Home > Publications database > Cooperation of BRAF(F595L) and mutant HRAS in histiocytic sarcoma provides new insights into oncogenic BRAF signaling. > print

001     128945
005     20240228143359.0
024 7 _ |a 10.1038/leu.2015.319
|2 doi
024 7 _ |a pmid:26582644
|2 pmid
024 7 _ |a 0887-6924
|2 ISSN
024 7 _ |a 1476-5551
|2 ISSN
024 7 _ |a altmetric:4809662
|2 altmetric
037 _ _ |a DKFZ-2017-04957
041 _ _ |a eng
082 _ _ |a 610
100 1 _ |a Kordes, M.
|b 0
245 _ _ |a Cooperation of BRAF(F595L) and mutant HRAS in histiocytic sarcoma provides new insights into oncogenic BRAF signaling.
260 _ _ |a Basingstoke
|c 2016
|b Nature Publ. Group
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 1524483381_2937
|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 Activating BRAF mutations, in particular V600E/K, drive many cancers and are considered mutually exclusive with mutant RAS, whereas inactivating BRAF mutations in the D(594)F(595)G(596) motif cooperate with RAS via paradoxical MEK/ERK activation. Due to the increasing use of comprehensive tumor genomic profiling, many non-V600 BRAF mutations are being detected whose functional consequences and therapeutic actionability are often unknown. We investigated an atypical BRAF mutation, F595L, which was identified along with mutant HRAS in histiocytic sarcoma and also occurs in epithelial cancers, melanoma and neuroblastoma, and determined its interaction with mutant RAS. Unlike other DFG motif mutants, BRAF(F595L) is a gain-of-function variant with intermediate activity that does not act paradoxically, but nevertheless cooperates with mutant RAS to promote oncogenic signaling, which is efficiently blocked by pan-RAF and MEK inhibitors. Mutation data from patients and cell lines show that BRAF(F595L), as well as other intermediate-activity BRAF mutations, frequently coincide with mutant RAS in various cancers. These data define a distinct class of activating BRAF mutations, extend the spectrum of patients with systemic histiocytoses and other malignancies who are candidates for therapeutic blockade of the RAF-MEK-ERK pathway and underscore the value of comprehensive genomic testing for uncovering the vulnerabilities of individual tumors.
536 _ _ |a 317 - Translational cancer research (POF3-317)
|0 G:(DE-HGF)POF3-317
|c POF3-317
|f POF III
|x 0
588 _ _ |a Dataset connected to CrossRef, PubMed,
650 _ 7 |a Biomarkers, Tumor
|2 NLM Chemicals
650 _ 7 |a BRAF protein, human
|0 EC 2.7.11.1
|2 NLM Chemicals
650 _ 7 |a Proto-Oncogene Proteins B-raf
|0 EC 2.7.11.1
|2 NLM Chemicals
650 _ 7 |a HRAS protein, human
|0 EC 3.6.5.2
|2 NLM Chemicals
650 _ 7 |a Proto-Oncogene Proteins p21(ras)
|0 EC 3.6.5.2
|2 NLM Chemicals
700 1 _ |a Röring, M.
|b 1
700 1 _ |a Heining, C.
|0 P:(DE-He78)1464357f7ec5faf677a390a414e50c88
|b 2
|u dkfz
700 1 _ |a Braun, S.
|b 3
700 1 _ |a Hutter, B.
|0 P:(DE-He78)135e8c8d1dd1b66b8127c3d1e3a9b6a0
|b 4
|u dkfz
700 1 _ |a Richter, D.
|0 P:(DE-He78)29306fd3ae9f1a9839ed888ebc5c8074
|b 5
|u dkfz
700 1 _ |a Geörg, C.
|0 P:(DE-He78)3f888debb126ff36634df058ccaaf2b4
|b 6
|u dkfz
700 1 _ |a Scholl, C.
|0 P:(DE-He78)2c1a21d1cf5fdc9e297512c9d1354250
|b 7
|u dkfz
700 1 _ |a Gröschel, S.
