PubMed:8662928 JSONTXT

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    sentences

    {"project":"sentences","denotations":[{"id":"T1","span":{"begin":0,"end":149},"obj":"Sentence"},{"id":"T2","span":{"begin":150,"end":452},"obj":"Sentence"},{"id":"T3","span":{"begin":453,"end":653},"obj":"Sentence"},{"id":"T4","span":{"begin":654,"end":756},"obj":"Sentence"},{"id":"T5","span":{"begin":757,"end":864},"obj":"Sentence"},{"id":"T6","span":{"begin":865,"end":1065},"obj":"Sentence"},{"id":"T7","span":{"begin":1066,"end":1197},"obj":"Sentence"},{"id":"T8","span":{"begin":1198,"end":1280},"obj":"Sentence"},{"id":"T9","span":{"begin":1281,"end":1491},"obj":"Sentence"},{"id":"T10","span":{"begin":1492,"end":1582},"obj":"Sentence"},{"id":"T11","span":{"begin":1583,"end":1741},"obj":"Sentence"},{"id":"T12","span":{"begin":1742,"end":1921},"obj":"Sentence"},{"id":"T13","span":{"begin":1922,"end":2105},"obj":"Sentence"},{"id":"T1","span":{"begin":0,"end":149},"obj":"Sentence"},{"id":"T2","span":{"begin":150,"end":452},"obj":"Sentence"},{"id":"T3","span":{"begin":453,"end":653},"obj":"Sentence"},{"id":"T4","span":{"begin":654,"end":756},"obj":"Sentence"},{"id":"T5","span":{"begin":757,"end":864},"obj":"Sentence"},{"id":"T6","span":{"begin":865,"end":1065},"obj":"Sentence"},{"id":"T7","span":{"begin":1066,"end":1197},"obj":"Sentence"},{"id":"T8","span":{"begin":1198,"end":1280},"obj":"Sentence"},{"id":"T9","span":{"begin":1281,"end":1491},"obj":"Sentence"},{"id":"T10","span":{"begin":1492,"end":1582},"obj":"Sentence"},{"id":"T11","span":{"begin":1583,"end":1741},"obj":"Sentence"},{"id":"T12","span":{"begin":1742,"end":1921},"obj":"Sentence"},{"id":"T13","span":{"begin":1922,"end":2105},"obj":"Sentence"}],"namespaces":[{"prefix":"_base","uri":"http://pubannotation.org/ontology/tao.owl#"}],"text":"Receptors for interleukin (IL)-10 and IL-6-type cytokines use similar signaling mechanisms for inducing transcription through IL-6 response elements.\nThe cytoplasmic domain of the receptor for interleukin 10 (IL-10R) contains two box 3 sequence motifs that have been identified in the signal-transducing receptor subunits for IL-6-type cytokines and noted to be required for activating STAT3 and inducing transcription through IL-6-responsive elements. To determine whether the IL-10R has signaling functions similar to IL-6R in cells normally expressing these receptors, leukocytes of the B-, T-, and NK-cell lineages were treated with either cytokine. Both cytokines activated factors that bound to the sis-inducible element and included STAT1 and STAT3. The cell response to IL-10 characteristically differed from that to IL-2/IL-15, IL-4, and interferon gamma. The signaling capabilities of the IL-10R for activating specific STAT proteins and inducing gene transcription were defined by reconstitution of receptor functions in transfected tissue culture cells. COS-1 cells, co-expressing the human IL-10R and individual STAT proteins, confirmed a preference of the IL-10R for STAT3 and STAT1. Unlike many hematopoietin receptors, the IL-10R did not detectably activate STAT5. The IL-10R, together with reporter gene constructs containing different IL-6-responsive gene elements, reconstituted in hepatoma cells an induction of transcription by IL-10 that was comparable to that by IL-6. This regulation could not be appreciably modified by enhanced expression of STAT proteins. The similar actions of IL-10R and IL-6R on the induction of endogenous IL-6-responsive genes were demonstrated in hepatoma cells stably expressing the IL-10R. These receptor functions required the presence of the box 3 motifs, as shown by the analysis of the mouse IL-10R constructs containing progressively truncated cytoplasmic domains. The data demonstrate that the IL-10R, unlike other members of the interferon receptor family, is highly effective in recruiting the signaling pathways of IL-6-type cytokine receptors."}

