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BIOL-20. BIOPROCESSING OF SURGICAL PEDIATRIC BRAIN TUMOR SPECIMENS FOR GENOME-GUIDED PERSONALIZED DRUG TESTING

Novel treatment approaches are urgently needed for pediatric central nervous system (CNS) tumors as they are the leading cause of cancer-related deaths in children. A lack of research materials impedes progress towards developing such therapies. Although various brain cancer biobanks exist, these ra...

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Autores principales: Nasajpour, Emon, Tran, Caitlynn, Garcia, Cesar, Lyle, Geoff, Guinle, Maria I Barros, Bagley, Bryce A, Lancero, Hope, Gibson, Eden E, Schouten, Troy, Mahaney, Kelly, Vogel, Hannes, Learned, Katrina, Vaske, Olena, Grant, Gerald A, Prolo, Laura M, Petritsch, Claudia K
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10260044/
http://dx.doi.org/10.1093/neuonc/noad073.039
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author Nasajpour, Emon
Tran, Caitlynn
Garcia, Cesar
Lyle, Geoff
Guinle, Maria I Barros
Bagley, Bryce A
Lancero, Hope
Gibson, Eden E
Schouten, Troy
Mahaney, Kelly
Vogel, Hannes
Learned, Katrina
Vaske, Olena
Grant, Gerald A
Prolo, Laura M
Petritsch, Claudia K
author_facet Nasajpour, Emon
Tran, Caitlynn
Garcia, Cesar
Lyle, Geoff
Guinle, Maria I Barros
Bagley, Bryce A
Lancero, Hope
Gibson, Eden E
Schouten, Troy
Mahaney, Kelly
Vogel, Hannes
Learned, Katrina
Vaske, Olena
Grant, Gerald A
Prolo, Laura M
Petritsch, Claudia K
author_sort Nasajpour, Emon
collection PubMed
description Novel treatment approaches are urgently needed for pediatric central nervous system (CNS) tumors as they are the leading cause of cancer-related deaths in children. A lack of research materials impedes progress towards developing such therapies. Although various brain cancer biobanks exist, these rarely store viable patient-derived tissue and cells for live cell analyses, including cell fate assays and testing for drug sensitivities. We propose that a biorepository of viable cell dissociates and tissue broadly representing CNS tumor entities overcomes these limitations. From a combination of molecular diagnoses and histopathologic assessment of over 90 samples collected, we generated a biorepository of roughly 35 distinct entities of pediatric CNS tumors in our Stanford neuro-bioprocessing cohort. Based on the Central Brain Tumor Registry of the United States, the proportion of subtypes represented in our cohort match that of the general population with exceptions. We established a standardized bioprocessing pipeline that can be used as a template for tissue collection and model development in the broader disease context and for multiple downstream applications. Our emphasis on cryostorage of viable cells and tissue facilitates ad hoc live cell analyses. In addition to gaining a better understanding of tumor pathophysiology, we attempted a rapid bed-to-bench-to-bedside approach using comparative RNA expression profile analyses in an individual patient’s pilocytic astrocytoma. Novel drug targets were identified by analyzing RNA transcripts that are highly expressed (outliers) compared with a compendium of 12,747 brain and non-brain tumor samples. We validated outliers as drug targets using acute cell isolates, and identified a novel target in recurrent low-grade glioma. These studies illustrate that biobanking of viable patient-derived material enables developing personalized therapies with the goal of improving patient outcomes. As demonstrated here, patient-derived acute cell isolates facilitate identifying drug vulnerability, creating an opportunity for more personalized treatment of patients with CNS tumors.