|0 P:(DE-He78)5120a331b1c28045c8ca6a8b1c73c95f
|b 8
|u dkfz
700 1 _ |a Roth, W.
|0 P:(DE-He78)6c54d919bb3371b6d7f277e2c6262a4a
|b 9
|u dkfz
700 1 _ |a Rosenwald, A.
|b 10
700 1 _ |a Geissinger, E.
|b 11
700 1 _ |a von Kalle, C.
|0 P:(DE-He78)5bacb661d5d7c0220d8f996d980ad8de
|b 12
|u dkfz
700 1 _ |a Jäger, D.
|0 P:(DE-He78)ed0321409c9cde20b380ae663dbcefd1
|b 13
|u dkfz
700 1 _ |a Brors, B.
|0 P:(DE-He78)fc949170377b58098e46141d95c72661
|b 14
|u dkfz
700 1 _ |a Weichert, W.
|b 15
700 1 _ |a Grüllich, C.
|b 16
700 1 _ |a Glimm, H.
|0 P:(DE-He78)157277fe62f07df1732f9d126a51d1b9
|b 17
|u dkfz
700 1 _ |a Brummer, T.
|b 18
700 1 _ |a Fröhling, Stefan
|0 P:(DE-He78)f0144d171d26dbedb67c9db1df35629d
|b 19
|e Last author
|u dkfz
773 _ _ |a 10.1038/leu.2015.319
|g Vol. 30, no. 4, p. 937 - 946
|0 PERI:(DE-600)2008023-2
|n 4
|p 937 - 946
|t Leukemia
|v 30
|y 2016
|x 1476-5551
909 C O |o oai:inrepo02.dkfz.de:128945
|p VDB
910 1 _ |a Deutsches Krebsforschungszentrum
|0 I:(DE-588b)2036810-0
|k DKFZ
|b 2
|6 P:(DE-He78)1464357f7ec5faf677a390a414e50c88
910 1 _ |a Deutsches Krebsforschungszentrum
|0 I:(DE-588b)2036810-0
|k DKFZ
|b 4
|6 P:(DE-He78)135e8c8d1dd1b66b8127c3d1e3a9b6a0
910 1 _ |a Deutsches Krebsforschungszentrum
|0 I:(DE-588b)2036810-0
|k DKFZ
|b 5
|6 P:(DE-He78)29306fd3ae9f1a9839ed888ebc5c8074
910 1 _ |a Deutsches Krebsforschungszentrum
|0 I:(DE-588b)2036810-0
|k DKFZ
|b 6
|6 P:(DE-He78)3f888debb126ff36634df058ccaaf2b4
910 1 _ |a Deutsches Krebsforschungszentrum
|0 I:(DE-588b)2036810-0
|k DKFZ
|b 7
|6 P:(DE-He78)2c1a21d1cf5fdc9e297512c9d1354250
910 1 _ |a Deutsches Krebsforschungszentrum
|0 I:(DE-588b)2036810-0
|k DKFZ
|b 8
|6 P:(DE-He78)5120a331b1c28045c8ca6a8b1c73c95f
910 1 _ |a Deutsches Krebsforschungszentrum
|0 I:(DE-588b)2036810-0
|k DKFZ
|b 9
|6 P:(DE-He78)6c54d919bb3371b6d7f277e2c6262a4a
910 1 _ |a Deutsches Krebsforschungszentrum
|0 I:(DE-588b)2036810-0
|k DKFZ
|b 12
|6 P:(DE-He78)5bacb661d5d7c0220d8f996d980ad8de
910 1 _ |a Deutsches Krebsforschungszentrum
|0 I:(DE-588b)2036810-0
|k DKFZ
|b 13
|6 P:(DE-He78)ed0321409c9cde20b380ae663dbcefd1
910 1 _ |a Deutsches Krebsforschungszentrum
|0 I:(DE-588b)2036810-0
|k DKFZ
|b 14
|6 P:(DE-He78)fc949170377b58098e46141d95c72661
910 1 _ |a Deutsches Krebsforschungszentrum
|0 I:(DE-588b)2036810-0
|k DKFZ
|b 17
|6 P:(DE-He78)157277fe62f07df1732f9d126a51d1b9
