F32CA284834
Project Grant
Overview
Grant Description
Identifying Genetic Vulnerabilities in KIAA1549-BRAF Mutant Pediatric Low-Grade Gliomas - Project Summary:
Pediatric low-grade gliomas (PLGGs) typically harbor only a single oncogenic driver event, which almost universally results in MAPK pathway activation. The most frequent of these alterations is a rearrangement that fuses the C-terminus of BRAF to the large transmembrane protein KIAA1549. Many patients whose tumors harbor this fusion respond to BRAF inhibitors, but challenges remain in extending clinical benefit to all patients.
A key challenge is that patients require chronic treatment with these inhibitors throughout childhood because tumors often rebound upon cessation of treatment. These inhibitors are associated with significant dose-limiting toxicity issues, likely because the MAPK pathway is essential for brain development. These observations suggest that we need to identify new therapeutic targets for PLGG.
The two core members of the POMT complex and two complex cofactors emerged as the top four dependencies in a genome-scale loss of function CRISPR/Cas9 screen. This dependency was specific for cells harboring the KIAA1549-BRAF fusion and were not dependencies in cells expressing BRAFV600E. The POMT complex is necessary for O-mannosylation of secreted and transmembrane proteins. This is striking because across all proteins in the human proteome, KIAA1549 is one of the proteins most affected by this post-translational modification.
It was originally hypothesized that the KIAA1549-BRAF fusion activates BRAF by truncating its negative regulatory domain, but this observation suggests that the KIAA1549 portion of the fusion may also be necessary for activating BRAF. The primary goals of this proposal are to understand why the POMT complex is a vulnerability in KIAA1549-BRAF mutant cells and to understand how the KIAA1549 portion of KIAA1549-BRAF regulates the activity of the fusion.
In Aim 1, I will test the hypothesis that POMT complex activity is necessary for the survival of KIAA1549-BRAF-dependent cells. In Aim 2, I will test the hypothesis that the POMT complex is required for O-mannosylation of KIAA1549-BRAF and that O-mannosylation of KIAA1549-BRAF is necessary for oncogenic signaling. In Aim 3, I will test the hypothesis that the KIAA1549 portion of the KIAA1549-BRAF fusion tethers BRAF to the plasma membrane and enhances its ability to activate the MAPK pathway.
Pediatric low-grade gliomas (PLGGs) typically harbor only a single oncogenic driver event, which almost universally results in MAPK pathway activation. The most frequent of these alterations is a rearrangement that fuses the C-terminus of BRAF to the large transmembrane protein KIAA1549. Many patients whose tumors harbor this fusion respond to BRAF inhibitors, but challenges remain in extending clinical benefit to all patients.
A key challenge is that patients require chronic treatment with these inhibitors throughout childhood because tumors often rebound upon cessation of treatment. These inhibitors are associated with significant dose-limiting toxicity issues, likely because the MAPK pathway is essential for brain development. These observations suggest that we need to identify new therapeutic targets for PLGG.
The two core members of the POMT complex and two complex cofactors emerged as the top four dependencies in a genome-scale loss of function CRISPR/Cas9 screen. This dependency was specific for cells harboring the KIAA1549-BRAF fusion and were not dependencies in cells expressing BRAFV600E. The POMT complex is necessary for O-mannosylation of secreted and transmembrane proteins. This is striking because across all proteins in the human proteome, KIAA1549 is one of the proteins most affected by this post-translational modification.
It was originally hypothesized that the KIAA1549-BRAF fusion activates BRAF by truncating its negative regulatory domain, but this observation suggests that the KIAA1549 portion of the fusion may also be necessary for activating BRAF. The primary goals of this proposal are to understand why the POMT complex is a vulnerability in KIAA1549-BRAF mutant cells and to understand how the KIAA1549 portion of KIAA1549-BRAF regulates the activity of the fusion.
In Aim 1, I will test the hypothesis that POMT complex activity is necessary for the survival of KIAA1549-BRAF-dependent cells. In Aim 2, I will test the hypothesis that the POMT complex is required for O-mannosylation of KIAA1549-BRAF and that O-mannosylation of KIAA1549-BRAF is necessary for oncogenic signaling. In Aim 3, I will test the hypothesis that the KIAA1549 portion of the KIAA1549-BRAF fusion tethers BRAF to the plasma membrane and enhances its ability to activate the MAPK pathway.
Awardee
Funding Goals
TO MAKE AVAILABLE SUPPORT TO NONPROFIT AND FOR-PROFIT INSTITUTIONS INTERESTED IN PROVIDING BIOMEDICAL TRAINING OPPORTUNITIES FOR INDIVIDUALS INTERESTED IN CAREERS IN BASIC, CLINICAL, AND PREVENTION RESEARCH IMPORTANT TO THE NATIONAL CANCER PROGRAM.
Grant Program (CFDA)
Awarding / Funding Agency
Place of Performance
Massachusetts
United States
Geographic Scope
State-Wide
The Broad Institute was awarded
Project Grant F32CA284834
worth $101,858
from National Cancer Institute in January 2024 with work to be completed primarily in Massachusetts United States.
The grant
has a duration of 1 year 1 months and
was awarded through assistance program 93.398 Cancer Research Manpower.
The Project Grant was awarded through grant opportunity Ruth L. Kirschstein National Research Service Award (NRSA) Individual Postdoctoral Fellowship (Parent F32).
Status
(Complete)
Last Modified 4/6/26
Period of Performance
1/15/24
Start Date
2/1/25
End Date
Funding Split
$101.9K
Federal Obligation
$0.0
Non-Federal Obligation
$101.9K
Total Obligated
Activity Timeline
Transaction History
Modifications to F32CA284834
Additional Detail
Award ID FAIN
F32CA284834
SAI Number
F32CA284834-456880415
Award ID URI
SAI UNAVAILABLE
Awardee Classifications
Nonprofit With 501(c)(3) IRS Status (Other Than An Institution Of Higher Education)
Awarding Office
75NC00 NIH National Cancer Institute
Funding Office
75NC00 NIH National Cancer Institute
Awardee UEI
H5G9NWEFHXN4
Awardee CAGE
5BP51
Performance District
MA-90
Senators
Edward Markey
Elizabeth Warren
Elizabeth Warren
Budget Funding
| Federal Account | Budget Subfunction | Object Class | Total | Percentage |
|---|---|---|---|---|
| National Cancer Institute, National Institutes of Health, Health and Human Services (075-0849) | Health research and training | Grants, subsidies, and contributions (41.0) | $71,792 | 100% |
Modified: 4/6/26