Wild-Type <i>BRAF</i> Is Required for Response to Panitumumab or Cetuximab in Metastatic Colorectal Cancer

Nicolantonio, Federica Di; Martini, Miriam; Molinari, Francesca; Sartore-Bianchi, Andrea; Arena, Sabrina; Saletti, Piercarlo; Dosso, Sara De; Mazzucchelli, Luca; Frattini, Milo; Siena, Salvatore; Bardelli, Alberto

doi:10.1200/jco.2008.18.0786

Cited by 1,495 publications

(1,129 citation statements)

References 36 publications

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“…As regards BRAF mutations, even if evaluated in a small subgroup of patients, our findings are consistent with the most part of published studies which have validated BRAF mutations obtained from primary tumour specimens as a strong negative prognostic biomarker in metastatic CRC (Ahn et al, 2014), showing a more aggressive and chemo-refractory behavior compared to wild-type tumours (Tran et al, 2011). However it's interesting to observe that the percentages of BRAF mutations (2-4%) in all the included studies is lower than those reported in the literature (5-10%) (Sridhar et al, 2005;Di Nicolantonio et al, 2008), likely due to the clinical selection of patients included in such studies. Indeed, because of their peculiar metastatic spread, BRAF-mutated tumours are usually detected as an advanced disease, rarely candidate for liver surgery.…”

Section: Discussionsupporting

confidence: 89%

Can KRAS and BRAF mutations limit the benefit of liver resection in metastatic colorectal cancer patients? A systematic review and meta-analysis

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Bronte

Bazan

et al. 2016

Critical Reviews in Oncology/Hematology

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Background: Clinical trials investigated the potential role of both KRAS and BRAF mutations, as prognostic biomarkers, in colorectal cancer (CRC) patients who underwent surgical treatment of CRC-related liver metastases (CLM), showing conflicting results. This meta-analysis aims to review all the studies reporting survival outcomes (recurrence free survival (RFS), and/or overall survival (OS)) of patients undergoing resection of CLM, stratified according to KRAS and/or BRAF mutation status. Materials and methods: Data from all published studies reporting survival outcomes (RFS and/or OS) of CRC patients who received resection of CLM, stratified by KRAS and/or BRAF mutation status were collected, according to the PRISMA guidelines. Pooled HRs were calculated for both the OS and/or RFS. Results: Seven eligible trials (1403 patients) were included. Pooled analysis showed that KRAS mutations predicted a significantly worse both RFS (HR: 1.65; 95% CI: 1.23-2.21) and OS (HR: 1.86; 95% CI: 1.51-2.30) in patients who underwent surgical resection of CLM. BRAF mutations were also associated with a significantly worse OS (HR: 3.90; 95% CI: 1.96-7.73) in this subgroup of patients. Conclusions: This meta-analysis suggests both KRAS and BRAF mutations as poor, prognostic biomarkers, associated with worse survival outcomes, in patients undergoing hepatic resection of CLM

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Section: Discussionsupporting

confidence: 89%

Can KRAS and BRAF mutations limit the benefit of liver resection in metastatic colorectal cancer patients? A systematic review and meta-analysis

Passiglia

Bronte

Bazan

et al. 2016

Critical Reviews in Oncology/Hematology

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“…215 The results showed that none of the patients who experienced a response displayed BRAF mutations, whereas 11 of 79 (14%) nonresponders carried a BRAF V600E allele. 215 As BRAF mutations are mutually exclusive to EGFR and KRAS mutations, it is likely to be associated with lack of response to EGFR TKIs. 138 …”

Section: Braf Mutationmentioning

confidence: 94%

“…215 BRAF mutations are found in 1-3% of lung cancers, most of which are adenocarcinomas. 206,212 BRAF mutations are found in a mutually exclusive pattern with KRAS mutations, suggesting that these genetic events activate a set of common downstream effectors of transformation.…”

Section: Braf Mutationmentioning

confidence: 99%

Molecular pathology of lung cancer: key to personalized medicine

et al. 2012

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The majority of lung adenocarcinoma patients with epidermal growth factor receptor-(EGFR) mutated or EML4-ALK rearrangement-positive tumors are sensitive to tyrosine kinase inhibitors. Both primary and acquired resistance in a significant number of those patients to these therapies remains a major clinical problem. The specific molecular mechanisms associated with tyrosine kinase inhibitor resistance are not fully understood. Clinicopathological observations suggest that molecular alterations involving so-called 'driver mutations' could be used as markers that aid in the selection of patients most likely to benefit from targeted therapies. In this review, we summarize recent developments involving the specific molecular mechanisms and markers that have been associated with primary and acquired resistance to EGFR-targeted therapy in lung adenocarcinomas. Understanding these mechanisms may provide new treatment avenues and improve current treatment algorithms.

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“…14 In the case of colorectal carcinomas, BRAFV600E mutation positive patients have significantly shorter progression-free survival when compared with patients with tumors with BRAF wild-type and its presence is shown to impair the therapeutic effect of drugs such as cetuximab and panitumumab. 15 The recognition of BRAFV600E mutation and its prognostic value has led to accelerated attempts to utilize it as a target for cancer therapy. Briefly, recent drugs targeted against mutated BRAF (particularly in melanomas) have shown great promise in early clinical trials.…”

mentioning

confidence: 99%

Immunohistochemistry with a mutation-specific monoclonal antibody as a screening tool for the BRAFV600E mutational status in primary cutaneous malignant melanoma

2013

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The V600E mutation of BRAF has emerged as both an effective biomarker and therapeutic target for select benign and malignant cutaneous and non-cutaneous human tumors and is typically determined using DNAbased techniques that include allele-specific PCR and direct DNA sequencing. Recently however, the development of new antibodies directed against the V600E protein has opened the door for an easier and more efficient strategy for identifying this mutation. Our present aim was to determine the efficacy of one such antibody, anti-B-Raf (V600E), a mouse monoclonal antibody in which the immunogen is a synthetic peptide derived from the internal region of BRAFV600E. A total of 35 cases of primary cutaneous melanoma were evaluated using a combination of DNA-based techniques that included allele-specific PCR and/or direct DNA sequencing and immunohistochemistry. Cases of papillary thyroid carcinomas (n ¼ 5) and colorectal carcinomas (n ¼ 5), known to harbor the BRAFV600E mutation, served as positive controls for the study. DNA analyses revealed that 6 of 35 (17%) cases of the primary cutaneous malignant melanoma possessed the BRAFV600E mutation. For immunohistochemical analyses, cytoplasmic positivity with anti-B-Raf was noted in 7 of 35 (20%) cases of primary melanoma and in all 10 positive controls. Statistical analyses of the data demonstrated that the sensitivity of the immunohistochemistry was 100% and specificity was 97%. Findings from the current study support the potential use of immunohistochemistry as an ancillary screening tool to assess the BRAFV600E mutation status in primary cutaneous melanoma.

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Wild-Type BRAF Is Required for Response to Panitumumab or Cetuximab in Metastatic Colorectal Cancer

Cited by 1,495 publications

References 36 publications

Can KRAS and BRAF mutations limit the benefit of liver resection in metastatic colorectal cancer patients? A systematic review and meta-analysis

Can KRAS and BRAF mutations limit the benefit of liver resection in metastatic colorectal cancer patients? A systematic review and meta-analysis

Molecular pathology of lung cancer: key to personalized medicine

Immunohistochemistry with a mutation-specific monoclonal antibody as a screening tool for the BRAFV600E mutational status in primary cutaneous malignant melanoma

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