910 1 _ |a Deutsches Krebsforschungszentrum
|0 I:(DE-588b)2036810-0
|k DKFZ
|b 19
|6 P:(DE-He78)f0144d171d26dbedb67c9db1df35629d
913 1 _ |a DE-HGF
|l Krebsforschung
|1 G:(DE-HGF)POF3-310
|0 G:(DE-HGF)POF3-317
|2 G:(DE-HGF)POF3-300
|v Translational cancer research
|x 0
|4 G:(DE-HGF)POF
|3 G:(DE-HGF)POF3
|b Gesundheit
914 1 _ |y 2016
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 JCR
|0 StatID:(DE-HGF)0100
|2 StatID
|b LEUKEMIA : 2015
915 _ _ |a DBCoverage
|0 StatID:(DE-HGF)0200
|2 StatID
|b SCOPUS
915 _ _ |a DBCoverage
|0 StatID:(DE-HGF)0600
|2 StatID
|b Ebsco Academic Search
915 _ _ |a Peer Review
|0 StatID:(DE-HGF)0030
|2 StatID
|b ASC
915 _ _ |a DBCoverage
|0 StatID:(DE-HGF)0199
|2 StatID
|b Thomson Reuters Master Journal List
915 _ _ |a WoS
|0 StatID:(DE-HGF)0110
|2 StatID
|b Science Citation Index
915 _ _ |a DBCoverage
|0 StatID:(DE-HGF)0150
|2 StatID
|b Web of Science Core Collection
915 _ _ |a WoS
|0 StatID:(DE-HGF)0111
|2 StatID
|b Science Citation Index Expanded
915 _ _ |a DBCoverage
|0 StatID:(DE-HGF)1030
|2 StatID
|b Current Contents - Life Sciences
915 _ _ |a DBCoverage
|0 StatID:(DE-HGF)1050
|2 StatID
|b BIOSIS Previews
915 _ _ |a IF >= 10
|0 StatID:(DE-HGF)9910
|2 StatID
|b LEUKEMIA : 2015
920 1 _ |0 I:(DE-He78)G100-20160331
|k G100
|l Translationale Onkologie
|x 0
920 1 _ |0 I:(DE-He78)G200-20160331
|k G200
|l Angewandte Bioinformatik
|x 1
920 1 _ |0 I:(DE-He78)G102-20160331
|k G102
|l Angewandte Funktionelle Genomik
|x 2
920 1 _ |0 I:(DE-He78)G010-20160331
|k G010
|l Geschäftsstelle
|x 3
920 1 _ |0 I:(DE-He78)G150-20160331
|k G150
|l Molekulare Tumorpathologie
|x 4
920 1 _ |0 I:(DE-He78)L101-20160331
|k L101
|l DKTK Heidelberg
|x 5
920 1 _ |0 I:(DE-He78)L601-20160331
|k L601
|l DKTK Freiburg
|x 6
920 1 _ |0 I:(DE-He78)D120-20160331
|k D120
|l Angewandte Tumor-Immunität
|x 7
920 1 _ |0 I:(DE-He78)G240-20160331
|k G240
|l Molekulare Leukämogenese
|x 8
980 _ _ |a journal
980 _ _ |a VDB
980 _ _ |a I:(DE-He78)G100-20160331
980 _ _ |a I:(DE-He78)G200-20160331
980 _ _ |a I:(DE-He78)G102-20160331
980 _ _ |a I:(DE-He78)G010-20160331
980 _ _ |a I:(DE-He78)G150-20160331
980 _ _ |a I:(DE-He78)L101-20160331
980 _ _ |a I:(DE-He78)L601-20160331
980 _ _ |a I:(DE-He78)D120-20160331
980 _ _ |a I:(DE-He78)G240-20160331
980 _ _ |a UNRESTRICTED

LibraryCollectionCLSMajorCLSMinorLanguageAuthor
Marc 21