Activated gp130 signaling selectively targets B cell differentiation to induce mature lymphoma and plasmacytoma.

Scherger, Anna K; Al-Maarri, Mona; Gonzalez-Menendez, Irene; Schick, Markus; Pechloff, Konstanze; Steiger, Katja; Sander, Sandrine; Keller, Ulrich; Thaler, Markus; Rose-John, Stefan; Maurer, Hans Carlo; Quintanilla-Martinez, Leticia; Maurer, Sabine; Ruland, Jürgen; Martella, Manuela; Öllinger, Rupert; Wunderlich, Frank T; Rad, Roland

doi:10.1172/jci.insight.128435

Items
Marc 21

001			144514
005			20240229112627.0
024	7	_	\|a 10.1172/jci.insight.128435 \|2 doi
024	7	_	\|a pmid:31391340 \|2 pmid
024	7	_	\|a altmetric:65259919 \|2 altmetric
037	_	_	\|a DKFZ-2019-01962
041	_	_	\|a eng
082	_	_	\|a 610
100	1	_	\|a Scherger, Anna K \|b 0
245	_	_	\|a Activated gp130 signaling selectively targets B cell differentiation to induce mature lymphoma and plasmacytoma.
260	_	_	\|a Ann Arbor, Michigan \|c 2019 \|b JCI Insight
336	7	_	\|a article \|2 DRIVER
336	7	_	\|a Output Types/Journal article \|2 DataCite
336	7	_	\|a Journal Article \|b journal \|m journal \|0 PUB:(DE-HGF)16 \|s 1681807065_19398 \|2 PUB:(DE-HGF)
336	7	_	\|a ARTICLE \|2 BibTeX
336	7	_	\|a JOURNAL_ARTICLE \|2 ORCID
336	7	_	\|a Journal Article \|0 0 \|2 EndNote
520	_	_	\|a Aberrant activity of the glycoprotein 130 130/JAK/STAT3 (gp130/JAK/STAT3) signaling axis is a recurrent event in inflammation and cancer. In particular, it is associated with a wide range of hematological malignancies, including multiple myeloma and leukemia. Novel targeted therapies have only been successful for some subtypes of these malignancies, underlining the need for developing robust mouse models to better dissect the role of this pathway in specific tumorigenic processes. Here, we investigated the role of selective gp130/JAK/STAT3 activation by generating a conditional mouse model. This model targeted constitutively active, cell-autonomous gp130 activity to B cells, as well as to the entire hematopoietic system. We found that regardless of the timing of activation in B cells, constitutively active gp130 signaling resulted in the formation specifically of mature B cell lymphomas and plasma cell disorders with full penetrance, only with different latencies, where infiltrating CD138+ cells were a dominant feature in every tumor. Furthermore, constitutively active gp130 signaling in all adult hematopoietic cells also led to the development specifically of largely mature, aggressive B cell cancers, again with a high penetrance of CD138+ tumors. Importantly, gp130 activity abrogated the differentiation block induced by a B cell-targeted Myc transgene and resulted in a complete penetrance of the gp130-associated, CD138+, mature B cell lymphoma phenotype. Thus, gp130 signaling selectively provides a strong growth and differentiation advantage for mature B cells and directs lymphomagenesis specifically toward terminally differentiated B cell cancers.
536	_	_	\|a 314 - Tumor immunology (POF3-314) \|0 G:(DE-HGF)POF3-314 \|c POF3-314 \|f POF III \|x 0
