Multiple Roles for the Receptor Tyrosine Kinase Axl in Tumor Formation

Holland, Sacha J.; Powell, Mark; Franci, Christian; Chan, Emily; Friera, Annabelle M.; Atchison, Robert E.; McLaughlin, John; Swift, Susan; Pali, Erlina S.; Yam, George; Wong, Stephen T.C.; Lasaga, Joe; Shen, Mary; Yu, Shichao; Xu, Weiduan; Hitoshi, Yasumichi; Bogenberger, Jakob; Nör, Jacques E.; Payan, Donald G.; Lorens, James B.

doi:10.1158/0008-5472.can-05-0993

Cited by 172 publications

(180 citation statements)

References 51 publications

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“…AXL is characterized by a unique extracellular composition consisting of immunoglobulin-like and fibronectin-type III-like domains, which are also found in adhesion molecules of the cadherin and immunoglobulin superfamily, therefore suggesting that AXL might regulate cell adhesion (Burchert et al, 1998). Other evidence is consistent with roles of AXL in tumor cell invasion, metastasis and survival (Jacob et al, 1999;Holland et al, 2005;Mahadevan et al, 2007).…”

Section: Introductionmentioning

confidence: 72%

AXL regulates mesothelioma proliferation and invasiveness

et al. 2010

Oncogene

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Mesothelioma is an asbestos-associated and notoriously chemotherapy-resistant neoplasm. Activation of the receptor tyrosine kinases (RTKs), epidermal growth factor receptor and MET, has been described in subsets of mesothelioma, suggesting that TKs might represent therapeutic targets in this highly lethal disease. We employed proteomic screening by phosphotyrosine immunoaffinity purification and tandem mass spectrometry to characterize RTK activation in mesothelioma cell lines. These assays demonstrated expression and activation of the AXL protein, which is an RTK with known oncogenic properties in non-mesothelial cancer types. AXL was expressed and activated strongly in 8 of 9 mesothelioma cell lines and 6 of 12 mesothelioma biopsies, including each of 12 mesotheliomas with spindle-cell histology. Somatic AXL mutations were not found, but all mesotheliomas expressed an alternatively spliced AXL transcript with in-frame deletion of exon 10, and six of seven mesothelioma cell lines expressed the AXL ligand, growth arrest-specific 6 (GAS6). GAS6 expression appeared to be functionally relevant, as indicated by modulation of AXL tyrosine phosphorylation by knockdown of endogeneous GAS6, and by administration of exogenous GAS6. AXL silencing by lentivirus-mediated short hairpin RNA suppressed mesothelioma migration and cellular proliferation due to G1 arrest. The AXL inhibitor DP-3975 inhibited cell migration and proliferation in mesotheliomas with strong AXL activation. DP-3975 response in these tumors was characterized by inhibition of PI3-K/AKT/mTOR and RAF/MAPK signaling. AXL inhibition suppressed mesothelioma anchorage-independent growth, with reduction in colony numbers and size. These studies suggest that AXL inhibitors warrant clinical evaluation in mesothelioma.

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Section: Introductionmentioning

confidence: 72%

AXL regulates mesothelioma proliferation and invasiveness

et al. 2010

Oncogene

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“…Axl is expressed on endothelial cells and enhances vascular endothelial growth factor (VEGF)-induced endothelial tubule formation (Holland et al, 2005;Li et al, 2009); we tested whether anti-Axl mAb could enhance the antitumor growth property of anti-VEGF (Liang et al, 2006). Anti-VEGF antibody alone and YW327.6S2 alone had similar effects on A549 tumor growth (Figure 2a).…”

Section: Generation Of a Phage Derived Mab That Blocks Axl's Functionmentioning

confidence: 99%

An anti-Axl monoclonal antibody attenuates xenograft tumor growth and enhances the effect of multiple anticancer therapies

Stawicki³

et al. 2010

Oncogene

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“…MP470 had an IC 50 of 2 mM in the GIST-R cell line ( Figure 3a) indicating that MP470 acts as an AXL kinase inhibitor. We utilized the MDA-MB-231 breast cancer cell line (as an independent positive control) that overexpresses an active tyrosine phosphorylated AXL (Holland et al, 2005) to evaluate the efficacy of MP470 to inhibit its phosphorylation. Western blotting analysis shows inhibition of tyrosine phosphorylation of AXL by MP470 at 1.0 mM ( Figure 3b) and is in the range observed for the GIST-R cells ( Figure 2a).…”

Section: Imatinib Resistance In Gastrointestinal Stromal Tumors D Mahmentioning

confidence: 99%

A novel tyrosine kinase switch is a mechanism of imatinib resistance in gastrointestinal stromal tumors

et al. 2007

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KIT or a-platelet-derived growth factor receptor (a-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 IMsensitive 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 growtharrest-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.

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Multiple Roles for the Receptor Tyrosine Kinase Axl in Tumor Formation

Cited by 172 publications

References 51 publications

AXL regulates mesothelioma proliferation and invasiveness

AXL regulates mesothelioma proliferation and invasiveness

An anti-Axl monoclonal antibody attenuates xenograft tumor growth and enhances the effect of multiple anticancer therapies

A novel tyrosine kinase switch is a mechanism of imatinib resistance in gastrointestinal stromal tumors

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