Radiotherapy-Induced Neurocognitive Impairment Is Driven by Heightened Apoptotic Priming in Early Life and Prevented by Blocking BAX

Although external beam radiotherapy (xRT) is commonly used to treat central nervous system (CNS) tumors in patients of all ages, young children treated with xRT frequently experience life-altering and dose-limiting neurocognitive impairment (NI) while adults do not. The lack of understanding of mech...

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Autores principales: Singh, Rumani, Yu, Stacey, Osman, Marwa, Inde, Zintis, Fraser, Cameron, Cleveland, Abigail H., Almanzar, Nicole, Lim, Chuan Bian, Joshi, Gaurav N., Spetz, Johan, Qin, Xingping, Toprani, Sneh M., Nagel, Zachary, Hocking, Matthew C., Cormack, Robert A., Yock, Torunn I., Miller, Jeffrey W., Yuan, Zhi-Min, Gershon, Timothy, Sarosiek, Kristopher A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Association for Cancer Research 2023
Materias:
Translational Cancer Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10570680/
https://www.ncbi.nlm.nih.gov/pubmed/37470810
http://dx.doi.org/10.1158/0008-5472.CAN-22-1337
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author Singh, Rumani
Yu, Stacey
Osman, Marwa
Inde, Zintis
Fraser, Cameron
Cleveland, Abigail H.
Almanzar, Nicole
Lim, Chuan Bian
Joshi, Gaurav N.
Spetz, Johan
Qin, Xingping
Toprani, Sneh M.
Nagel, Zachary
Hocking, Matthew C.
Cormack, Robert A.
Yock, Torunn I.
Miller, Jeffrey W.
Yuan, Zhi-Min
Gershon, Timothy
Sarosiek, Kristopher A.
author_facet Singh, Rumani
Yu, Stacey
Osman, Marwa
Inde, Zintis
Fraser, Cameron
Cleveland, Abigail H.
Almanzar, Nicole
Lim, Chuan Bian
Joshi, Gaurav N.
Spetz, Johan
Qin, Xingping
Toprani, Sneh M.
Nagel, Zachary
Hocking, Matthew C.
Cormack, Robert A.
Yock, Torunn I.
Miller, Jeffrey W.
Yuan, Zhi-Min
Gershon, Timothy
Sarosiek, Kristopher A.
author_sort Singh, Rumani
collection PubMed
description Although external beam radiotherapy (xRT) is commonly used to treat central nervous system (CNS) tumors in patients of all ages, young children treated with xRT frequently experience life-altering and dose-limiting neurocognitive impairment (NI) while adults do not. The lack of understanding of mechanisms responsible for these differences has impeded the development of neuroprotective treatments. Using a newly developed mouse model of xRT-induced NI, we found that neurocognitive function is impaired by ionizing radiation in a dose- and age-dependent manner, with the youngest animals being most affected. Histologic analysis revealed xRT-driven neuronal degeneration and cell death in neurogenic brain regions in young animals but not adults. BH3 profiling showed that neural stem and progenitor cells, neurons, and astrocytes in young mice are highly primed for apoptosis, rendering them hypersensitive to genotoxic damage. Analysis of single-cell RNA sequencing data revealed that neural cell vulnerability stems from heightened expression of proapoptotic genes including BAX, which is associated with developmental and mitogenic signaling by MYC. xRT induced apoptosis in primed neural cells by triggering a p53- and PUMA-initiated, proapoptotic feedback loop requiring cleavage of BID and culminating in BAX oligomerization and caspase activation. Notably, loss of BAX protected against apoptosis induced by proapoptotic signaling in vitro and prevented xRT-induced apoptosis in neural cells in vivo as well as neurocognitive sequelae. On the basis of these findings, preventing xRT-induced apoptosis specifically in immature neural cells by blocking BAX, BIM, or BID via direct or upstream mechanisms is expected to ameliorate NI in pediatric patients with CNS tumor. SIGNIFICANCE: Age- and differentiation-dependent apoptotic priming plays a pivotal role in driving radiotherapy-induced neurocognitive impairment and can be targeted for neuroprotection in pediatric patients.