588	_	_	\|a Dataset connected to CrossRef, PubMed,
700	1	_	\|a Al-Maarri, Mona \|b 1
700	1	_	\|a Maurer, Hans Carlo \|b 2
700	1	_	\|a Schick, Markus \|b 3
700	1	_	\|a Maurer, Sabine \|b 4
700	1	_	\|a Öllinger, Rupert \|b 5
700	1	_	\|a Gonzalez-Menendez, Irene \|b 6
700	1	_	\|a Martella, Manuela \|b 7
700	1	_	\|a Thaler, Markus \|b 8
700	1	_	\|a Pechloff, Konstanze \|0 P:(DE-He78)1357588a5c7b2c3f249da63f694a0cdf \|b 9
700	1	_	\|a Steiger, Katja \|0 P:(DE-HGF)0 \|b 10
700	1	_	\|a Sander, Sandrine \|0 P:(DE-He78)3c4e3363a68498c72ad042b849e11f3a \|b 11
700	1	_	\|a Ruland, Jürgen \|0 P:(DE-HGF)0 \|b 12
700	1	_	\|a Rad, Roland \|0 P:(DE-He78)340f7c2dcaedeae68e4a62c281c7350b \|b 13
700	1	_	\|a Quintanilla-Martinez, Leticia \|b 14
700	1	_	\|a Wunderlich, Frank T \|b 15
700	1	_	\|a Rose-John, Stefan \|b 16
700	1	_	\|a Keller, Ulrich \|0 P:(DE-HGF)0 \|b 17
773	_	_	\|a 10.1172/jci.insight.128435 \|g Vol. 4, no. 15, p. e128435 \|0 PERI:(DE-600)2874757-4 \|n 15 \|p e128435 \|t JCI insight \|v 4 \|y 2019 \|x 2379-3708
909	C	O	\|p VDB \|o oai:inrepo02.dkfz.de:144514
910	1	_	\|a Deutsches Krebsforschungszentrum \|0 I:(DE-588b)2036810-0 \|k DKFZ \|b 9 \|6 P:(DE-He78)1357588a5c7b2c3f249da63f694a0cdf
910	1	_	\|a Deutsches Krebsforschungszentrum \|0 I:(DE-588b)2036810-0 \|k DKFZ \|b 10 \|6 P:(DE-HGF)0
910	1	_	\|a Deutsches Krebsforschungszentrum \|0 I:(DE-588b)2036810-0 \|k DKFZ \|b 11 \|6 P:(DE-He78)3c4e3363a68498c72ad042b849e11f3a
910	1	_	\|a Deutsches Krebsforschungszentrum \|0 I:(DE-588b)2036810-0 \|k DKFZ \|b 12 \|6 P:(DE-HGF)0
910	1	_	\|a Deutsches Krebsforschungszentrum \|0 I:(DE-588b)2036810-0 \|k DKFZ \|b 13 \|6 P:(DE-He78)340f7c2dcaedeae68e4a62c281c7350b
910	1	_	\|a Deutsches Krebsforschungszentrum \|0 I:(DE-588b)2036810-0 \|k DKFZ \|b 17 \|6 P:(DE-HGF)0
913	1	_	\|a DE-HGF \|b Gesundheit \|l Krebsforschung \|1 G:(DE-HGF)POF3-310 \|0 G:(DE-HGF)POF3-314 \|3 G:(DE-HGF)POF3 \|2 G:(DE-HGF)POF3-300 \|4 G:(DE-HGF)POF \|v Tumor immunology \|x 0
914	1	_	\|y 2019
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)0300 \|2 StatID \|b Medline
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)0310 \|2 StatID \|b NCBI Molecular Biology Database
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)0320 \|2 StatID \|b PubMed Central
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)0199 \|2 StatID \|b Clarivate Analytics Master Journal List
915	_	_	\|a WoS \|0 StatID:(DE-HGF)0112 \|2 StatID \|b Emerging Sources Citation Index
915	_	_	\|a DBCoverage \|0 StatID:(DE-HGF)0150 \|2 StatID \|b Web of Science Core Collection
920	1	_	\|0 I:(DE-He78)D180-20160331 \|k D180 \|l NWG Erworbene Immunität und Lymphome \|x 0
920	1	_	\|0 I:(DE-He78)L701-20160331 \|k L701 \|l DKTK München \|x 1
980	_	_	\|a journal
980	_	_	\|a VDB
980	_	_	\|a I:(DE-He78)D180-20160331
980	_	_	\|a I:(DE-He78)L701-20160331
980	_	_	\|a UNRESTRICTED

Library	Collection	CLSMajor	CLSMinor	Language	Author

Marc 21

guest :: login DKFZ
		Search		Submit		Personalize Your alerts Your baskets Your searches		Help