Targeted MAPK pathway inhibitors in patients with disseminated pilocytic astrocytomas

Anastasia Drobysheva; Laura J Klesse; Daniel C Bowers; Veena Rajaram; Dinesh Rakheja; Charles F Timmons; Jason Wang; Korgun Koral; Lynn Gargan; Erica Ramos; Jason Y Park

doi:10.6004/jnccn.2017.0139

Targeted MAPK pathway inhibitors in patients with disseminated pilocytic astrocytomas

Anastasia Drobysheva, Laura J Klesse, Daniel C Bowers, Veena Rajaram, Dinesh Rakheja, Charles F Timmons, Jason Wang, Korgun Koral, Lynn Gargan, Erica Ramos, Jason Y Park

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23 Scopus citations

Abstract

This report presents a series of 5 pediatric patients with disseminated pilocytic astrocytomas and frequent nonfusion activating mutations. Genetic variants in these patients' tumors include BRAF p.Val600Glu, BRAF p.Val600Asp, and KRAS p.Gly60-Gln62ins7. The 2 patients with BRAF-mutated tumors were treated with dabrafenib or a combination of dabrafenib plus trametinib. The patients had either near complete resolution of the primary tumor (BRAF p.Val600Glu) or a stable primary tumor (BRAF p.Val600Asp). Both patients showed improvement in leptomeningeal dissemination without significant toxicity. Genomic testing of disseminated pilocytic astrocytomas, particularly those arising at extracerebellar locations, may result in the identification of mutations associated with ERK/MAPK activation. Patients with these activating mutations may benefit from targeted therapies.

Original language	English (US)
Pages (from-to)	978-982
Number of pages	5
Journal	JNCCN Journal of the National Comprehensive Cancer Network
Volume	15
Issue number	8
DOIs	https://doi.org/10.6004/jnccn.2017.0139
State	Published - Aug 2017

ASJC Scopus subject areas

Oncology

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title = "Targeted MAPK pathway inhibitors in patients with disseminated pilocytic astrocytomas",

abstract = "This report presents a series of 5 pediatric patients with disseminated pilocytic astrocytomas and frequent nonfusion activating mutations. Genetic variants in these patients' tumors include BRAF p.Val600Glu, BRAF p.Val600Asp, and KRAS p.Gly60-Gln62ins7. The 2 patients with BRAF-mutated tumors were treated with dabrafenib or a combination of dabrafenib plus trametinib. The patients had either near complete resolution of the primary tumor (BRAF p.Val600Glu) or a stable primary tumor (BRAF p.Val600Asp). Both patients showed improvement in leptomeningeal dissemination without significant toxicity. Genomic testing of disseminated pilocytic astrocytomas, particularly those arising at extracerebellar locations, may result in the identification of mutations associated with ERK/MAPK activation. Patients with these activating mutations may benefit from targeted therapies.",

author = "Anastasia Drobysheva and Klesse, {Laura J} and Bowers, {Daniel C} and Veena Rajaram and Dinesh Rakheja and Timmons, {Charles F} and Jason Wang and Korgun Koral and Lynn Gargan and Erica Ramos and Park, {Jason Y}",

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year = "2017",

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AU - Drobysheva, Anastasia

AU - Klesse, Laura J

AU - Bowers, Daniel C

AU - Rajaram, Veena

AU - Rakheja, Dinesh

AU - Timmons, Charles F

AU - Wang, Jason

AU - Koral, Korgun

AU - Gargan, Lynn

AU - Ramos, Erica

AU - Park, Jason Y

PY - 2017/8

Y1 - 2017/8

N2 - This report presents a series of 5 pediatric patients with disseminated pilocytic astrocytomas and frequent nonfusion activating mutations. Genetic variants in these patients' tumors include BRAF p.Val600Glu, BRAF p.Val600Asp, and KRAS p.Gly60-Gln62ins7. The 2 patients with BRAF-mutated tumors were treated with dabrafenib or a combination of dabrafenib plus trametinib. The patients had either near complete resolution of the primary tumor (BRAF p.Val600Glu) or a stable primary tumor (BRAF p.Val600Asp). Both patients showed improvement in leptomeningeal dissemination without significant toxicity. Genomic testing of disseminated pilocytic astrocytomas, particularly those arising at extracerebellar locations, may result in the identification of mutations associated with ERK/MAPK activation. Patients with these activating mutations may benefit from targeted therapies.

AB - This report presents a series of 5 pediatric patients with disseminated pilocytic astrocytomas and frequent nonfusion activating mutations. Genetic variants in these patients' tumors include BRAF p.Val600Glu, BRAF p.Val600Asp, and KRAS p.Gly60-Gln62ins7. The 2 patients with BRAF-mutated tumors were treated with dabrafenib or a combination of dabrafenib plus trametinib. The patients had either near complete resolution of the primary tumor (BRAF p.Val600Glu) or a stable primary tumor (BRAF p.Val600Asp). Both patients showed improvement in leptomeningeal dissemination without significant toxicity. Genomic testing of disseminated pilocytic astrocytomas, particularly those arising at extracerebellar locations, may result in the identification of mutations associated with ERK/MAPK activation. Patients with these activating mutations may benefit from targeted therapies.

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Targeted MAPK pathway inhibitors in patients with disseminated pilocytic astrocytomas

Abstract

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