<i>RAS</i>Mutations in Cutaneous Squamous-Cell Carcinomas in Patients Treated with BRAF Inhibitors

Su, Fei; Virós, Amaya; Milagre, Carla; Trunzer, Kerstin; Bollag, Gideon; Spleiss, Olivia; Reis‐Filho, Jorge S.; Kong, Xiangju; Koya, Richard C.; Flaherty, Keith T.; Chapman, Paul B.; Kim, Min Jung; Hayward, Robert; Martin, Matthew W.; Yang, Hong; Wang, Qiongqing; Hilton, Holly; Hang, Julie S.; Noé, Johannes; Lambros, Maryou; Geyer, Felipe C.; Dhomen, Nathalie; Niculescu‐Duvaz, Ion; Zambon, Alfonso; Niculescu‐Duvaz, Dan; Preece, Natasha; Robert, Lídia; Otte, Nicholas; Mok, Stephen; Kee, Damien; Ma, Yan; Zhang, Chao; Habets, Gaston; Burton, Elizabeth A.; Wong, Bernice H.; Nguyen, Hoa; Kockx, Mark; Andries, Luc; Lestini, Brian; Nolop, K. B.; Lee, Richard J.; Joe, Andrew K.; Troy, James L.; González, René; Hutson, Thomas E.; Puzanov, Igor; Chmielowski, Bartosz; Springer, Caroline J.; McArthur, Grant A.; Sosman, Jeffrey A.; Lo, Roger S.; Ribas, Antoni; Marais, Richard

doi:10.1056/nejmoa1105358

Cited by 958 publications

(754 citation statements)

References 34 publications

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“…Small-molecule inhibitors of BRAF V600 kinase (vemurafenib, dabrafenib) significantly improved survival compared with chemotherapy in metastatic melanoma with BRAF V600 mutation, though resistance usually occcurs after a median 6-7 months and second malignancies can appear (19,20). BRAF inhibitors can provoke the reactivation of MAPK pathway downstream of BRAF kinase in a ras-dependent manner (21). Paradoxical activation of the MAPK pathway occurs not only in BRAFmutant melanoma cells, but in the BRAF wild-type and rasmutant normal cells driving the appearance of secondary cancers like hyperproliferative cutaneous lesions (21), primary melanoma (22) or leukaemia (23).…”

Section: Discussionmentioning

confidence: 99%

Combined dabrafenib and trametinib treatment in a case of chemotherapy-refractory extrahepatic BRAF V600E mutant cholangiocarcinoma: dramatic clinical and radiological response with a confusing synchronic new liver lesion

Kocsis

Árokszállási

András

et al. 2017

J. Gastrointest. Oncol.

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Since the prognosis of advanced cholangiocarcinoma (CCA) remains poor with traditional chemotherapy, attention has shifted to molecularly targeted agents. Results of available clinical studies reveal little or no benefit of using targeted agents in advanced CCA. Limitations of these trials could be the lack of comprehensive molecular and genetic characterization of CCA samples in order to identify potential drug targets. Here we report a case of a 59-year-old female with chemotherapy-refractor, metastatic extrahepatic cholangiocarcinoma (EHCCA). After failure of first-line chemotherapy with cisplatin plus gemcitabine, next generation sequencing (NGS) based tumor molecular profiling was performed on aspiration cytological sample, that revealed BRAF V600E mutation. Multidisciplinary team decided on the initiation of combined treatment with BRAF and MEK inhibitors. Dabrafenib was started orally 150 mg twice a day, adding trametinib 2 mg once a day. Right from the initiation of targeted therapy, significant clinical improvement had been observed. Even though the first restaging computed tomography (CT) scan at 8 weeks revealed spectacular decrease in all metastatic sites, a new hepatic mass of 67 mm × 40 mm was identified and interpreted as new metastatic lesion. As the clinical and radiological response was contradictory, CT-guided biopsy was taken from the hepatic lesion while the therapy was continued on. Histopathologic evaluation excluded the hepatic lesion from being a metastasis, instead described it as a fibrotic, inflammatory lesion.At 12 week, PET CT confirmed further tumor regression with complete regression of the multiple cerebral metastases. The therapy has been extremely well tolerated by the patient. According to our knowledge, this is the first reported case on a successful treatment of EHCCA with the combination of dabrafenib and trametinib. Our case highlights the importance of molecular profiling in CCA, in order to find potential actionable driver mutations for personalised treatment.