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spelling pubmed-102600442023-06-13 BIOL-20. BIOPROCESSING OF SURGICAL PEDIATRIC BRAIN TUMOR SPECIMENS FOR GENOME-GUIDED PERSONALIZED DRUG TESTING Nasajpour, Emon Tran, Caitlynn Garcia, Cesar Lyle, Geoff Guinle, Maria I Barros Bagley, Bryce A Lancero, Hope Gibson, Eden E Schouten, Troy Mahaney, Kelly Vogel, Hannes Learned, Katrina Vaske, Olena Grant, Gerald A Prolo, Laura M Petritsch, Claudia K Neuro Oncol Final Category: Basic Biology/Stem Cells/Models - BIOL Novel treatment approaches are urgently needed for pediatric central nervous system (CNS) tumors as they are the leading cause of cancer-related deaths in children. A lack of research materials impedes progress towards developing such therapies. Although various brain cancer biobanks exist, these rarely store viable patient-derived tissue and cells for live cell analyses, including cell fate assays and testing for drug sensitivities. We propose that a biorepository of viable cell dissociates and tissue broadly representing CNS tumor entities overcomes these limitations. From a combination of molecular diagnoses and histopathologic assessment of over 90 samples collected, we generated a biorepository of roughly 35 distinct entities of pediatric CNS tumors in our Stanford neuro-bioprocessing cohort. Based on the Central Brain Tumor Registry of the United States, the proportion of subtypes represented in our cohort match that of the general population with exceptions. We established a standardized bioprocessing pipeline that can be used as a template for tissue collection and model development in the broader disease context and for multiple downstream applications. Our emphasis on cryostorage of viable cells and tissue facilitates ad hoc live cell analyses. In addition to gaining a better understanding of tumor pathophysiology, we attempted a rapid bed-to-bench-to-bedside approach using comparative RNA expression profile analyses in an individual patient’s pilocytic astrocytoma. Novel drug targets were identified by analyzing RNA transcripts that are highly expressed (outliers) compared with a compendium of 12,747 brain and non-brain tumor samples. We validated outliers as drug targets using acute cell isolates, and identified a novel target in recurrent low-grade glioma. These studies illustrate that biobanking of viable patient-derived material enables developing personalized therapies with the goal of improving patient outcomes. As demonstrated here, patient-derived acute cell isolates facilitate identifying drug vulnerability, creating an opportunity for more personalized treatment of patients with CNS tumors. Oxford University Press 2023-06-12 /pmc/articles/PMC10260044/ http://dx.doi.org/10.1093/neuonc/noad073.039 Text en © The Author(s) 2023. Published by Oxford University Press on behalf of the Society for Neuro-Oncology. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Final Category: Basic Biology/Stem Cells/Models - BIOL
Nasajpour, Emon
Tran, Caitlynn
Garcia, Cesar
Lyle, Geoff
Guinle, Maria I Barros
Bagley, Bryce A
Lancero, Hope
Gibson, Eden E
Schouten, Troy
Mahaney, Kelly
Vogel, Hannes
Learned, Katrina
Vaske, Olena
Grant, Gerald A
Prolo, Laura M
Petritsch, Claudia K
BIOL-20. BIOPROCESSING OF SURGICAL PEDIATRIC BRAIN TUMOR SPECIMENS FOR GENOME-GUIDED PERSONALIZED DRUG TESTING
title BIOL-20. BIOPROCESSING OF SURGICAL PEDIATRIC BRAIN TUMOR SPECIMENS FOR GENOME-GUIDED PERSONALIZED DRUG TESTING
title_full BIOL-20. BIOPROCESSING OF SURGICAL PEDIATRIC BRAIN TUMOR SPECIMENS FOR GENOME-GUIDED PERSONALIZED DRUG TESTING
title_fullStr BIOL-20. BIOPROCESSING OF SURGICAL PEDIATRIC BRAIN TUMOR SPECIMENS FOR GENOME-GUIDED PERSONALIZED DRUG TESTING
title_full_unstemmed BIOL-20. BIOPROCESSING OF SURGICAL PEDIATRIC BRAIN TUMOR SPECIMENS FOR GENOME-GUIDED PERSONALIZED DRUG TESTING
title_short BIOL-20. BIOPROCESSING OF SURGICAL PEDIATRIC BRAIN TUMOR SPECIMENS FOR GENOME-GUIDED PERSONALIZED DRUG TESTING
title_sort biol-20. bioprocessing of surgical pediatric brain tumor specimens for genome-guided personalized drug testing
topic Final Category: Basic Biology/Stem Cells/Models - BIOL
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10260044/
http://dx.doi.org/10.1093/neuonc/noad073.039
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