    jnlpba-st-training

    {"project":"jnlpba-st-training","denotations":[{"id":"T1","span":{"begin":14,"end":57},"obj":"protein"},{"id":"T2","span":{"begin":126,"end":148},"obj":"DNA"},{"id":"T3","span":{"begin":154,"end":172},"obj":"protein"},{"id":"T4","span":{"begin":193,"end":207},"obj":"protein"},{"id":"T5","span":{"begin":209,"end":215},"obj":"protein"},{"id":"T6","span":{"begin":230,"end":251},"obj":"protein"},{"id":"T7","span":{"begin":285,"end":321},"obj":"protein"},{"id":"T8","span":{"begin":326,"end":345},"obj":"protein"},{"id":"T9","span":{"begin":386,"end":391},"obj":"protein"},{"id":"T10","span":{"begin":427,"end":451},"obj":"DNA"},{"id":"T11","span":{"begin":478,"end":484},"obj":"protein"},{"id":"T12","span":{"begin":520,"end":525},"obj":"protein"},{"id":"T13","span":{"begin":572,"end":582},"obj":"cell_type"},{"id":"T14","span":{"begin":590,"end":618},"obj":"cell_type"},{"id":"T15","span":{"begin":659,"end":668},"obj":"protein"},{"id":"T16","span":{"begin":705,"end":726},"obj":"DNA"},{"id":"T17","span":{"begin":740,"end":745},"obj":"protein"},{"id":"T18","span":{"begin":750,"end":755},"obj":"protein"},{"id":"T19","span":{"begin":778,"end":783},"obj":"protein"},{"id":"T20","span":{"begin":825,"end":835},"obj":"protein"},{"id":"T21","span":{"begin":837,"end":841},"obj":"protein"},{"id":"T22","span":{"begin":847,"end":863},"obj":"protein"},{"id":"T23","span":{"begin":899,"end":905},"obj":"protein"},{"id":"T24","span":{"begin":930,"end":943},"obj":"protein"},{"id":"T25","span":{"begin":1032,"end":1064},"obj":"cell_line"},{"id":"T26","span":{"begin":1066,"end":1077},"obj":"cell_line"},{"id":"T27","span":{"begin":1103,"end":1109},"obj":"protein"},{"id":"T28","span":{"begin":1125,"end":1138},"obj":"protein"},{"id":"T29","span":{"begin":1170,"end":1176},"obj":"protein"},{"id":"T30","span":{"begin":1181,"end":1186},"obj":"protein"},{"id":"T31","span":{"begin":1191,"end":1196},"obj":"protein"},{"id":"T32","span":{"begin":1210,"end":1233},"obj":"protein"},{"id":"T33","span":{"begin":1239,"end":1245},"obj":"protein"},{"id":"T34","span":{"begin":1274,"end":1279},"obj":"protein"},{"id":"T35","span":{"begin":1285,"end":1291},"obj":"protein"},{"id":"T36","span":{"begin":1353,"end":1382},"obj":"DNA"},{"id":"T37","span":{"begin":1401,"end":1415},"obj":"cell_type"},{"id":"T38","span":{"begin":1449,"end":1454},"obj":"protein"},{"id":"T39","span":{"begin":1486,"end":1490},"obj":"protein"},{"id":"T40","span":{"begin":1568,"end":1581},"obj":"protein"},{"id":"T41","span":{"begin":1606,"end":1612},"obj":"protein"},{"id":"T42","span":{"begin":1617,"end":1622},"obj":"protein"},{"id":"T43","span":{"begin":1654,"end":1675},"obj":"DNA"},{"id":"T44","span":{"begin":1697,"end":1711},"obj":"cell_type"},{"id":"T45","span":{"begin":1734,"end":1740},"obj":"protein"},{"id":"T46","span":{"begin":1796,"end":1808},"obj":"protein"},{"id":"T47","span":{"begin":1848,"end":1854},"obj":"protein"},{"id":"T48","span":{"begin":1877,"end":1920},"obj":"protein"},{"id":"T49","span":{"begin":1952,"end":1958},"obj":"protein"},{"id":"T50","span":{"begin":2076,"end":2104},"obj":"protein"}],"text":"Receptors for interleukin (IL)-10 and IL-6-type cytokines use similar signaling mechanisms for inducing transcription through IL-6 response elements.\nThe cytoplasmic domain of the receptor for interleukin 10 (IL-10R) contains two box 3 sequence motifs that have been identified in the signal-transducing receptor subunits for IL-6-type cytokines and noted to be required for activating STAT3 and inducing transcription through IL-6-responsive elements. To determine whether the IL-10R has signaling functions similar to IL-6R in cells normally expressing these receptors, leukocytes of the B-, T-, and NK-cell lineages were treated with either cytokine. Both cytokines activated factors that bound to the sis-inducible element and included STAT1 and STAT3. The cell response to IL-10 characteristically differed from that to IL-2/IL-15, IL-4, and interferon gamma. The signaling capabilities of the IL-10R for activating specific STAT proteins and inducing gene transcription were defined by reconstitution of receptor functions in transfected tissue culture cells. COS-1 cells, co-expressing the human IL-10R and individual STAT proteins, confirmed a preference of the IL-10R for STAT3 and STAT1. Unlike many hematopoietin receptors, the IL-10R did not detectably activate STAT5. The IL-10R, together with reporter gene constructs containing different IL-6-responsive gene elements, reconstituted in hepatoma cells an induction of transcription by IL-10 that was comparable to that by IL-6. This regulation could not be appreciably modified by enhanced expression of STAT proteins. The similar actions of IL-10R and IL-6R on the induction of endogenous IL-6-responsive genes were demonstrated in hepatoma cells stably expressing the IL-10R. These receptor functions required the presence of the box 3 motifs, as shown by the analysis of the mouse IL-10R constructs containing progressively truncated cytoplasmic domains. The data demonstrate that the IL-10R, unlike other members of the interferon receptor family, is highly effective in recruiting the signaling pathways of IL-6-type cytokine receptors."}