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Section: Discussionmentioning

confidence: 99%

Combined dabrafenib and trametinib treatment in a case of chemotherapy-refractory extrahepatic BRAF V600E mutant cholangiocarcinoma: dramatic clinical and radiological response with a confusing synchronic new liver lesion

Kocsis

Árokszállási

András

et al. 2017

J. Gastrointest. Oncol.

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“…A BRAF inhibitorok specifikus mellékhatásaként benignus (pl. papilloma) és (pre)malignus bőrtumorok (keratoacanthoma, spinalioma 19-26%-ban, második primer melanoma 1,6-2,4%-.ban) alakulhatnak ki (5. ábra), melyek kezelése sebészi eltávolítás, a terápia felfüggesztése nem szükséges (20,23,24). A háttérben a RAS-mutáns, de BRAF vad típusú sejtekben az inhibitor okozta paradox MAPK-útvonal aktiváció játszik elsősorban szerepet.…”

Section: Braf Inhibitor Kezelés (Hatékonyság Mellékhatás)unclassified

Targeted therapy for BRAF-mutation positive metastatic melanoma

Szabó¹,

Ócsai²,

Kiss³

et al. 2017

BVSZ

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ÖSSZEFOGLALÁS A BRAFV600E/K génmutáció a melanoma kialakulásá-ban és progressziójában is fontos pathogenetikai tényező. Az esetek felében kimutatható a tumor metasztázisban és hatásának ellensúlyozására kifejlesztett célzott molekulá- Kulcsszavak: áttétes melanoma -BRAF inhibitor -MEK inhibitor -gyógyszer mellékhatás SUMMARY An important pathogenic factor in both the development and progression of melanoma is the V600E/K mutation of BRAF, which can be found in half of metastatic tumors. It is unsurprising therefore that molecular inhibitors targeting its effect are able to offer significantly higher progression free and overall survival as compared to conventional chemotherapy in the majority of patients diagnosed with metastatic melanoma. Moreover, the combination of BRAF-and MEK inhibitor therapy has greatly improved the prognosis of patients with confirmed mutations in distant metastases, showing that optimal use of new therapeutic agents by broadening clinical expertise is an effective way of expanding the inventory of anti-melanoma agents. The management of potential adverse events related to new treatments is also improved by their widespread use and the consequent enhancement of practical knowledge related to the new agents, ultimately leading to the improvement of quality of life of patients. Key words: metastatic melanoma -BRAF inhibitor -MEK inhibitor -drug adverse eventA melanoma pathofiziológiájáról szerzett, az elmúlt év-tizedben robbanásszerűen felhalmozódott ismereteink és a modern biotechnológia lehetővé tették új típusú onkoterá-piák megjelenését, mint amilyenek a célzott molekuláris inhibitorok vagy a biológiai terápiák, és ezzel megváltoztatták a metasztatikus betegek túlélési esélyeit és átírták a korábbi kezelési irányvonalakat (1-3). A melanoma kialakulásában és progressziójában kulcsszerepet játszó génmutációk komplex módon, az intracelluláris jelátviteli folyamatok kö-zötti egyensúly megbomlását okozva vezetnek megnöve-kedett sejttúléléséhez, kórosan fokozott sejtproliferációhoz. Az egyik legfontosabb pathogenetikai lépés a MAPK (Mitogén Aktivált Protein-Kináz)-útvonal aktivitásának fokozódása (4), ami igen gyakran, a melanomás eseteknek a 160 Levelező szerző: Dr. Szabó Imre Lőrinc

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“…Sanger sequencing consists of polymerase chain reaction (PCR) amplification of the DNAís region of interest, limited by dideoxynucleotide end termination, followed by sequence reading. This technique has analytical sensitivity of 10-20% (Su et al, 2012;Lee et al, 2010;Morandi et al, 2012). The Cobas ® is another available method, based on real time PCR, with DNA probes designed specifically to detect V600 mutations: V600E, V600 K, and V600D.…”

Section: B-raf Mutation Detectionmentioning

confidence: 99%

“…Hypothetically, BRAF inhibitors exert a paradoxical activating effect over WT BRAF in keratinocytes, leading to cell proliferation and apoptosis inhibition (Su et al, 2012). Concomitant use of MEK and B-Raf inhibitors reduced dramatically the incidence of second cutaneous tumors in melanoma patients, by blocking MAPK pathway in a target downstream than B-Raf Long et al, 2014) (Fig.…”

Section: First and Second-generation B-raf Inhibitorsmentioning

confidence: 99%

“…Theoretically, this may reduce the incidence of side effects observed with previous B-Raf inhibitors, especially new cutaneous tumors, which have been associated to WT B-Raf activation in keratinocytes (Su et al, 2012). A phase I/II trial is currently recruiting colorectal and melanoma cancer patients to receive LGX818 (NCT01436656).…”

Section: New Drugs In Clinical Developmentmentioning

confidence: 99%

See 1 more Smart Citation

BRAF mutations in non-small cell lung cancer: has finally Janus opened the door?

Caparica

Castro

Gil-Bazo

et al. 2016

Critical Reviews in Oncology/Hematology

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RASMutations in Cutaneous Squamous-Cell Carcinomas in Patients Treated with BRAF Inhibitors

Cited by 958 publications

References 34 publications

Combined dabrafenib and trametinib treatment in a case of chemotherapy-refractory extrahepatic BRAF V600E mutant cholangiocarcinoma: dramatic clinical and radiological response with a confusing synchronic new liver lesion

Combined dabrafenib and trametinib treatment in a case of chemotherapy-refractory extrahepatic BRAF V600E mutant cholangiocarcinoma: dramatic clinical and radiological response with a confusing synchronic new liver lesion

Targeted therapy for BRAF-mutation positive metastatic melanoma

BRAF mutations in non-small cell lung cancer: has finally Janus opened the door?

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