Circulating pEGFR Is a Candidate Response Biomarker of Cetuximab Therapy in Colorectal Cancer

Κάτσιλα, Θεοδώρα; Juliachs, Mercèe; Gregori, Josep Fortiana; Macarulla, Teresa; Villarreal, Laura; Bardelli, Alberto; Torrance, Chris; Élez, Elena; Tabernero, Josep; Villanueva, Josep

doi:10.1158/1078-0432.ccr-14-0361

Cited by 22 publications

(13 citation statements)

References 35 publications

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“…Some of these unconventionally secreted proteins have a welldefined intracellular function (6). We have previously shown that the unconventional secretion of the EGFR correlates with the response of colorectal cancer patients to the therapeutic antibody cetuximab (8). Agreeing with our observations, proteins classically located intracellularly such as HSP90, tRNA synthetases, and HMGB1 have recently been identified in the extracellular space performing alternative functions related to cancer (9)(10)(11).…”

Section: Introductionsupporting

confidence: 76%

Extracellular HMGA1 Promotes Tumor Invasion and Metastasis in Triple-Negative Breast Cancer

Méndez¹,

Peg

Salvans³

et al. 2018

Clinical Cancer Research

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The study of the cancer secretome suggests that a fraction of the intracellular proteome could play unanticipated roles in the extracellular space during tumorigenesis. A project aimed at investigating the invasive secretome led us to study the alternative extracellular function of the nuclear protein high mobility group A1 (HMGA1) in breast cancer invasion and metastasis. Antibodies against HMGA1 were tested in signaling, adhesion, migration, invasion, and metastasis assays using breast cancer cell lines and xenograft models. Fluorescence microscopy was used to determine the subcellular localization of HMGA1 in cell lines, xenograft, and patient-derived xenograft models. A cohort of triple-negative breast cancer (TNBC) patients was used to study the correlation between subcellular localization of HMGA1 and the incidence of metastasis. Our data show that treatment of invasive cells with HMGA1-blocking antibodies in the extracellular space impairs their migration and invasion abilities. We also prove that extracellular HMGA1 (eHMGA1) becomes a ligand for the Advanced glycosylation end product-specific receptor (RAGE), inducing pERK signaling and increasing migration and invasion. Using the cytoplasmic localization of HMGA1 as a surrogate marker of secretion, we showed that eHMGA1 correlates with the incidence of metastasis in a cohort of TNBC patients. Furthermore, we show that HMGA1 is enriched in the cytoplasm of tumor cells at the invasive front of primary tumors and in metastatic lesions in xenograft models. Our results strongly suggest that eHMGA1 could become a novel drug target in metastatic TNBC and a biomarker predicting the onset of distant metastasis.

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Section: Introductionsupporting

confidence: 76%

Extracellular HMGA1 Promotes Tumor Invasion and Metastasis in Triple-Negative Breast Cancer

Méndez¹,

Peg

Salvans³

et al. 2018

Clinical Cancer Research

Self Cite

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“…Interestingly, we observed that two compounds with limited effects in 2D culture displayed enhanced activity in the 3D setting (PX‐866 and AZD6482); this raises the possibility that certain PI3K inhibitors may be underestimated based on adherent culture results alone. This needs careful exploration given that 3D disease models can be more reflective of the drug sensitivity profile found in patients (Katsila et al., ).…”

Section: Discussionmentioning

confidence: 99%

Enhancing the evaluation of PI3K inhibitors through 3D melanoma models

Shannan

Chen

Watters

et al. 2016

Pigment Cell Melanoma Res

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Targeted therapies for mutant BRAF metastatic melanoma are effective but not curative due to acquisition of resistance. PI3K signaling is a common mediator of therapy resistance in melanoma; thus, the need for effective PI3K inhibitors is critical. However, testing PI3K inhibitors in adherent cultures is not always reflective of their potential in vivo. To emphasize this, we compared PI3K inhibitors of different specificity in two- and three-dimensional (2D, 3D) melanoma models and show that drug response predictions gain from evaluation using 3D models. Our results in 3D demonstrate the anti-invasive potential of PI3K inhibitors and that drugs such as PX-866 have beneficial activity in physiological models alone and when combined with BRAF inhibition. These assays finally help highlight pathway effectors that could be involved in drug response in different environments (e.g. p4E-BP1). Our findings show the advantages of 3D melanoma models to enhance our understanding of PI3K inhibitors.

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“…They noted that during cetuximab treatment, pEGFR levels increased in patients who responded well to treatment, did not evolve in patients with stabilisation of the disease, and decreased in patients with disease progression. The authors subsequently validated this hypothesis by measuring the secretome in 3D cultures obtained from several lines of SW48 colorectal cancer cells with different sensitivities to cetuximab [60]. This latter study is a good example of a proteomic study performed on human samples and validated by in vitro cell models, hence promoting the use of 3D cell cultures obtained directly from patient samples to pre-test the treatment.…”

Section: Proteomics For Biomarker Researchmentioning

confidence: 97%

Clinical Proteomics in Colorectal Cancer, a Promising Tool for Improving Personalised Medicine

Chauvin

Boisvert

2018

Proteomes

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Colorectal cancer is the third most common and the fourth most lethal cancer worldwide. In most of cases, patients are diagnosed at an advanced or even metastatic stage, thus explaining the high mortality. The lack of proper clinical tests and the complicated procedures currently used for detecting this cancer, as well as for predicting the response to treatment and the outcome of a patient’s resistance in guiding clinical practice, are key elements driving the search for biomarkers. In the present overview, the different biomarkers (diagnostic, prognostic, treatment resistance) discovered through proteomics studies in various colorectal cancer study models (blood, stool, biopsies), including the different proteomic techniques used for the discovery of these biomarkers, are reviewed, as well as the various tests used in clinical practice and those currently in clinical phase. These studies define the limits and perspectives related to proteomic biomarker research for personalised medicine in colorectal cancer.

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Circulating pEGFR Is a Candidate Response Biomarker of Cetuximab Therapy in Colorectal Cancer

Cited by 22 publications

References 35 publications

Extracellular HMGA1 Promotes Tumor Invasion and Metastasis in Triple-Negative Breast Cancer

Extracellular HMGA1 Promotes Tumor Invasion and Metastasis in Triple-Negative Breast Cancer

Enhancing the evaluation of PI3K inhibitors through 3D melanoma models

Clinical Proteomics in Colorectal Cancer, a Promising Tool for Improving Personalised Medicine

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