    pubmed-sentences-benchmark

    {"project":"pubmed-sentences-benchmark","denotations":[{"id":"S1","span":{"begin":0,"end":149},"obj":"Sentence"},{"id":"S2","span":{"begin":150,"end":452},"obj":"Sentence"},{"id":"S3","span":{"begin":453,"end":653},"obj":"Sentence"},{"id":"S4","span":{"begin":654,"end":756},"obj":"Sentence"},{"id":"S5","span":{"begin":757,"end":864},"obj":"Sentence"},{"id":"S6","span":{"begin":865,"end":1065},"obj":"Sentence"},{"id":"S7","span":{"begin":1066,"end":1197},"obj":"Sentence"},{"id":"S8","span":{"begin":1198,"end":1280},"obj":"Sentence"},{"id":"S9","span":{"begin":1281,"end":1491},"obj":"Sentence"},{"id":"S10","span":{"begin":1492,"end":1582},"obj":"Sentence"},{"id":"S11","span":{"begin":1583,"end":1741},"obj":"Sentence"},{"id":"S12","span":{"begin":1742,"end":1921},"obj":"Sentence"},{"id":"S13","span":{"begin":1922,"end":2105},"obj":"Sentence"}],"text":"Receptors for interleukin (IL)-10 and IL-6-type cytokines use similar signaling mechanisms for inducing transcription through IL-6 response elements.\nThe cytoplasmic domain of the receptor for interleukin 10 (IL-10R) contains two box 3 sequence motifs that have been identified in the signal-transducing receptor subunits for IL-6-type cytokines and noted to be required for activating STAT3 and inducing transcription through IL-6-responsive elements. To determine whether the IL-10R has signaling functions similar to IL-6R in cells normally expressing these receptors, leukocytes of the B-, T-, and NK-cell lineages were treated with either cytokine. Both cytokines activated factors that bound to the sis-inducible element and included STAT1 and STAT3. The cell response to IL-10 characteristically differed from that to IL-2/IL-15, IL-4, and interferon gamma. The signaling capabilities of the IL-10R for activating specific STAT proteins and inducing gene transcription were defined by reconstitution of receptor functions in transfected tissue culture cells. COS-1 cells, co-expressing the human IL-10R and individual STAT proteins, confirmed a preference of the IL-10R for STAT3 and STAT1. Unlike many hematopoietin receptors, the IL-10R did not detectably activate STAT5. The IL-10R, together with reporter gene constructs containing different IL-6-responsive gene elements, reconstituted in hepatoma cells an induction of transcription by IL-10 that was comparable to that by IL-6. This regulation could not be appreciably modified by enhanced expression of STAT proteins. The similar actions of IL-10R and IL-6R on the induction of endogenous IL-6-responsive genes were demonstrated in hepatoma cells stably expressing the IL-10R. These receptor functions required the presence of the box 3 motifs, as shown by the analysis of the mouse IL-10R constructs containing progressively truncated cytoplasmic domains. The data demonstrate that the IL-10R, unlike other members of the interferon receptor family, is highly effective in recruiting the signaling pathways of IL-6-type cytokine receptors."}

