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硫酸锌对酵母细胞的毒性作用 被引量:2
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作者 吴丽华 陈燕飞 +3 位作者 仪慧兰 张国栋 关慧婷 唐颂 《西北农林科技大学学报(自然科学版)》 CSCD 北大核心 2020年第2期129-136,共8页
【目的】研究硫酸锌对酵母细胞的毒性作用,为揭示高浓度锌的毒性作用机理提供依据。【方法】以模式生物酵母细胞为材料,在YPD培养基中添加终浓度为0,0.5,1,3,5和10 mmol/L的硫酸锌进行毒性试验。缓解组为抗氧化剂AsA、NO清除剂c-PTIO和C... 【目的】研究硫酸锌对酵母细胞的毒性作用,为揭示高浓度锌的毒性作用机理提供依据。【方法】以模式生物酵母细胞为材料,在YPD培养基中添加终浓度为0,0.5,1,3,5和10 mmol/L的硫酸锌进行毒性试验。缓解组为抗氧化剂AsA、NO清除剂c-PTIO和Ca^2+螯合剂EGTA分别与0.5或5 mmol/L硫酸锌同时作用。培养一定时间后,采用分光光度法、美蓝染色法和流式细胞术,研究硫酸锌对酵母细胞生长、细胞死亡率及胞内ROS、NO和Ca^2+水平的影响。【结果】低浓度硫酸锌(0.5 mmol/L)促进酵母细胞生长,而高浓度硫酸锌(1~10 mmol/L)抑制酵母细胞生长,诱导细胞死亡,且细胞死亡率随着硫酸锌浓度升高和胁迫时间延长而逐渐升高。酵母细胞经5 mmol/L硫酸锌胁迫12或24 h后,胞内ROS、NO和Ca^2+水平均显著高于对照组;但加入对应抗氧化剂AsA、NO清除剂c-PTIO和Ca^2+螯合剂EGTA后,酵母细胞死亡率均显著低于硫酸锌单独处理组。【结论】高浓度硫酸锌可诱导酵母细胞死亡,在此过程中ROS、NO和Ca^2+水平显著提高,从而造成毒性。 展开更多
关键词 硫酸锌 酵母细胞 毒性机理 细胞死亡
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钢纤维掺量对碱矿渣混凝土力学性能的影响 被引量:2
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作者 袁晓辉 石艳羽 +3 位作者 陈宜新 关慧亭 芦峰 陈秀云 《信阳师范学院学报(自然科学版)》 CAS 北大核心 2023年第4期656-662,共7页
为研究钢纤维掺量对碱矿渣混凝土力学性能的影响规律,制作钢纤维碱矿渣混凝土抗压力学性能试验试件共计54个,进行立方体抗压强度、棱柱体抗压强度、弹性模量和泊松比试验研究,并对试件内部微裂缝进行定性和定量分析,揭示钢纤维对碱矿渣... 为研究钢纤维掺量对碱矿渣混凝土力学性能的影响规律,制作钢纤维碱矿渣混凝土抗压力学性能试验试件共计54个,进行立方体抗压强度、棱柱体抗压强度、弹性模量和泊松比试验研究,并对试件内部微裂缝进行定性和定量分析,揭示钢纤维对碱矿渣混凝土的增强增韧机理。结果显示:与钢纤维掺量有关的立方体抗压强度修正公式理论计算值与试验结果吻合良好;一定范围内的钢纤维掺量对该材料的强度、弹性模量和泊松比均有提高作用,过大的掺量会造成混凝土材料内部发生结团现象,界面过渡区增多,降低其力学性能;碱矿渣混凝土配合比下的最佳钢纤维掺量为1.4%。 展开更多
关键词 钢纤维碱矿渣混凝土 钢纤维掺量 抗压力学性能 最佳掺量
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Effects of Jiazhu decoction in combination with cyclophosphamide on breast cancer in mice 被引量:4
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作者 guan huiting Xie Su +6 位作者 Liu Shangyi Xie Qing Hou Shengkai Liu Huarong Zhang Yunjie Hu Yaqing Zhang Chenyu 《Journal of Traditional Chinese Medicine》 SCIE CAS CSCD 2019年第5期642-648,共7页
OBJECTIVE: To investigate the therapeutic effects of Jiazhu decoction (JZD) in combination with cyclophosphamide (CTX) on the growth of breast cancer in mice and to explore the possible molecular mechanisms of action.... OBJECTIVE: To investigate the therapeutic effects of Jiazhu decoction (JZD) in combination with cyclophosphamide (CTX) on the growth of breast cancer in mice and to explore the possible molecular mechanisms of action. METHODS: BALB/c mice were randomly divided into four groups of 10 (untreated model group, JZD group, CTX group, and JZD + CTX group) and subcutaneously injected with 4T1 mouse breast cancer cells. Tumors were allowed to establish for ~7 d before initiation of treatment with CTX (100 mg/kg every week by intraperitoneal injection) and/or JZD (0.015 mL of 1.65 g/mL crude drug, administered daily by gavage). The model group received equivalent volumes of vehicle on the same schedules. Tumor volumes were measured every 3 d. Mice were sacrificed after 3 weeks of treatment, and tumors were excised and subjected to RT-qPCR and western blot analysis to evaluate expression of the Wnt/β-catenin signaling pathway components β-catenin, c-Myc, and cyclin D1 at the mRNA and protein levels. RESULTS: The mean tumor volume was smaller and the growth rate was slower in the CTX and JZD + CTX groups compared with the model group (P < 0.05), and in the JZD + CTX group compared with the CTX and JZD groups (P < 0.05). Tumor growth was inhibited by 35.4% and 48.1% by CTX and JZD + CTX treatment, respectively (P < 0.001). The expression of β-catenin, c-Myc, and cyclin D1 mRNA and protein in tumors was significantly lower in mice treated with JZD or JZD + CTX compared with the untreated mice (P < 0.05), and was significantly lower in mice treated with JZD + CTX compared with either JZD or CTX alone (P < 0.05). CONCLUSION: JZD inhibited the growth of mouse breast cancer cells in vivo, possibly by reducing the expression of β-catenin, c-Myc, and cyclin D1. Combination therapy with JZD plus CTX had a more potent inhibitory effect on breast cancer growth compared with either agent alone. 展开更多
关键词 BREAST NEOPLASMS CYCLOPHOSPHAMIDE WNT signaling pathway Jiazhu DECOCTION
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