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spelling pubmed-105706802023-10-14 Radiotherapy-Induced Neurocognitive Impairment Is Driven by Heightened Apoptotic Priming in Early Life and Prevented by Blocking BAX Singh, Rumani Yu, Stacey Osman, Marwa Inde, Zintis Fraser, Cameron Cleveland, Abigail H. Almanzar, Nicole Lim, Chuan Bian Joshi, Gaurav N. Spetz, Johan Qin, Xingping Toprani, Sneh M. Nagel, Zachary Hocking, Matthew C. Cormack, Robert A. Yock, Torunn I. Miller, Jeffrey W. Yuan, Zhi-Min Gershon, Timothy Sarosiek, Kristopher A. Cancer Res Translational Cancer Biology Although external beam radiotherapy (xRT) is commonly used to treat central nervous system (CNS) tumors in patients of all ages, young children treated with xRT frequently experience life-altering and dose-limiting neurocognitive impairment (NI) while adults do not. The lack of understanding of mechanisms responsible for these differences has impeded the development of neuroprotective treatments. Using a newly developed mouse model of xRT-induced NI, we found that neurocognitive function is impaired by ionizing radiation in a dose- and age-dependent manner, with the youngest animals being most affected. Histologic analysis revealed xRT-driven neuronal degeneration and cell death in neurogenic brain regions in young animals but not adults. BH3 profiling showed that neural stem and progenitor cells, neurons, and astrocytes in young mice are highly primed for apoptosis, rendering them hypersensitive to genotoxic damage. Analysis of single-cell RNA sequencing data revealed that neural cell vulnerability stems from heightened expression of proapoptotic genes including BAX, which is associated with developmental and mitogenic signaling by MYC. xRT induced apoptosis in primed neural cells by triggering a p53- and PUMA-initiated, proapoptotic feedback loop requiring cleavage of BID and culminating in BAX oligomerization and caspase activation. Notably, loss of BAX protected against apoptosis induced by proapoptotic signaling in vitro and prevented xRT-induced apoptosis in neural cells in vivo as well as neurocognitive sequelae. On the basis of these findings, preventing xRT-induced apoptosis specifically in immature neural cells by blocking BAX, BIM, or BID via direct or upstream mechanisms is expected to ameliorate NI in pediatric patients with CNS tumor. SIGNIFICANCE: Age- and differentiation-dependent apoptotic priming plays a pivotal role in driving radiotherapy-induced neurocognitive impairment and can be targeted for neuroprotection in pediatric patients. American Association for Cancer Research 2023-10-13 2023-07-20 /pmc/articles/PMC10570680/ /pubmed/37470810 http://dx.doi.org/10.1158/0008-5472.CAN-22-1337 Text en ©2023 The Authors; Published by the American Association for Cancer Research https://creativecommons.org/licenses/by-nc-nd/4.0/This open access article is distributed under the Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0) license.
spellingShingle Translational Cancer Biology
Singh, Rumani
Yu, Stacey
Osman, Marwa
Inde, Zintis
Fraser, Cameron
Cleveland, Abigail H.
Almanzar, Nicole
Lim, Chuan Bian
Joshi, Gaurav N.
Spetz, Johan
Qin, Xingping
Toprani, Sneh M.
Nagel, Zachary
Hocking, Matthew C.
Cormack, Robert A.
Yock, Torunn I.
Miller, Jeffrey W.
Yuan, Zhi-Min
Gershon, Timothy
Sarosiek, Kristopher A.
Radiotherapy-Induced Neurocognitive Impairment Is Driven by Heightened Apoptotic Priming in Early Life and Prevented by Blocking BAX
title Radiotherapy-Induced Neurocognitive Impairment Is Driven by Heightened Apoptotic Priming in Early Life and Prevented by Blocking BAX
title_full Radiotherapy-Induced Neurocognitive Impairment Is Driven by Heightened Apoptotic Priming in Early Life and Prevented by Blocking BAX
title_fullStr Radiotherapy-Induced Neurocognitive Impairment Is Driven by Heightened Apoptotic Priming in Early Life and Prevented by Blocking BAX
title_full_unstemmed Radiotherapy-Induced Neurocognitive Impairment Is Driven by Heightened Apoptotic Priming in Early Life and Prevented by Blocking BAX
title_short Radiotherapy-Induced Neurocognitive Impairment Is Driven by Heightened Apoptotic Priming in Early Life and Prevented by Blocking BAX
title_sort radiotherapy-induced neurocognitive impairment is driven by heightened apoptotic priming in early life and prevented by blocking bax
topic Translational Cancer Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10570680/
https://www.ncbi.nlm.nih.gov/pubmed/37470810
http://dx.doi.org/10.1158/0008-5472.CAN-22-1337
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