The biology of personalized cancer medicine: Facing individual complexities underlying hallmark capabilities

Palma, Michele De; Hanahan, Douglas

doi:10.1016/j.molonc.2012.01.011

Cited by 142 publications

(99 citation statements)

References 161 publications

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“…Alternatively, combination with anti-HGF antibodies could be envisioned to enhance the pharmacologic effect of a MET-selective drug, thus accomplishing a more favorable therapeutic response at the highest tolerated dose. With respect to the latter possibility, it should be kept in mind that only a minor fraction of patients eligible for a targeted therapy based on genetic testing respond clinically to pharmacologic blockade of the corresponding target (45). Considering the high levels of HGF frequently found in the tumor microenvironment, innate resistance to MET inhibitors in a significant percentage of these nonresponders could probably be overcome by HGF neutralization using agents like ficlatuzumab, thereby contributing to increasing the overall response rate.…”

Section: Discussionmentioning

confidence: 99%

Microenvironment-Derived HGF Overcomes Genetically Determined Sensitivity to Anti-MET Drugs

et al. 2014

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Cell-based drug screenings indicate that tumors displaying c-MET gene amplification are "addicted" to MET signaling and therefore are very sensitive to MET-targeted agents. However, these screenings were conducted in the absence of the MET ligand, hepatocyte growth factor (HGF), which is abundant in the tumor microenvironment. Sensitivity of six MET-addicted human tumor cells to three MET kinase inhibitors (JNJ-38877605, PHA-665752, crizotinib) and one antagonistic anti-MET antibody (DN30 Fab) was analyzed in the absence or presence of HGF, in a stroma-tumor coculture system, and by combining anti-MET drugs with an HGF neutralizing antibody (ficlatuzumab) in human HGF knock-in mice bearing c-MET-amplified tumors. In all models examined, HGF promoted resistance to MET-targeted agents, affecting both their potency and efficacy. HGF-induced resistance was due to restoration of physiologic GAB1-mediated PI3K activation that compensated for loss of aberrant HER3-dependent PI3K signaling. Ficlatuzumab restored sensitivity to MET-targeted agents in coculture systems and overcame resistance to JNJ-38877605, crizotinib, and DN30 Fab in human HGF knock-in mice. These data suggest that c-MET-amplified tumor cells-which normally exhibit ligand-independent, constitutive MET activation-become dependent on HGF for survival upon pharmacologic MET inhibition. Because HGF is frequently overexpressed in human cancer, this mechanism may represent a major cause of resistance to anti-MET therapies. The ability of ficlatuzumab to overcome HGF-mediated resistance generates proof of principle that vertical inhibition of both a tyrosine kinase receptor and its ligand can be therapeutically beneficial and opens new perspectives for the treatment of MET-dependent tumors. Cancer Res; 74(22); 6598-609. Ó2014 AACR.

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Section: Discussionmentioning

confidence: 99%

Microenvironment-Derived HGF Overcomes Genetically Determined Sensitivity to Anti-MET Drugs

et al. 2014

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“…Due to the vast heterogeneity of fibroblasts, as well as their different origins, much of the accumulating knowledge on the functional roles and activation pathways of fibroblasts may be tumour typeand tumour stage-specific. Nevertheless, clinical oncology is progressing increasingly towards a new era of integrative cancer therapy, based on personalized diagnostics that takes into account the individual complexities of tumours, including cells, pathways, and molecular mediators in the tumour microenvironment [118]. As a result, cancer therapeutics is moving progressively towards combinatorial approaches that act synergistically by targeting intrinsic pathways in neoplastic cells, as well as extrinsic tumour-enabling pathways in the tumour microenvironment.…”

Section: Discussionmentioning

confidence: 99%

From sentinel cells to inflammatory culprits: cancer‐associated fibroblasts in tumour‐related inflammation

Servais

Erez

2012

The Journal of Pathology

130

110

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“…Non-small cell lung cancers that exhibit mutational activation of the EGF receptor (EGFR) tyrosine kinase respond to EGFR inhibitors, whereas those with an intrachromosomal translocation of anaplastic lymphoma kinase ( ALK ) express constitutively active ALK fusion proteins that confer hypersensitivity to ALK inhibitors. Melanomas displaying a mutationally active BRAF kinase undergo massive regression following treatment with specifi c BRAF inhibitors ( 1 ).…”

Section: Introductionmentioning

confidence: 99%

Compensatory Pathways in Oncogenic Kinase Signaling and Resistance to Targeted Therapies: Six Degrees of Separation

Trusolino¹,

Bertotti²

2012

Cancer Discovery

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Summary :The effi cacy of targeted therapies against mutationally activated kinases is typically limited by the engagement of growth-promoting cues that compensate for inhibition of the targeted kinase. Initial studies have highlighted the contribution of genomic alterations, functional characteristics, and signaling feedback loops-all intrinsic to cancer cells-in sustaining such substitute activities. New evidence now indicates that the relative expression of growth factor ligands produced by the tumor microenvironment can relay redundant survival pathways, which may broadly impair responsiveness to kinase inhibitors. Cancer Discov; 2(10); 876-80.

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The biology of personalized cancer medicine: Facing individual complexities underlying hallmark capabilities

Cited by 142 publications

References 161 publications

Microenvironment-Derived HGF Overcomes Genetically Determined Sensitivity to Anti-MET Drugs

Microenvironment-Derived HGF Overcomes Genetically Determined Sensitivity to Anti-MET Drugs

From sentinel cells to inflammatory culprits: cancer‐associated fibroblasts in tumour‐related inflammation

Compensatory Pathways in Oncogenic Kinase Signaling and Resistance to Targeted Therapies: Six Degrees of Separation

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