FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W112486650> ?p ?o ?g. }

• W112486650 endingPage "1330" @default.
• W112486650 startingPage "1323" @default.
• W112486650 abstract "A strong transcriptional enhancer was created by oligomerization of a short segment from the immunoglobulin heavy chain (IgH) enhancer. This segment was analyzed in parallel for biological activity in vivo and factor binding in vitro. In transfection experiments the oligomerized segment stimulates transcription in a cell type-specific manner similar to the entire IgH enhancer. Transfections of mutants identified two sequence motifs whose integrity is required for efficient and cell type-specific activity of this enhancer. The first is a sequence suggested previously to be bound by a factor in vivo, and the second is a highly conserved decanucleotide which also occurs in Ig variable gene promoters. The ability of these two sequence motifs to bind proteins in vitro was tested by band shift assays. Under our in vitro conditions we could not detect proteins binding to the in vivo footprint region. However, we found protein factors binding to the decanucleotide. A ubiquitous form of this factor is present in every cell line analyzed. Additional variants are detected exclusively in cells where the IgH enhancer and the segment thereof are active. Elimination of the decanucleotide motif is not only a strong down mutation in vivo but also abolishes binding of all factor variants in vitro. Thus our data suggest that the two enhancer motifs analyzed are involved in positive rather than negative control of transcription." @default.
• W112486650 created "2016-06-24" @default.
• W112486650 creator A5041009980 @default.
• W112486650 creator A5047979903 @default.
• W112486650 creator A5071043734 @default.
• W112486650 creator A5072633844 @default.
• W112486650 creator A5077535856 @default.
• W112486650 date "1987-05-01" @default.
• W112486650 modified "2023-09-28" @default.
• W112486650 title "Cell type-specificity elements of the immunoglobulin heavy chain gene enhancer." @default.
• W112486650 cites W126863029 @default.
• W112486650 cites W145927914 @default.
• W112486650 cites W1579796122 @default.
• W112486650 cites W1774422856 @default.
• W112486650 cites W1775639561 @default.
• W112486650 cites W1857597002 @default.
• W112486650 cites W1929658734 @default.
• W112486650 cites W1965267927 @default.
• W112486650 cites W1968075576 @default.
• W112486650 cites W1971285426 @default.
• W112486650 cites W1977209713 @default.
• W112486650 cites W1977950418 @default.
• W112486650 cites W1978439483 @default.
• W112486650 cites W1983253653 @default.
• W112486650 cites W1986291674 @default.
• W112486650 cites W1993243592 @default.
• W112486650 cites W1993280477 @default.
• W112486650 cites W1993984366 @default.
• W112486650 cites W2001187632 @default.
• W112486650 cites W2002499610 @default.
• W112486650 cites W2002873026 @default.
• W112486650 cites W2004563262 @default.
• W112486650 cites W2006761445 @default.
• W112486650 cites W2013545053 @default.
• W112486650 cites W2018352453 @default.
• W112486650 cites W2027469396 @default.
• W112486650 cites W2030696171 @default.
• W112486650 cites W2031300940 @default.
• W112486650 cites W2035434814 @default.
• W112486650 cites W2038218774 @default.
• W112486650 cites W2043070717 @default.
• W112486650 cites W2045583364 @default.
• W112486650 cites W2057893650 @default.
• W112486650 cites W2058212923 @default.
• W112486650 cites W2059576474 @default.
• W112486650 cites W2063586844 @default.
• W112486650 cites W2068926754 @default.
• W112486650 cites W2071771940 @default.
• W112486650 cites W2074596664 @default.
• W112486650 cites W2088094960 @default.
• W112486650 cites W2088272992 @default.
• W112486650 cites W2089593395 @default.
• W112486650 cites W2093988305 @default.
• W112486650 cites W2094571268 @default.
• W112486650 cites W2105580594 @default.
• W112486650 cites W2108734957 @default.
• W112486650 cites W2125792044 @default.
• W112486650 cites W2127297640 @default.
• W112486650 cites W2149563853 @default.
• W112486650 cites W2158837478 @default.
• W112486650 cites W2161524167 @default.
• W112486650 cites W2174692915 @default.
• W112486650 cites W2208849928 @default.
• W112486650 cites W2416131873 @default.
• W112486650 cites W2428905324 @default.
• W112486650 cites W2578150941 @default.
• W112486650 cites W324734061 @default.
• W112486650 doi "https://doi.org/10.1002/j.1460-2075.1987.tb02371.x" @default.
• W112486650 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/553936" @default.
• W112486650 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/3038516" @default.
• W112486650 hasPublicationYear "1987" @default.
• W112486650 type Work @default.
• W112486650 sameAs 112486650 @default.
• W112486650 citedByCount "242" @default.
• W112486650 countsByYear W1124866502015 @default.
• W112486650 crossrefType "journal-article" @default.
• W112486650 hasAuthorship W112486650A5041009980 @default.
• W112486650 hasAuthorship W112486650A5047979903 @default.
• W112486650 hasAuthorship W112486650A5071043734 @default.
• W112486650 hasAuthorship W112486650A5072633844 @default.
• W112486650 hasAuthorship W112486650A5077535856 @default.
• W112486650 hasBestOaLocation W1124866501 @default.
• W112486650 hasConcept C101762097 @default.
• W112486650 hasConcept C104317684 @default.
• W112486650 hasConcept C111936080 @default.
• W112486650 hasConcept C143065580 @default.
• W112486650 hasConcept C150194340 @default.
• W112486650 hasConcept C153911025 @default.
• W112486650 hasConcept C167625842 @default.
• W112486650 hasConcept C199216141 @default.
• W112486650 hasConcept C202751555 @default.
• W112486650 hasConcept C21592294 @default.
• W112486650 hasConcept C21784809 @default.
• W112486650 hasConcept C54355233 @default.
• W112486650 hasConcept C86339819 @default.
• W112486650 hasConcept C86803240 @default.
• W112486650 hasConcept C94966510 @default.
• W112486650 hasConcept C95444343 @default.

• next