    genia-medco-coref

    {"project":"genia-medco-coref","denotations":[{"id":"C2","span":{"begin":14,"end":33},"obj":"NP"},{"id":"C43","span":{"begin":38,"end":43},"obj":"NP"},{"id":"C6","span":{"begin":38,"end":57},"obj":"NP"},{"id":"C17","span":{"begin":14,"end":57},"obj":"NP"},{"id":"C15","span":{"begin":0,"end":57},"obj":"NP"},{"id":"C8","span":{"begin":126,"end":148},"obj":"NP"},{"id":"C10","span":{"begin":104,"end":148},"obj":"NP"},{"id":"C1","span":{"begin":193,"end":207},"obj":"NP"},{"id":"C3","span":{"begin":176,"end":216},"obj":"NP"},{"id":"C4","span":{"begin":226,"end":251},"obj":"NP"},{"id":"C5","span":{"begin":252,"end":256},"obj":"NP"},{"id":"C44","span":{"begin":326,"end":331},"obj":"NP"},{"id":"C7","span":{"begin":326,"end":345},"obj":"NP"},{"id":"C20","span":{"begin":386,"end":391},"obj":"NP"},{"id":"C45","span":{"begin":427,"end":432},"obj":"NP"},{"id":"C9","span":{"begin":427,"end":451},"obj":"NP"},{"id":"C11","span":{"begin":405,"end":451},"obj":"NP"},{"id":"C12","span":{"begin":474,"end":484},"obj":"NP"},{"id":"C13","span":{"begin":520,"end":525},"obj":"NP"},{"id":"C14","span":{"begin":555,"end":570},"obj":"NP"},{"id":"C16","span":{"begin":654,"end":668},"obj":"NP"},{"id":"C18","span":{"begin":679,"end":686},"obj":"NP"},{"id":"C19","span":{"begin":687,"end":691},"obj":"NP"},{"id":"C29","span":{"begin":740,"end":745},"obj":"NP"},{"id":"C21","span":{"begin":750,"end":755},"obj":"NP"},{"id":"C23","span":{"begin":757,"end":774},"obj":"NP"},{"id":"C22","span":{"begin":778,"end":783},"obj":"NP"},{"id":"C24","span":{"begin":817,"end":821},"obj":"NP"},{"id":"C25","span":{"begin":895,"end":905},"obj":"NP"},{"id":"C26","span":{"begin":1093,"end":1109},"obj":"NP"},{"id":"C27","span":{"begin":1166,"end":1176},"obj":"NP"},{"id":"C28","span":{"begin":1181,"end":1186},"obj":"NP"},{"id":"C30","span":{"begin":1191,"end":1196},"obj":"NP"},{"id":"C31","span":{"begin":1235,"end":1245},"obj":"NP"},{"id":"C32","span":{"begin":1281,"end":1291},"obj":"NP"},{"id":"C46","span":{"begin":1353,"end":1358},"obj":"NP"},{"id":"C33","span":{"begin":1449,"end":1454},"obj":"NP"},{"id":"C34","span":{"begin":1416,"end":1454},"obj":"NP"},{"id":"C35","span":{"begin":1455,"end":1459},"obj":"NP"},{"id":"C36","span":{"begin":1486,"end":1490},"obj":"NP"},{"id":"C37","span":{"begin":1606,"end":1612},"obj":"NP"},{"id":"C38","span":{"begin":1617,"end":1622},"obj":"NP"},{"id":"C47","span":{"begin":1654,"end":1659},"obj":"NP"},{"id":"C39","span":{"begin":1730,"end":1740},"obj":"NP"},{"id":"C40","span":{"begin":1792,"end":1808},"obj":"NP"},{"id":"C41","span":{"begin":1948,"end":1958},"obj":"NP"},{"id":"C48","span":{"begin":2076,"end":2081},"obj":"NP"},{"id":"C42","span":{"begin":2076,"end":2104},"obj":"NP"}],"relations":[{"id":"R1","pred":"coref-xxx","subj":"C1","obj":"C2"},{"id":"R2","pred":"coref-part-whole","subj":"C3","obj":"C15"},{"id":"R3","pred":"coref-relat","subj":"C5","obj":"C4"},{"id":"R4","pred":"coref-ident","subj":"C44","obj":"C43"},{"id":"R5","pred":"coref-ident","subj":"C7","obj":"C6"},{"id":"R6","pred":"coref-ident","subj":"C45","obj":"C44"},{"id":"R7","pred":"coref-ident","subj":"C9","obj":"C8"},{"id":"R8","pred":"coref-ident","subj":"C11","obj":"C10"},{"id":"R9","pred":"coref-ident","subj":"C12","obj":"C3"},{"id":"R10","pred":"coref-part-whole","subj":"C13","obj":"C15"},{"id":"R11","pred":"coref-xxx","subj":"C14","obj":"C15"},{"id":"R12","pred":"coref-ident","subj":"C16","obj":"C17"},{"id":"R13","pred":