Standard name |
MAHADEVAN_GIST_MORPHOLOGICAL_SWITCH |
Systematic name |
M6900 |
Brief description |
Genes up-regulated in the GIST (gastrointestinal stromal tumor) cell line resistant to imatinib [PubChem=5291] that may correlate with the morphological switch in these cells. |
Full description or abstract |
KIT or alpha-platelet-derived growth factor receptor (alpha-PDGFR) activating mutations are the pathogenic mechanisms that characterize gastrointestinal stromal tumors (GIST). Despite excellent responses to imatinib mesylate (IM), patients are relapsing. We developed an IM-resistant GIST cell line (GIST-R) from the IM-sensitive GIST882 cell line (GIST-S) by growing these cells in IM. Gene expression profiling (GEP) of GIST-S, GIST-R cells and two IM resistant GIST patients demonstrated that KIT is downregulated implying a major role in IM resistance. Instead, GIST-R cells have acquired IM resistance by overexpressing the oncogenic receptor tyrosine kinase - AXL - in a 'kinase switch'. Further, the two IM resistant GIST patients express AXL and not c-Kit, seen by immunohistochemistry (IHC). Real time reverse transcriptase-polymerase chain reaction and Western blotting of the GIST-S and GIST-R cells confirmed the switch from Kit to AXL. In GIST-R, AXL is tyrosine phosphorylated and its ligand growth-arrest-specific gene 6 is overexpressed implying autocrine activation. The kinase switch is associated with a morphological change from spindle to epithelioid. Molecular modeling of the kinase domain of mutant c-Kit (V654A) and AXL showed no binding to IM but efficient binding to MP470, a novel c-Kit/AXL kinase inhibitor. MP470 synergizes with docetaxel (taxotere) and is cytotoxic to GIST cells. |
Collection |
C2: Curated CGP: Chemical and Genetic Perturbations |
Source publication |
Pubmed 17325667 Authors: Mahadevan D,Cooke L,Riley C,Swart R,Simons B,Della Croce K,Wisner L,Iorio M,Shakalya K,Garewal H,Nagle R,Bearss D |
Exact source |
Table 2 |
Related gene sets |
(show 3 additional gene sets from the source publication)
(show 19 gene sets from the same authors)
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External links |
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Source species |
Homo sapiens |
Contributed by |
Arthur Liberzon (MSigDB Team) |
Source platform or identifier namespace |
HUMAN_GENE_SYMBOL |
Dataset references |
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NCI-60 cell lines (National Cancer Institute)
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Human tissue compendium (Novartis)
Global Cancer Map (Broad Institute)
NCI-60 cell lines (National Cancer Institute)
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these 15 genes
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15 genes by gene family
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Show members |
(show 15 source identifiers mapped to 15 genes)
Source Id |
NCBI (Entrez) Gene Id |
Gene Symbol |
Gene Description |
CDH13 |
1012 |
CDH13 |
cadherin 13 [Source:HGNC Symbol;Acc:HGNC:1753] |
CDH6 |
1004 |
CDH6 |
cadherin 6 [Source:HGNC Symbol;Acc:HGNC:1765] |
CTGF |
1490 |
CCN2 |
cellular communication network factor 2 [Sourc... |
ELMO1 |
9844 |
ELMO1 |
engulfment and cell motility 1 [Source:HGNC Sy... |
FSCN1 |
6624 |
FSCN1 |
fascin actin-bundling protein 1 [Source:HGNC S... |
ITGA3 |
3675 |
ITGA3 |
integrin subunit alpha 3 [Source:HGNC Symbol;A... |
MMP2 |
4313 |
MMP2 |
matrix metallopeptidase 2 [Source:HGNC Symbol;... |
MMP3 |
4314 |
MMP3 |
matrix metallopeptidase 3 [Source:HGNC Symbol;... |
MYO10 |
4651 |
MYO10 |
myosin X [Source:HGNC Symbol;Acc:HGNC:7593] |
NEDD9 |
4739 |
NEDD9 |
neural precursor cell expressed, developmental... |
PDLIM1 |
9124 |
PDLIM1 |
PDZ and LIM domain 1 [Source:HGNC Symbol;Acc:H... |
SPOCK |
6695 |
SPOCK1 |
SPARC (osteonectin), cwcv and kazal like domai... |
SPP1 |
6696 |
SPP1 |
secreted phosphoprotein 1 [Source:HGNC Symbol;... |
TFPI2 |
7980 |
TFPI2 |
tissue factor pathway inhibitor 2 [Source:HGNC... |
TPM2 |
7169 |
TPM2 |
tropomyosin 2 [Source:HGNC Symbol;Acc:HGNC:12011] |
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Version history |
3.0: First introduced
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