Age-related effects of X-ray irradiation on mouse hippocampus

Arianna Casciati; Katalin Dobos; Francesca Antonelli; Anett Benedek; Stefan J. Kempf; Montserrat Bellés; Andrea Balogh; Mirella Tanori; Luis Heredia; Michael J. Atkinson; Christine von Toerne; Omid Azimzadeh; Anna Saran; Geza Sáfrány; Mohammed A. Benotmane; M. Victoria Linares-Vidal; Soile Tapio; Katalin Lumniczky; Simonetta Pazzaglia

doi:10.18632/oncotarget.8575

Age-related effects of X-ray irradiation on mouse hippocampus

Arianna Casciati, Katalin Dobos, Francesca Antonelli, Anett Benedek, Stefan J. Kempf, Montserrat Bellés, Andrea Balogh, Mirella Tanori, Luis Heredia, Michael J. Atkinson, Christine von Toerne, Omid Azimzadeh, Anna Saran, Geza Sáfrány, Mohammed A. Benotmane, M. Victoria Linares-Vidal, Soile Tapio, Katalin Lumniczky, Simonetta Pazzaglia

Technical University of Munich

Research output: Contribution to journal › Article › peer-review

57 Scopus citations

Abstract

Therapeutic irradiation of pediatric and adult patients can profoundly affect adult neurogenesis, and cognitive impairment manifests as a deficit in hippocampal-dependent functions. Age plays a major role in susceptibility to radiation, and younger children are at higher risk of cognitive decay when compared to adults. Cranial irradiation affects hippocampal neurogenesis by induction of DNA damage in neural progenitors, through the disruption of the neurogenic microenvironment, and defective integration of newborn neurons into the neuronal network. Our goal here was to assess cellular and molecular alterations induced by cranial X-ray exposure to low/moderate doses (0.1 and 2 Gy) in the hippocampus of mice irradiated at the postnatal ages of day 10 or week 10, as well as the dependency of these phenomena on age at irradiation. To this aim, changes in the cellular composition of the dentate gyrus, mitochondrial functionality, proteomic profile in the hippocampus, as well as cognitive performance were evaluated by a multidisciplinary approach. Our results suggest the induction of specific alterations in hippocampal neurogenesis, microvascular density and mitochondrial functions, depending on age at irradiation. A better understanding of how irradiation impairs hippocampal neurogenesis at low and moderate doses is crucial to minimize adverse effects of therapeutic irradiation, contributing also to radiation safety regulations.

Original language	English
Pages (from-to)	28040-28058
Number of pages	19
Journal	Oncotarget
Volume	7
Issue number	19
DOIs	https://doi.org/10.18632/oncotarget.8575
State	Published - 10 May 2016

Keywords

Cognitive effects
Hippocampal neurogenesis
Mitochondria
Proteomics
Radiation

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10.18632/oncotarget.8575

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Casciati, A., Dobos, K., Antonelli, F., Benedek, A., Kempf, S. J., Bellés, M., Balogh, A., Tanori, M., Heredia, L., Atkinson, M. J., von Toerne, C., Azimzadeh, O., Saran, A., Sáfrány, G., Benotmane, M. A., Linares-Vidal, M. V., Tapio, S., Lumniczky, K., & Pazzaglia, S. (2016). Age-related effects of X-ray irradiation on mouse hippocampus. Oncotarget, 7(19), 28040-28058. https://doi.org/10.18632/oncotarget.8575

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title = "Age-related effects of X-ray irradiation on mouse hippocampus",

abstract = "Therapeutic irradiation of pediatric and adult patients can profoundly affect adult neurogenesis, and cognitive impairment manifests as a deficit in hippocampal-dependent functions. Age plays a major role in susceptibility to radiation, and younger children are at higher risk of cognitive decay when compared to adults. Cranial irradiation affects hippocampal neurogenesis by induction of DNA damage in neural progenitors, through the disruption of the neurogenic microenvironment, and defective integration of newborn neurons into the neuronal network. Our goal here was to assess cellular and molecular alterations induced by cranial X-ray exposure to low/moderate doses (0.1 and 2 Gy) in the hippocampus of mice irradiated at the postnatal ages of day 10 or week 10, as well as the dependency of these phenomena on age at irradiation. To this aim, changes in the cellular composition of the dentate gyrus, mitochondrial functionality, proteomic profile in the hippocampus, as well as cognitive performance were evaluated by a multidisciplinary approach. Our results suggest the induction of specific alterations in hippocampal neurogenesis, microvascular density and mitochondrial functions, depending on age at irradiation. A better understanding of how irradiation impairs hippocampal neurogenesis at low and moderate doses is crucial to minimize adverse effects of therapeutic irradiation, contributing also to radiation safety regulations.",