"coref-relat","subj":"C19","obj":"C18"},{"id":"R14","pred":"coref-ident","subj":"C21","obj":"C20"},{"id":"R15","pred":"coref-ident","subj":"C22","obj":"C1"},{"id":"R16","pred":"coref-pron","subj":"C24","obj":"C23"},{"id":"R17","pred":"coref-ident","subj":"C25","obj":"C12"},{"id":"R18","pred":"coref-ident","subj":"C26","obj":"C25"},{"id":"R19","pred":"coref-ident","subj":"C27","obj":"C26"},{"id":"R20","pred":"coref-ident","subj":"C28","obj":"C21"},{"id":"R21","pred":"coref-ident","subj":"C30","obj":"C29"},{"id":"R22","pred":"coref-ident","subj":"C31","obj":"C27"},{"id":"R23","pred":"coref-ident","subj":"C32","obj":"C31"},{"id":"R24","pred":"coref-ident","subj":"C46","obj":"C45"},{"id":"R25","pred":"coref-ident","subj":"C33","obj":"C22"},{"id":"R26","pred":"coref-relat","subj":"C35","obj":"C34"},{"id":"R27","pred":"coref-ident","subj":"C36","obj":"C7"},{"id":"R28","pred":"coref-ident","subj":"C37","obj":"C32"},{"id":"R29","pred":"coref-ident","subj":"C38","obj":"C13"},{"id":"R30","pred":"coref-ident","subj":"C47","obj":"C46"},{"id":"R31","pred":"coref-ident","subj":"C39","obj":"C37"},{"id":"R32","pred":"coref-ident","subj":"C40","obj":"C4"},{"id":"R33","pred":"coref-ident","subj":"C41","obj":"C39"},{"id":"R34","pred":"coref-ident","subj":"C48","obj":"C47"},{"id":"R35","pred":"coref-part-whole","subj":"C42","obj":"C15"}],"text":"Receptors for interleukin (IL)-10 and IL-6-type cytokines use similar signaling mechanisms for inducing transcription through IL-6 response elements.\nThe cytoplasmic domain of the receptor for interleukin 10 (IL-10R) contains two box 3 sequence motifs that have been identified in the signal-transducing receptor subunits for IL-6-type cytokines and noted to be required for activating STAT3 and inducing transcription through IL-6-responsive elements. To determine whether the IL-10R has signaling functions similar to IL-6R in cells normally expressing these receptors, leukocytes of the B-, T-, and NK-cell lineages were treated with either cytokine. Both cytokines activated factors that bound to the sis-inducible element and included STAT1 and STAT3. The cell response to IL-10 characteristically differed from that to IL-2/IL-15, IL-4, and interferon gamma. The signaling capabilities of the IL-10R for activating specific STAT proteins and inducing gene transcription were defined by reconstitution of receptor functions in transfected tissue culture cells. COS-1 cells, co-expressing the human IL-10R and individual STAT proteins, confirmed a preference of the IL-10R for STAT3 and STAT1. Unlike many hematopoietin receptors, the IL-10R did not detectably activate STAT5. The IL-10R, together with reporter gene constructs containing different IL-6-responsive gene elements, reconstituted in hepatoma cells an induction of transcription by IL-10 that was comparable to that by IL-6. This regulation could not be appreciably modified by enhanced expression of STAT proteins. The similar actions of IL-10R and IL-6R on the induction of endogenous IL-6-responsive genes were demonstrated in hepatoma cells stably expressing the IL-10R. These receptor functions required the presence of the box 3 motifs, as shown by the analysis of the mouse IL-10R constructs containing progressively truncated cytoplasmic domains. The data demonstrate that the IL-10R, unlike other members of the interferon receptor family, is highly effective in recruiting the signaling pathways of IL-6-type cytokine receptors."}

