BRAF mutations in low-grade serous ovarian cancer and response to BRAF inhibition

Balleine, Rosemary L.; Bowtell, D.; Bowtell, David D.L.; Chenevix-Trench, G.; Chiew, Yoke-Eng; DeFazio, A.; deFazio, Anna; Dobrovic, Alexander; Etemadmoghadam, Dariush; Fereday, S.; Fereday, Sian; Gao, Bo; Gertig, D.; Green, A.; Grimmond, Sean M.; Harnett, Paul R.; Harrap, K.; Hogg, Russell; Kan, Casina; Kennedy, Catherine J.; Moore, S.; Moujaber, Tania; Patch, Ann-Marie; Pearson, John V.; Saunders, Catherine; Srirangan, Sivatharsny; Traficante, N.; Traficante, Nadia; Waddell, Nicola; Wain, Gerard V.; Webb, P.

BRAF mutations in low-grade serous ovarian cancer and response to BRAF inhibition

Authors: Rosemary L. Balleine
D. Bowtell
David D.L. Bowtell
G. Chenevix-Trench
Yoke-Eng Chiew
A. DeFazio
Anna deFazio
Alexander Dobrovic
Dariush Etemadmoghadam
S. Fereday
Sian Fereday
Bo Gao
D. Gertig
A. Green
Sean M. Grimmond
Paul R. Harnett
K. Harrap
Russell Hogg
Casina Kan
Catherine J. Kennedy
S. Moore
Tania Moujaber
Ann-Marie Patch
John V. Pearson
Catherine Saunders
Sivatharsny Srirangan
N. Traficante
Nadia Traficante
Nicola Waddell
Gerard V. Wain
P. Webb
Publication date: 1 January 2018
Publisher: 'American Society of Clinical Oncology (ASCO)'
Doi

Abstract

Purpose Low-grade serous ovarian carcinoma (LGSC) responds poorly to chemotherapy and is characterized by activating mutations in the Ras sarcoma-mitogen-activated protein kinase (RAS-MAPK) pathway, including oncogenic BRAF. However, response to BRAF inhibitors is tumor-type specific. Significant improvement in survival is seen in patients with BRAF-mutant melanoma, but other cancer types, such as colorectal cancers, are generally less sensitive. We examined the frequency and characteristics of BRAF-mutated LGSC and described the response to treatment with BRAF inhibitors. Patients and Methods Mutations were assessed in LGSC (N = 65) by using targeted, exome, and whole-genome sequencing. Patient characteristics, treatment, and clinical outcome were assessed, and the median follow-up time was more than 5 years. BRAF inhibitors were trialed in two patients with a somatic BRAF V600E mutation: one patient received dabrafenib monotherapy and was monitored clinically, biochemically (cancer antigen [CA]-125 levels), and with positron emission tomography (PET) imaging. Expression of the BRAF V600E protein in this patient was assessed by immunohistochemistry. Results Among patients with LGSC, nine (13.8%) of 65 had a somatic BRAF mutation. Of the nine patients with BRAF mutation-positive LGSC, four experienced progressive disease that did not respond to conventional chemotherapy. Two of the patients experienced progression quickly and died as a result of disease progression, and two received targeted treatment. Two patients with BRAF V600E mutation received BRAF inhibitors at relapse and both achieved durable responses. Conclusion BRAF mutations are not uncommon in patients with LGSC and should be routinely tested, because BRAF inhibitors can be an effective treatment for these patients. The results highlight the need for targeted treatment in this rare tumor type, and a prospective study is needed to formally assess the response rate and clinical benefit

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