Targeted Therapy for BRAF Mutant Brain Tumors

Appaji Rayi; Iyad Alnahhas; Shirley Ong; Pierre Giglio; Vinay K. Puduvalli

doi:10.1007/s11864-021-00901-9

Targeted Therapy for BRAF Mutant Brain Tumors

Appaji Rayi, Iyad Alnahhas, Shirley Ong, Pierre Giglio, Vinay K. Puduvalli

Neuro-Oncology

Research output: Contribution to journal › Review article › peer-review

3 Scopus citations

Abstract

Molecular heterogeneity has confounded attempts to target individual pathways in brain tumors. However, gliomas with BRAF mutations have been identified as being uniquely vulnerable to targeted therapies. Such mutations are predominantly seen in brain tumors of the adolescent and young adult population. Given that accurate and timely identification of such mutations is essential for offering appropriate treatment, treatment centers should offer both immunohistochemical and sequencing methods for detection of these mutations to guide treatment. Additional studies of these tumors at recurrence would also allow identification of breakthrough resistance mechanisms that may also be targetable for treatment. Due to the relative rarity of these tumors, multicenter collaborative studies will be essential in achieving long term control of these tumors.

Original language	English (US)
Article number	105
Journal	Current treatment options in oncology
Volume	22
Issue number	11
DOIs	https://doi.org/10.1007/s11864-021-00901-9
State	Published - Nov 2021

ASJC Scopus subject areas

Oncology
Pharmacology (medical)

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title = "Targeted Therapy for BRAF Mutant Brain Tumors",

abstract = "Molecular heterogeneity has confounded attempts to target individual pathways in brain tumors. However, gliomas with BRAF mutations have been identified as being uniquely vulnerable to targeted therapies. Such mutations are predominantly seen in brain tumors of the adolescent and young adult population. Given that accurate and timely identification of such mutations is essential for offering appropriate treatment, treatment centers should offer both immunohistochemical and sequencing methods for detection of these mutations to guide treatment. Additional studies of these tumors at recurrence would also allow identification of breakthrough resistance mechanisms that may also be targetable for treatment. Due to the relative rarity of these tumors, multicenter collaborative studies will be essential in achieving long term control of these tumors.",

author = "Appaji Rayi and Iyad Alnahhas and Shirley Ong and Pierre Giglio and Puduvalli, {Vinay K.}",

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T1 - Targeted Therapy for BRAF Mutant Brain Tumors

AU - Rayi, Appaji

AU - Alnahhas, Iyad

AU - Ong, Shirley

AU - Giglio, Pierre

AU - Puduvalli, Vinay K.

PY - 2021/11

Y1 - 2021/11

N2 - Molecular heterogeneity has confounded attempts to target individual pathways in brain tumors. However, gliomas with BRAF mutations have been identified as being uniquely vulnerable to targeted therapies. Such mutations are predominantly seen in brain tumors of the adolescent and young adult population. Given that accurate and timely identification of such mutations is essential for offering appropriate treatment, treatment centers should offer both immunohistochemical and sequencing methods for detection of these mutations to guide treatment. Additional studies of these tumors at recurrence would also allow identification of breakthrough resistance mechanisms that may also be targetable for treatment. Due to the relative rarity of these tumors, multicenter collaborative studies will be essential in achieving long term control of these tumors.

AB - Molecular heterogeneity has confounded attempts to target individual pathways in brain tumors. However, gliomas with BRAF mutations have been identified as being uniquely vulnerable to targeted therapies. Such mutations are predominantly seen in brain tumors of the adolescent and young adult population. Given that accurate and timely identification of such mutations is essential for offering appropriate treatment, treatment centers should offer both immunohistochemical and sequencing methods for detection of these mutations to guide treatment. Additional studies of these tumors at recurrence would also allow identification of breakthrough resistance mechanisms that may also be targetable for treatment. Due to the relative rarity of these tumors, multicenter collaborative studies will be essential in achieving long term control of these tumors.

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Targeted Therapy for BRAF Mutant Brain Tumors

Abstract

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