    GENIAcorpus

    {"project":"GENIAcorpus","denotations":[{"id":"T1","span":{"begin":126,"end":148},"obj":"DNA_family_or_group"},{"id":"T2","span":{"begin":154,"end":172},"obj":"protein_domain_or_region"},{"id":"T3","span":{"begin":193,"end":207},"obj":"protein_molecule"},{"id":"T4","span":{"begin":209,"end":215},"obj":"protein_molecule"},{"id":"T5","span":{"begin":285,"end":321},"obj":"protein_subunit"},{"id":"T6","span":{"begin":326,"end":345},"obj":"protein_family_or_group"},{"id":"T7","span":{"begin":386,"end":391},"obj":"protein_molecule"},{"id":"T8","span":{"begin":427,"end":451},"obj":"DNA_family_or_group"},{"id":"T9","span":{"begin":478,"end":484},"obj":"protein_molecule"},{"id":"T10","span":{"begin":520,"end":525},"obj":"protein_molecule"},{"id":"T11","span":{"begin":572,"end":582},"obj":"cell_type"},{"id":"T12","span":{"begin":659,"end":668},"obj":"protein_family_or_group"},{"id":"T13","span":{"begin":705,"end":726},"obj":"DNA_family_or_group"},{"id":"T14","span":{"begin":740,"end":745},"obj":"protein_molecule"},{"id":"T15","span":{"begin":750,"end":755},"obj":"protein_molecule"},{"id":"T16","span":{"begin":778,"end":783},"obj":"protein_molecule"},{"id":"T17","span":{"begin":825,"end":835},"obj":"protein_molecule"},{"id":"T18","span":{"begin":837,"end":841},"obj":"protein_molecule"},{"id":"T19","span":{"begin":847,"end":863},"obj":"protein_molecule"},{"id":"T20","span":{"begin":899,"end":905},"obj":"protein_molecule"},{"id":"T21","span":{"begin":930,"end":943},"obj":"protein_family_or_group"},{"id":"T22","span":{"begin":1032,"end":1064},"obj":"cell_line"},{"id":"T23","span":{"begin":1066,"end":1077},"obj":"cell_line"},{"id":"T24","span":{"begin":1103,"end":1109},"obj":"protein_molecule"},{"id":"T25","span":{"begin":1125,"end":1138},"obj":"protein_family_or_group"},{"id":"T26","span":{"begin":1170,"end":1176},"obj":"protein_molecule"},{"id":"T27","span":{"begin":1181,"end":1186},"obj":"protein_molecule"},{"id":"T28","span":{"begin":1191,"end":1196},"obj":"protein_molecule"},{"id":"T29","span":{"begin":1210,"end":1233},"obj":"protein_family_or_group"},{"id":"T30","span":{"begin":1239,"end":1245},"obj":"protein_molecule"},{"id":"T31","span":{"begin":1274,"end":1279},"obj":"protein_molecule"},{"id":"T32","span":{"begin":1285,"end":1291},"obj":"protein_molecule"},{"id":"T33","span":{"begin":1353,"end":1382},"obj":"DNA_family_or_group"},{"id":"T34","span":{"begin":1401,"end":1415},"obj":"cell_type"},{"id":"T35","span":{"begin":1449,"end":1454},"obj":"protein_molecule"},{"id":"T36","span":{"begin":1486,"end":1490},"obj":"protein_molecule"},{"id":"T37","span":{"begin":1568,"end":1581},"obj":"protein_family_or_group"},{"id":"T38","span":{"begin":1606,"end":1612},"obj":"protein_molecule"},{"id":"T39","span":{"begin":1617,"end":1622},"obj":"protein_molecule"},{"id":"T40","span":{"begin":1654,"end":1658},"obj":"protein_molecule"},{"id":"T41","span":{"begin":1697,"end":1711},"obj":"cell_type"},{"id":"T42","span":{"begin":1734,"end":1740},"obj":"protein_molecule"},{"id":"T43","span":{"begin":1848,"end":1854},"obj":"protein_molecule"},{"id":"T44","span":{"begin":1877,"end":1920},"obj":"protein_domain_or_region"},{"id":"T45","span":{"begin":1952,"end":1958},"obj":"protein_molecule"},{"id":"T46","span":{"begin":2076,"end":2080},"obj":"protein_molecule"}],"text":"Receptors for interleukin (IL)-10 and IL-6-type cytokines use similar signaling mechanisms for inducing transcription through IL-6 response elements.\nThe cytoplasmic domain of the receptor for interleukin 10 (IL-10R) contains two box 3 sequence motifs that have been identified in the signal-transducing receptor subunits for IL-6-type cytokines and noted to be required for activating STAT3 and inducing transcription through IL-6-responsive elements. To determine whether the IL-10R has signaling functions similar to IL-6R in cells normally expressing these receptors, leukocytes of the B-, T-, and NK-cell lineages were treated with either cytokine. Both cytokines activated factors that bound to the sis-inducible element and included STAT1 and STAT3. The cell response to IL-10 characteristically differed from that to IL-2/IL-15, IL-4, and interferon gamma. The signaling capabilities of the IL-10R for activating specific STAT proteins and inducing gene transcription were defined by reconstitution of receptor functions in transfected tissue culture cells. COS-1 cells, co-expressing the human IL-10R and individual STAT proteins, confirmed a preference of the IL-10R for STAT3 and STAT1. Unlike many hematopoietin receptors, the IL-10R did not detectably activate STAT5. The IL-10R, together with reporter gene constructs containing different IL-6-responsive gene elements, reconstituted in hepatoma cells an induction of transcription by IL-10 that was comparable to that by IL-6. This regulation could not be appreciably modified by enhanced expression of STAT proteins. The similar actions of IL-10R and IL-6R on the induction of endogenous IL-6-responsive genes were demonstrated in hepatoma cells stably expressing the IL-10R. These receptor functions required the presence of the box 3 motifs, as shown by the analysis of the mouse IL-10R constructs containing progressively truncated cytoplasmic domains. The data demonstrate that the IL-10R, unlike other members of the interferon receptor family, is highly effective in recruiting the signaling pathways of IL-6-type cytokine receptors."}

