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Sex and tissue-specific differences in low-dose radiation-induced oncogenic signaling.

机译:低剂量辐射诱导的致癌信号中的性别和组织特异性差异。

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PURPOSE: The possible adverse health effects of low-dose radiation (LDR) exposure constitute a growing concern. Clinically and environmentally relevant exposures occur predominantly under chronic conditions, notwithstanding that most studies of LDR effects have been performed using a single acute exposure. Sex- and tissue-specificity of the LDR-induced changes have not been considered before. We investigated LDR-related expression patterns in muscle, liver and spleen of male and female mice subjected to acute and chronic LDR exposure. Genes involved in oncogenic signaling were of specific interest, as radiation is a well-known carcinogen. MATERIALS AND METHODS: We analyzed the expression pattern of genes coding for growth factors and growth-factor receptors, cytoplasmic serine/threonine protein kinases, G-proteins and nuclear DNA-binding proteins, and other important components of oncogenic signaling. RESULTS: We found sex- and tissue-specific changes in the expression of Ras superfamily members (Nras,Rab2, Rab34, Vav2), protein kinase C (PKC) isoforms (PKCbeta, PKCmu), AP-1 factor components (Jun, JunB and FosB), Wnt signaling pathway members as well as in a variety of other cellular proto-oncogenes and oncogenes. Importantly, Western blot analysis of JunB, PKCmu and Rab2 proteins supported the transcriptomic data. CONCLUSIONS: Substantially different protein levels were observed in all three tissues (muscle, spleen and liver) of acutely and chronically irradiated female and male animals. Based on the obtained data and available literature, we discuss several possible mechanisms that may contribute to radiation-induced carcinogenesis in various tissues of males and females. From our results we could identify the genes that may serve as sex- and tissue-specific biomarkers of the LDR exposure.
机译:目的:低剂量辐射(LDR)可能对健康造成的不利影响日益引起人们的关注。尽管大多数LDR效应研究都是使用单一急性暴露进行的,但临床和环境相关暴露主要发生在慢性条件下。以前从未考虑过LDR引起的变化的性别和组织特异性。我们调查了急性和慢性LDR暴露的雄性和雌性小鼠肌肉,肝脏和脾脏中与LDR相关的表达模式。由于放射线是众所周知的致癌物,因此涉及致癌信号的基因特别受关注。材料与方法:我们分析了编码生长因子和生长因子受体,胞质丝氨酸/苏氨酸蛋白激酶,G蛋白和核DNA结合蛋白以及致癌信号的其他重要成分的基因的表达模式。结果:我们发现性别和组织特定的表达变化的Ras超家族成员(Nras,Rab2,Rab34,Vav2),蛋白激酶C(PKC)同工型(PKCbeta,PKCmu),AP-1因子组成(Jun,JunB)和FosB),Wnt信号通路成员以及各种其他细胞原癌基因和致癌基因。重要的是,JunB,PKCmu和Rab2蛋白的蛋白质印迹分析支持了转录组数据。结论:在急性和慢性照射的雌性和雄性动物的所有三个组织(肌肉,脾脏和肝脏)中观察到的蛋白质水平基本不同。基于获得的数据和可用的文献,我们讨论了几种可能的机制,这些机制可能有助于男性和女性的各种组织中的辐射诱导的癌变。从我们的结果中,我们可以鉴定出可能作为LDR暴露的性别和组织特异性生物标志物的基因。

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