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性别差异是否会影响放射性肺毒性?遗传和组织病理学预测因子的实验研究。

Does Gender Difference Effect Radiation-Induced Lung Toxicity? An Experimental Study by Genetic and Histopathological Predictors.

机构信息

Trakya University Faculty of Medicine, Department of Radiation Oncology, Edirne, Turkey.

Eskisehir Osmangazi University Faculty of Medicine, Department of Radiation Oncology, Eskisehir, Turkey.

出版信息

Radiat Res. 2022 Mar 1;197(3):280-288. doi: 10.1667/RADE-21-00075.1.

Abstract

Several studies have reported differences in radiation toxicity between the sexes, but these differences have not been tested with respect to histopathology and genes. This animal study aimed to show an association between histopathological findings of radiation-induced lung toxicity and the genes ATM, SOD2, TGF-β1, XRCC1, XRCC3 and HHR2. In all, 120 animals were randomly divided into 2 control groups (male and female) and experimental groups comprising fifteen rats stratified by sex, radiotherapy (0 Gy vs. 10 Gy), and time to sacrifice (6, 12, and 24 weeks postirradiation). Histopathological evaluations for lung injury, namely, intra-alveolar edema, alveolar neutrophils, intra-alveolar erythrocytes, activated macrophages, intra-alveolar fibrosis, hyaline arteriosclerosis, and collapse were performed under a light microscope using a grid system; the evaluations were semi quantitatively scored. Then, the alveolar wall thickness was measured. Real-time quantitative reverse transcription PCR (RT-qPCR) was used to determine gene expression differences in ATM, TGF-β1, XRCC1, XRCC3, SOD2 and HHR2L among the groups. Histopathological data showed that radiation-induced acute, subacute, and chronic lung toxicity were worse in male rats. The expression levels of the evaluated genes were significantly higher in females than males in the control group, but this difference was lost over time after radiotherapy. Less toxicity in females may be attributable to the fact that the expression of the evaluated genes was higher in normal lung tissue in females than in males and the changes in gene expression patterns in the postradiotherapy period played a protective role in females. Additional data related to pulmonary function, lung weights, imaging, or outcomes are needed to support this data that is based on histopathology alone.

摘要

几项研究报告了性别之间辐射毒性的差异,但这些差异尚未在组织病理学和基因方面得到验证。本动物研究旨在展示放射性肺毒性的组织病理学发现与 ATM、SOD2、TGF-β1、XRCC1、XRCC3 和 HHR2 基因之间的关联。总共 120 只动物被随机分为 2 个对照组(雄性和雌性)和实验组,实验组由 15 只大鼠组成,按性别、放疗(0 Gy 与 10 Gy)和放疗后牺牲时间(6、12 和 24 周)分层。使用网格系统在光镜下对肺损伤的组织病理学评估,即肺泡内水肿、肺泡中性粒细胞、肺泡内红细胞、活化的巨噬细胞、肺泡内纤维化、玻璃样动脉粥样硬化和塌陷进行评估;评估结果进行半定量评分。然后测量肺泡壁厚度。使用实时定量逆转录 PCR(RT-qPCR)确定各组中 ATM、TGF-β1、XRCC1、XRCC3、SOD2 和 HHR2L 基因表达的差异。组织病理学数据显示,雄性大鼠的放射性急性、亚急性和慢性肺毒性更严重。在对照组中,雌性的基因表达水平明显高于雄性,但在放疗后,这种差异随着时间的推移而消失。雌性的毒性较低可能归因于以下事实:在雌性的正常肺组织中,评估基因的表达高于雄性,并且放疗后基因表达模式的变化在雌性中起保护作用。需要与肺功能、肺重、影像学或结果相关的其他数据来支持仅基于组织病理学的这一数据。

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