    mondo_disease

    {"project":"mondo_disease","denotations":[{"id":"T1","span":{"begin":1401,"end":1409},"obj":"Disease"},{"id":"T2","span":{"begin":1697,"end":1705},"obj":"Disease"}],"attributes":[{"id":"A1","pred":"mondo_id","subj":"T1","obj":"http://purl.obolibrary.org/obo/MONDO_0007256"},{"id":"A2","pred":"mondo_id","subj":"T2","obj":"http://purl.obolibrary.org/obo/MONDO_0007256"}],"text":"Receptors for interleukin (IL)-10 and IL-6-type cytokines use similar signaling mechanisms for inducing transcription through IL-6 response elements.\nThe cytoplasmic domain of the receptor for interleukin 10 (IL-10R) contains two box 3 sequence motifs that have been identified in the signal-transducing receptor subunits for IL-6-type cytokines and noted to be required for activating STAT3 and inducing transcription through IL-6-responsive elements. To determine whether the IL-10R has signaling functions similar to IL-6R in cells normally expressing these receptors, leukocytes of the B-, T-, and NK-cell lineages were treated with either cytokine. Both cytokines activated factors that bound to the sis-inducible element and included STAT1 and STAT3. The cell response to IL-10 characteristically differed from that to IL-2/IL-15, IL-4, and interferon gamma. The signaling capabilities of the IL-10R for activating specific STAT proteins and inducing gene transcription were defined by reconstitution of receptor functions in transfected tissue culture cells. COS-1 cells, co-expressing the human IL-10R and individual STAT proteins, confirmed a preference of the IL-10R for STAT3 and STAT1. Unlike many hematopoietin receptors, the IL-10R did not detectably activate STAT5. The IL-10R, together with reporter gene constructs containing different IL-6-responsive gene elements, reconstituted in hepatoma cells an induction of transcription by IL-10 that was comparable to that by IL-6. This regulation could not be appreciably modified by enhanced expression of STAT proteins. The similar actions of IL-10R and IL-6R on the induction of endogenous IL-6-responsive genes were demonstrated in hepatoma cells stably expressing the IL-10R. These receptor functions required the presence of the box 3 motifs, as shown by the analysis of the mouse IL-10R constructs containing progressively truncated cytoplasmic domains. The data demonstrate that the IL-10R, unlike other members of the interferon receptor family, is highly effective in recruiting the signaling pathways of IL-6-type cytokine receptors."}

    NCBITAXON

    {"project":"NCBITAXON","denotations":[{"id":"T1","span":{"begin":1097,"end":1102},"obj":"OrganismTaxon"},{"id":"T2","span":{"begin":1842,"end":1847},"obj":"OrganismTaxon"}],"attributes":[{"id":"A1","pred":"db_id","subj":"T1","obj":"9606"},{"id":"A2","pred":"db_id","subj":"T2","obj":"10088"},{"id":"A3","pred":"db_id","subj":"T2","obj":"10090"}],"text":"Receptors for interleukin (IL)-10 and IL-6-type cytokines use similar signaling mechanisms for inducing transcription through IL-6 response elements.\nThe cytoplasmic domain of the receptor for interleukin 10 (IL-10R) contains two box 3 sequence motifs that have been identified in the signal-transducing receptor subunits for IL-6-type cytokines and noted to be required for activating STAT3 and inducing transcription through IL-6-responsive elements. To determine whether the IL-10R has signaling functions similar to IL-6R in cells normally expressing these receptors, leukocytes of the B-, T-, and NK-cell lineages were treated with either cytokine. Both cytokines activated factors that bound to the sis-inducible element and included STAT1 and STAT3. The cell response to IL-10 characteristically differed from that to IL-2/IL-15, IL-4, and interferon gamma. The signaling capabilities of the IL-10R for activating specific STAT proteins and inducing gene transcription were defined by reconstitution of receptor functions in transfected tissue culture cells. COS-1 cells, co-expressing the human IL-10R and individual STAT proteins, confirmed a preference of the IL-10R for STAT3 and STAT1. Unlike many hematopoietin receptors, the IL-10R did not detectably activate STAT5. The IL-10R, together with reporter gene constructs containing different IL-6-responsive gene elements, reconstituted in hepatoma cells an induction of transcription by IL-10 that was comparable to that by IL-6. This regulation could not be appreciably modified by enhanced expression of STAT proteins. The similar actions of IL-10R and IL-6R on the induction of endogenous IL-6-responsive genes were demonstrated in hepatoma cells stably expressing the IL-10R. These receptor functions required the presence of the box 3 motifs, as shown by the analysis of the mouse IL-10R constructs containing progressively truncated cytoplasmic domains. The data demonstrate that the IL-10R, unlike other members of the interferon receptor family, is highly effective in recruiting the signaling pathways of IL-6-type cytokine receptors."}