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author = "Arianna Casciati and Katalin Dobos and Francesca Antonelli and Anett Benedek and Kempf, {Stefan J.} and Montserrat Bell{\'e}s and Andrea Balogh and Mirella Tanori and Luis Heredia and Atkinson, {Michael J.} and {von Toerne}, Christine and Omid Azimzadeh and Anna Saran and Geza S{\'a}fr{\'a}ny and Benotmane, {Mohammed A.} and Linares-Vidal, {M. Victoria} and Soile Tapio and Katalin Lumniczky and Simonetta Pazzaglia",

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Casciati, A, Dobos, K, Antonelli, F, Benedek, A, Kempf, SJ, Bellés, M, Balogh, A, Tanori, M, Heredia, L, Atkinson, MJ, von Toerne, C, Azimzadeh, O, Saran, A, Sáfrány, G, Benotmane, MA, Linares-Vidal, MV, Tapio, S, Lumniczky, K & Pazzaglia, S 2016, 'Age-related effects of X-ray irradiation on mouse hippocampus', Oncotarget, vol. 7, no. 19, pp. 28040-28058. https://doi.org/10.18632/oncotarget.8575

TY - JOUR

T1 - Age-related effects of X-ray irradiation on mouse hippocampus

AU - Casciati, Arianna

AU - Dobos, Katalin

AU - Antonelli, Francesca

AU - Benedek, Anett

AU - Kempf, Stefan J.

AU - Bellés, Montserrat

AU - Balogh, Andrea

AU - Tanori, Mirella

AU - Heredia, Luis

AU - Atkinson, Michael J.

AU - von Toerne, Christine

AU - Azimzadeh, Omid

AU - Saran, Anna

AU - Sáfrány, Geza

AU - Benotmane, Mohammed A.

AU - Linares-Vidal, M. Victoria

AU - Tapio, Soile

AU - Lumniczky, Katalin

AU - Pazzaglia, Simonetta

PY - 2016/5/10

Y1 - 2016/5/10

N2 - Therapeutic irradiation of pediatric and adult patients can profoundly affect adult neurogenesis, and cognitive impairment manifests as a deficit in hippocampal-dependent functions. Age plays a major role in susceptibility to radiation, and younger children are at higher risk of cognitive decay when compared to adults. Cranial irradiation affects hippocampal neurogenesis by induction of DNA damage in neural progenitors, through the disruption of the neurogenic microenvironment, and defective integration of newborn neurons into the neuronal network. Our goal here was to assess cellular and molecular alterations induced by cranial X-ray exposure to low/moderate doses (0.1 and 2 Gy) in the hippocampus of mice irradiated at the postnatal ages of day 10 or week 10, as well as the dependency of these phenomena on age at irradiation. To this aim, changes in the cellular composition of the dentate gyrus, mitochondrial functionality, proteomic profile in the hippocampus, as well as cognitive performance were evaluated by a multidisciplinary approach. Our results suggest the induction of specific alterations in hippocampal neurogenesis, microvascular density and mitochondrial functions, depending on age at irradiation. A better understanding of how irradiation impairs hippocampal neurogenesis at low and moderate doses is crucial to minimize adverse effects of therapeutic irradiation, contributing also to radiation safety regulations.

AB - Therapeutic irradiation of pediatric and adult patients can profoundly affect adult neurogenesis, and cognitive impairment manifests as a deficit in hippocampal-dependent functions. Age plays a major role in susceptibility to radiation, and younger children are at higher risk of cognitive decay when compared to adults. Cranial irradiation affects hippocampal neurogenesis by induction of DNA damage in neural progenitors, through the disruption of the neurogenic microenvironment, and defective integration of newborn neurons into the neuronal network. Our goal here was to assess cellular and molecular alterations induced by cranial X-ray exposure to low/moderate doses (0.1 and 2 Gy) in the hippocampus of mice irradiated at the postnatal ages of day 10 or week 10, as well as the dependency of these phenomena on age at irradiation. To this aim, changes in the cellular composition of the dentate gyrus, mitochondrial functionality, proteomic profile in the hippocampus, as well as cognitive performance were evaluated by a multidisciplinary approach. Our results suggest the induction of specific alterations in hippocampal neurogenesis, microvascular density and mitochondrial functions, depending on age at irradiation. A better understanding of how irradiation impairs hippocampal neurogenesis at low and moderate doses is crucial to minimize adverse effects of therapeutic irradiation, contributing also to radiation safety regulations.

KW - Cognitive effects

KW - Hippocampal neurogenesis

KW - Mitochondria

KW - Proteomics

KW - Radiation

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DO - 10.18632/oncotarget.8575

M3 - Article

C2 - 27057631

AN - SCOPUS:84968784459

SN - 1949-2553

VL - 7

SP - 28040

EP - 28058

JO - Oncotarget

JF - Oncotarget

IS - 19

ER -

Age-related effects of X-ray irradiation on mouse hippocampus

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Keywords

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