1997577538 cites W2145030204 @default.
• W1997577538 cites W2145708130 @default.
• W1997577538 cites W2148806075 @default.
• W1997577538 cites W2155779547 @default.
• W1997577538 cites W2157325100 @default.
• W1997577538 cites W2157979692 @default.
• W1997577538 cites W2158485667 @default.
• W1997577538 cites W2163855374 @default.
• W1997577538 cites W2166083796 @default.
• W1997577538 cites W2166438464 @default.
• W1997577538 cites W2169108727 @default.
• W1997577538 cites W2169969151 @default.
• W1997577538 cites W4235950651 @default.
• W1997577538 cites W4256235973 @default.
• W1997577538 cites W4313379132 @default.
• W1997577538 doi "https://doi.org/10.1182/blood-2008-02-140277" @default.
• W1997577538 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/2518910" @default.
• W1997577538 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/18550852" @default.
• W1997577538 hasPublicationYear "2008" @default.
• W1997577538 type Work @default.
• W1997577538 sameAs 1997577538 @default.
• W1997577538 citedByCount "127" @default.
• W1997577538 countsByYear W19975775382012 @default.
• W1997577538 countsByYear W19975775382013 @default.
• W1997577538 countsByYear W19975775382014 @default.
• W1997577538 countsByYear W19975775382015 @default.
• W1997577538 countsByYear W19975775382016 @default.
• W1997577538 countsByYear W19975775382017 @default.
• W1997577538 countsByYear W19975775382018 @default.
• W1997577538 countsByYear W19975775382019 @default.
• W1997577538 countsByYear W19975775382020 @default.
• W1997577538 countsByYear W19975775382021 @default.
• W1997577538 countsByYear W19975775382022 @default.
• W1997577538 countsByYear W19975775382023 @default.
• W1997577538 crossrefType "journal-article" @default.
• W1997577538 hasAuthorship W1997577538A5000015397 @default.
• W1997577538 hasAuthorship W1997577538A5006842293 @default.
• W1997577538 hasAuthorship W1997577538A5009269974 @default.
• W1997577538 hasAuthorship W1997577538A5021119678 @default.
• W1997577538 hasAuthorship W1997577538A5039374832 @default.
• W1997577538 hasAuthorship W1997577538A5077212585 @default.
• W1997577538 hasAuthorship W1997577538A5081864075 @default.
• W1997577538 hasAuthorship W1997577538A5087227188 @default.
• W1997577538 hasBestOaLocation W19975775381 @default.
• W1997577538 hasConcept C126322002 @default.
• W1997577538 hasConcept C150903083 @default.
• W1997577538 hasConcept C203014093 @default.

• next