KRAS or BRAF mutation status is a useful predictor of sensitivity to MEK inhibition in ovarian cancer

Nakayama, Naomi; Nakayama, Katsuhiro; Yeasmin, Sabina; Ishibashi, Mariko; Katagiri, Atsuko; Iida, Kouji; Fukumoto, Manabu; Miyazaki, Kohji

doi:10.1038/sj.bjc.6604783

Cited by 90 publications

(83 citation statements)

References 36 publications

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“…Profound growth inhibition and apoptosis were observed in CI-1040-treated ovarian cancer cells with mutations in either KRAS or BRAF, compared with ovarian cancer cells containing wild-type KRAS/BRAF. 39 Although KRAS-mutated lung cancers, which comprise 20-30% of non-small cell lung cancers, are known not to respond to targeted therapies, recently it was shown that the combination of PI3K and MEK inhibitors may be a very potent combination in the treatment of KRAS-mutated lung cancers. When mouse models of lung cancer driven by mutant KRAS were treated with a combination of pan-PI3K, a mammalian target of rapamycin inhibitor, and an MEK inhibitor, there was marked synergy in shrinking these tumors.…”

Section: Discussionmentioning

confidence: 99%

Targeted genomic profiling reveals recurrent KRAS mutations and gain of chromosome 1q in mesonephric carcinomas of the female genital tract

et al. 2015

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Mesonephric carcinoma is a rare form of gynecologic cancer derived from mesonephric remnants usually located in the lateral wall of the uterine cervix. An analogous tumor occurs in the adnexa, female adnexal tumor of probable Wolffian origin. The pathogenesis and molecular events in mesonephric carcinoma are not known. The aim of this study was to examine the molecular alterations in mesonephric carcinoma to identify driver mutations and therapeutically targetable mutations. This study consisted of 19 tumors from 17 patients: 18 mesonephric carcinomas (15 primary tumors and three metastatic tumors) and 1 female adnexal tumor of probable Wolffian origin. In two patients, both primary and metastatic tumors were available. Genomic DNA was isolated and targeted next-generation sequencing was performed to detect mutations, copy number variations, and structural variants by surveying full exonic regions of 300 cancer genes and 113 selected intronic regions across 35 genes. Fluorescence in situ hybridization (FISH) for 1p and 1q was performed in two cases. Eighty-one percent (13/16) of mesonephric carcinomas had either a KRAS (n = 12) or NRAS (n = 1) mutation. Mutations in chromatin remodeling genes (ARID1A, ARID1B, or SMARCA4) were present in 62% of mesonephric carcinomas. All mesonephric carcinomas lacked mutations in PIK3CA and PTEN. The most common copy number alteration was 1q gain, found in 12 (75%) mesonephric carcinomas; this was confirmed by FISH in two cases. Mesonephric carcinoma is characterized by molecular alterations that differ from those of more common variants of cervical and endometrial adenocarcinoma, which harbor KRAS/NRAS mutations in 7% and 25% of cases, respectively. KRAS/NRAS mutations are common in mesonephric carcinoma and are often accompanied by gain of 1q and mutations in chromatin remodeling genes. Targeting inhibitors of the RAS/MAPK pathway may be useful in the treatment of mesonephric carcinoma.

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Section: Discussionmentioning

confidence: 99%

Targeted genomic profiling reveals recurrent KRAS mutations and gain of chromosome 1q in mesonephric carcinomas of the female genital tract

et al. 2015

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“…9 Meanwhile, these variants are the active subjects of clinical trials with MEK inhibitors in ovarian cancers. 29 Similarly, the p.Val600Glu variant of BRAF is druggable in melanoma, 12,30,31 whereas recent evidence indicates its potential predictive utility in colorectal cancer patients treated with EGFR inhibitors. 32 Figure 3 shows in further detail how sequence variants were classified for each of the four primary sites of cancer in our study.…”

Section: Resultsmentioning

confidence: 99%

A classification system for clinical relevance of somatic variants identified in molecular profiling of cancer

Sukhai

Craddock

Thomas

et al. 2016

Genetics in Medicine

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“…The results of a phase III study have demonstrated that GSK1120212 is associated with a significant improvement in progression-free survival and overall survival, compared with chemotherapy, in patients with V600E or V600K BRAF-mutated advanced melanoma (23). Several studies have shown that KRAS and/ or BRAF mutations are associated with the sensitivity to MEK inhibitors in melanoma, thyroid cancer, colon cancer, and ovarian cancer (23)(24)(25)(26)(27). However, very limited information is available about the somatic MEK1 mutations in human malignancies.…”

Section: Discussionmentioning

confidence: 99%

MEK Inhibitor for Gastric Cancer with MEK1 Gene Mutations

Sogabe

Togashi

Katô

et al. 2014

Molecular Cancer Therapeutics

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The prognosis for patients with unresectable advanced or recurrent gastric cancer remains poor. The identification of additional oncogenes with influences similar to those of epidermal growth factor receptor gene mutations, upon which the growth of cancer cells is dependent, is needed. In this study, we evaluated sensitivity to MEK inhibitors (GSK1120212 and PD0325901) in several gastric cancer cell lines in vitro and found three poorly differentiated gastric cancer cell lines that were hypersensitive to the inhibitors. The sequence analyses in these three cell lines revealed that one cell line had a novel MEK1 mutation, while the other two had previously reported KRAS and MEK1 mutations, respectively; the gene statuses of the other resistant cell lines were all wild-type. Experiments using MEK1 expression vectors demonstrated that the MEK1 mutations induced the phosphorylation of ERK1/2 and had a transforming potential, enhancing the tumorigenicity. The MEK inhibitor dramatically reduced the phosphorylation of ERK1/2 and induced apoptosis in the cell lines with MEK1 mutations. In vivo, tumor growth was also dramatically decreased by an inhibitor. One of the 46 gastric cancer clinical samples that were examined had a MEK1 mutation; this tumor had a poorly differentiated histology. Considering the addiction of cancer cells to active MEK1 mutations for proliferation, gastric cancer with such oncogenic MEK1 mutations might be suitable for targeted therapy with MEK inhibitors.

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KRAS or BRAF mutation status is a useful predictor of sensitivity to MEK inhibition in ovarian cancer

Cited by 90 publications

References 36 publications

Targeted genomic profiling reveals recurrent KRAS mutations and gain of chromosome 1q in mesonephric carcinomas of the female genital tract

Targeted genomic profiling reveals recurrent KRAS mutations and gain of chromosome 1q in mesonephric carcinomas of the female genital tract

A classification system for clinical relevance of somatic variants identified in molecular profiling of cancer

MEK Inhibitor for Gastric Cancer with MEK1 Gene Mutations

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