Evaluating Melanoma Drug Response and Therapeutic Escape with Quantitative Proteomics

Rebecca, Vito W.; Wood, Elizabeth R.; Fedorenko, Inna V.; Paraiso, Kim H.T.; Haarberg, H. Eirik; Chen, Yi; Xiang, Yun; Sarnaik, Amod A.; Gibney, Geoffrey T.; Sondak, Vernon K.; Koomen, John M.; Smalley, Keiran S.M.

doi:10.1074/mcp.m113.037424

Cited by 53 publications

(44 citation statements)

References 48 publications

(49 reference statements)

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“…Our data adds to this and suggest that amuvatinib may be of utility in some NRAS -mutant melanomas, particularly those that are dependent upon the targets of this drug. The emerging evidence suggests that NRAS -mutant melanomas are more diverse than BRAF -mutant melanoma, potentially requiring the development of highly personalized therapeutic strategies on a patient-by-patient basis (20). Enhanced genetic profiling integrated with quantitative proteomic profiling is likely to play a key role in future therapy selection that allows durable responses to be achieved.…”

Section: Resultsmentioning

confidence: 99%

Amuvatinib has cytotoxic effects against NRAS-mutant melanoma but not BRAF-mutant melanoma

Fedorenko¹,

Fang²,

Koomen³

et al. 2014

Melanoma Research

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Effective targeted therapy strategies are still lacking for the 15–20% of melanoma patients whose melanomas are driven by oncogenic NRAS. We here report on the NRAS-specific behavior of amuvatinib, a kinase inhibitor with activity against c-KIT, Axl, PDGFRα and Rad51. An analysis of BRAF- and NRAS-mutant melanoma cell lines showed the NRAS-mutant cohort to be enriched for targets of amuvatinib, including Axl, c-KIT and the Axl ligand Gas6. Increasing concentrations of amuvatinib selectively inhibited the growth of NRAS- but not BRAF-mutant melanoma cell lines, an effect associated with induction of S- and G2/M-phase cell cycle arrest and induction of apoptosis. Mechanistically, amuvatinib was noted to either inhibit Axl, AKT and MAPK signaling or Axl and AKT signaling and to induce a DNA damage response. In 3D cell culture experiments, amuvatinib was cytotoxic against NRAS-mutant melanoma cell lines. Thus we show for the first time that amuvatinib has pro-apoptotic activity against melanoma cell lines, with selectivity observed for those harboring oncogenic NRAS.

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Section: Resultsmentioning

confidence: 99%

Amuvatinib has cytotoxic effects against NRAS-mutant melanoma but not BRAF-mutant melanoma

Fedorenko¹,

Fang²,

Koomen³

et al. 2014

Melanoma Research

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“…From a different angle, aiming at developing a method for routine evaluation of personalized treatments against melanoma, Rebecca et al [76] studied the effect of HSP90 inhibition by targeted proteomics measuring specifically about 80 signaling proteins and a few heat shock proteins. HSP90 inhibition resulted in increase of HSP71 (an inducible cytosolic HSP70 isoform) and both HSP90 isoforms levels in a NRAS mutant cell line.…”

Section: Global Impact Of Hsp90 Inhibition On the Proteomementioning

confidence: 99%

Proteomic interrogation of HSP90 and insights for medical research

Weidenauer

Wang

Joshi

et al. 2017

Expert Review of Proteomics

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Introduction Heat shock protein 90 (HSP90) regulates protein homeostasis in eukaryotes. As a ‘professional interactor’, HSP90 binds to and chaperones many proteins and has both housekeeping and disease-related functions but its regulation remains in part elusive. HSP90 complexes are a target for therapy, notably against cancer, and several inhibitors are currently in clinical trials. Proteomic studies have revealed the vast interaction network of HSP90 and, in doing so, the extent of cellular processes the chaperone takes part in, especially in yeast and human cells. Furthermore, small-molecule inhibitors were used to probe the global impact of its inhibition on the proteome. Areas covered We review here recent HSP90-related interactomics and total proteome studies and their relevance for research on cancer, neurodegenerative and pathogen diseases. Expert commentary Proteomics experiments are our best chance to identify the context-dependent global proteome of HSP90 and thus uncover and understand its disease-specific biology. However, understanding the complexity of HSP90 will require multiple complementary, quantitative approaches and novel bioinformatics to translate interactions into ordered functional networks and pathways. Developing therapies will necessitate more knowledge on HSP90 complexes and networks with disease relevance and on total proteome changes induced by their perturbation. Most work has been done in cancer, thus a lot remains to be done in the context of other diseases.

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“…As recently highlighted, the specific role such receptors play in cancer development and progression has still to be largely clarified [35]. The stimulatory role of PDGF-BB and PDGFR-beta has been demonstrated in several cells and tissues, including melanoma [36–40]. Non-selective inhibitors of both PDGFR-beta and PDGFR-alpha, such as imatinib and dasatinib, are known to partially inhibit melanoma growth, but the role of the alpha or beta receptors has not been fully clarified yet [41–43].…”

Section: Introductionmentioning

confidence: 99%

PDGFR-alpha inhibits melanoma growth via CXCL10/IP-10: a multi-omicsapproach

et al. 2016

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Melanoma is the most aggressive skin-cancer, showing high mortality at advanced stages. Platelet Derived Growth Factor Receptor-alpha (PDGFR-alpha) potently inhibits melanoma- and endothelium-proliferation and its expression is significantly reduced in melanoma-biopsies, suggesting that melanoma progression eliminates cells expressing PDGFR-alpha. In the present study transient overexpression of PDGFR-alpha in endothelial (HUVEC) and melanoma (SKMel-28, A375, Preyer) human-cells shows strong anti-proliferative effects, with profound transcriptome and miRNome deregulation. PDGFR-alpha overexpression strongly affects expression of 82 genes in HUVEC (41 up-, 41 down-regulated), and 52 genes in SKMel-28 (43 up-, 9 down-regulated). CXCL10/IP-10 transcript showed up to 20 fold-increase, with similar changes detectable at the protein level. miRNA expression profiling in cells overexpressing PDGFR-alpha identified 14 miRNAs up- and 40 down-regulated, with miR-503 being the most down-regulated (6.4 fold-reduction). miR-503, miR-630 and miR-424 deregulation was confirmed by qRT-PCR. Interestingly, the most upregulated transcript (i.e., CXCL10/IP-10) was a validated miR-503 target and CXCL10/IP-10 neutralization significantly reverted the anti-proliferative action of PDGFR-alpha, and PDGFR-alpha inhibition by Dasatinb totally reverted the CXCL10/IP10 induction, further supporting a functional interplay of these factors. Finally, integration of transcriptomics and miRNomics data highlighted several pathways affected by PDGFR-alpha.This study demonstrates for the first time that PDGFR-alpha strongly inhibits endothelial and melanoma cells proliferation in a CXCL10/IP-10 dependent way, via miR-503 down-regulation.

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Evaluating Melanoma Drug Response and Therapeutic Escape with Quantitative Proteomics

Cited by 53 publications

References 48 publications

Amuvatinib has cytotoxic effects against NRAS-mutant melanoma but not BRAF-mutant melanoma

Amuvatinib has cytotoxic effects against NRAS-mutant melanoma but not BRAF-mutant melanoma

Proteomic interrogation of HSP90 and insights for medical research

PDGFR-alpha inhibits melanoma growth via CXCL10/IP-10: a multi-omicsapproach

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