1999
DOI: 10.1046/j.1523-1747.1999.00488.x
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Clustering of Activating Mutations in c-KIT’s Juxtamembrane Coding Region in Canine Mast Cell Neoplasms

Abstract: The proto-oncogene c-KIT encodes a growth factor receptor, KIT, with ligand-dependent tyrosine kinase activity that is expressed by several cell types including mast cells. c-KIT juxtamembrane coding region mutations causing constitutive activation of KIT are capable of transforming cell lines and have been identified in a human mast cell line and in situ in human gastrointestinal stromal tumors, but have not been demonstrated in situ in neoplastic mast cells from any species. To determine whether c-KIT juxtam… Show more

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Cited by 140 publications
(189 citation statements)
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“…3A and B). Discussion L576P is a rare mutation located in the JMD of KIT described in GISTs (6-10), melanomas (11), and canine GISTs and mastocytomas (12,13). We observed three L576P mutations among 332 profiled GISTs, of which we report upon two cases here (the third being enrolled into the 62024 EORTC trial).…”
Section: Molecular Dynamic Simulationsmentioning
confidence: 66%
See 1 more Smart Citation
“…3A and B). Discussion L576P is a rare mutation located in the JMD of KIT described in GISTs (6-10), melanomas (11), and canine GISTs and mastocytomas (12,13). We observed three L576P mutations among 332 profiled GISTs, of which we report upon two cases here (the third being enrolled into the 62024 EORTC trial).…”
Section: Molecular Dynamic Simulationsmentioning
confidence: 66%
“…In particular, the COS-7 cells expressing the L576P/KIT c-DNA revealed spontaneous KIT phosphorylation (13), and in vitro sensitivity tests highlighted the need of a tenfold higher dose of imatinib to switch off activated L576P/KIT with respect to V599D/KIT (11).…”
Section: Molecular Dynamic Simulationsmentioning
confidence: 99%
“…23 Mastocytosis also frequently expresses mutated c-kit, which confers constitutive activation. However, this mutation occurs in codon 816, resulting in residue substitutions in the activation loop, 24 and is insensitive to imatinib in vitro. 25 Despite the frequent expression of c-kit in AML and MDS patients, mutations are reported rarely.…”
Section: Discussionmentioning
confidence: 99%
“…61 Internal tandem duplications are not unique to FLT3, as similar mutations have been reported to occur in the related receptor KIT (in canine mastocytomas) and in other (nonhuman) genes. 81,82 Partial tandem duplications of the mixed lineage leukemia (MLL) gene have been found in both AML and ALL, sometimes in conjunction with an FLT3/ITD mutation. [83][84][85][86] The cause of these duplication events has been speculated upon, but remains unknown.…”
Section: Flt3/itd Mutationsmentioning
confidence: 99%
“…[97][98][99] An activating tandem duplication within the juxtamembrane region of KIT was identified in a canine mastocytoma, and a variety of activating point mutations within this region of the receptor have been found in human gastrointestinal stromal tumors. 81,100 An activating juxtamembrane point mutation was also identified in the PDGF receptor. 97 …”
Section: Flt3 In Leukemia M Levis and D Smallmentioning
confidence: 99%