    Anatomy-UBERON

    {"project":"Anatomy-UBERON","denotations":[{"id":"T1","span":{"begin":154,"end":165},"obj":"Body_part"},{"id":"T2","span":{"begin":572,"end":582},"obj":"Body_part"},{"id":"T3","span":{"begin":1044,"end":1050},"obj":"Body_part"},{"id":"T4","span":{"begin":1901,"end":1912},"obj":"Body_part"}],"attributes":[{"id":"A1","pred":"uberon_id","subj":"T1","obj":"http://purl.obolibrary.org/obo/GO_0005737"},{"id":"A2","pred":"uberon_id","subj":"T2","obj":"http://purl.obolibrary.org/obo/CL_0000738"},{"id":"A3","pred":"uberon_id","subj":"T3","obj":"http://purl.obolibrary.org/obo/UBERON_0000479"},{"id":"A4","pred":"uberon_id","subj":"T4","obj":"http://purl.obolibrary.org/obo/GO_0005737"}],"text":"Receptors for interleukin (IL)-10 and IL-6-type cytokines use similar signaling mechanisms for inducing transcription through IL-6 response elements.\nThe cytoplasmic domain of the receptor for interleukin 10 (IL-10R) contains two box 3 sequence motifs that have been identified in the signal-transducing receptor subunits for IL-6-type cytokines and noted to be required for activating STAT3 and inducing transcription through IL-6-responsive elements. To determine whether the IL-10R has signaling functions similar to IL-6R in cells normally expressing these receptors, leukocytes of the B-, T-, and NK-cell lineages were treated with either cytokine. Both cytokines activated factors that bound to the sis-inducible element and included STAT1 and STAT3. The cell response to IL-10 characteristically differed from that to IL-2/IL-15, IL-4, and interferon gamma. The signaling capabilities of the IL-10R for activating specific STAT proteins and inducing gene transcription were defined by reconstitution of receptor functions in transfected tissue culture cells. COS-1 cells, co-expressing the human IL-10R and individual STAT proteins, confirmed a preference of the IL-10R for STAT3 and STAT1. Unlike many hematopoietin receptors, the IL-10R did not detectably activate STAT5. The IL-10R, together with reporter gene constructs containing different IL-6-responsive gene elements, reconstituted in hepatoma cells an induction of transcription by IL-10 that was comparable to that by IL-6. This regulation could not be appreciably modified by enhanced expression of STAT proteins. The similar actions of IL-10R and IL-6R on the induction of endogenous IL-6-responsive genes were demonstrated in hepatoma cells stably expressing the IL-10R. These receptor functions required the presence of the box 3 motifs, as shown by the analysis of the mouse IL-10R constructs containing progressively truncated cytoplasmic domains. The data demonstrate that the IL-10R, unlike other members of the interferon receptor family, is highly effective in recruiting the signaling pathways of IL-6-type cytokine receptors."}

    CL-cell

    {"project":"CL-cell","denotations":[{"id":"T1","span":{"begin":572,"end":582},"obj":"Cell"},{"id":"T2","span":{"begin":602,"end":609},"obj":"Cell"},{"id":"T3","span":{"begin":1051,"end":1064},"obj":"Cell"}],"attributes":[{"id":"A1","pred":"cl_id","subj":"T1","obj":"http://purl.obolibrary.org/obo/CL:0000738"},{"id":"A2","pred":"cl_id","subj":"T2","obj":"http://purl.obolibrary.org/obo/CL:0000623"},{"id":"A3","pred":"cl_id","subj":"T3","obj":"http://purl.obolibrary.org/obo/CL:0000010"}],"text":"Receptors for interleukin (IL)-10 and IL-6-type cytokines use similar signaling mechanisms for inducing transcription through IL-6 response elements.\nThe cytoplasmic domain of the receptor for interleukin 10 (IL-10R) contains two box 3 sequence motifs that have been identified in the signal-transducing receptor subunits for IL-6-type cytokines and noted to be required for activating STAT3 and inducing transcription through IL-6-responsive elements. To determine whether the IL-10R has signaling functions similar to IL-6R in cells normally expressing these receptors, leukocytes of the B-, T-, and NK-cell lineages were treated with either cytokine. Both cytokines activated factors that bound to the sis-inducible element and included STAT1 and STAT3. The cell response to IL-10 characteristically differed from that to IL-2/IL-15, IL-4, and interferon gamma. The signaling capabilities of the IL-10R for activating specific STAT proteins and inducing gene transcription were defined by reconstitution of receptor functions in transfected tissue culture cells. COS-1 cells, co-expressing the human IL-10R and individual STAT proteins, confirmed a preference of the IL-10R for STAT3 and STAT1. Unlike many hematopoietin receptors, the IL-10R did not detectably activate STAT5. The IL-10R, together with reporter gene constructs containing different IL-6-responsive gene elements, reconstituted in hepatoma cells an induction of transcription by IL-10 that was comparable to that by IL-6. This regulation could not be appreciably modified by enhanced expression of STAT proteins. The similar actions of IL-10R and IL-6R on the induction of endogenous IL-6-responsive genes were demonstrated in hepatoma cells stably expressing the IL-10R. These receptor functions required the presence of the box 3 motifs, as shown by the analysis of the mouse IL-10R constructs containing progressively truncated cytoplasmic domains. The data demonstrate that the IL-10R, unlike other members of the interferon receptor family, is highly effective in recruiting the signaling pathways of IL-6-type cytokine receptors."}