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X射线照射对小鼠海马体的年龄相关影响。

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

作者信息

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

机构信息

Laboratory of Biomedical Technologies, Agenzia Nazionale per le Nuove Tecnologie, l'Energia e lo Sviluppo Economico Sostenibile (ENEA), Rome, Italy.

National Public Health Center - National Research Directorate for Radiobiology and Radiohygiene, Budapest, Hungary.

出版信息

Oncotarget. 2016 May 10;7(19):28040-58. doi: 10.18632/oncotarget.8575.

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.

摘要

对儿科和成年患者进行治疗性放疗会深刻影响成年神经发生,认知障碍表现为海马体依赖功能的缺陷。年龄在辐射易感性中起主要作用,与成年人相比,年幼儿童认知衰退的风险更高。颅脑照射通过诱导神经祖细胞中的DNA损伤、破坏神经发生微环境以及新生神经元融入神经网络存在缺陷等方式,影响海马体神经发生。我们的目标是评估在出生后第10天或第10周接受低/中剂量(0.1和2 Gy)颅脑X射线照射的小鼠海马体中,由照射诱导的细胞和分子变化,以及这些现象对照射时年龄的依赖性。为此,我们采用多学科方法评估了齿状回的细胞组成、线粒体功能、海马体中的蛋白质组学特征以及认知表现。我们的结果表明,根据照射时的年龄不同,海马体神经发生、微血管密度和线粒体功能会出现特定改变。更好地理解低剂量和中等剂量照射如何损害海马体神经发生,对于将治疗性放疗的不良影响降至最低至关重要,这也有助于辐射安全法规的制定。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dcd2/5053708/2465d47989ae/oncotarget-07-28040-g001.jpg

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