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抗抑郁药对非小细胞肺癌术后抑郁患者认知功能和睡眠质量影响
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作者 魏桂莲 张泽丽 +3 位作者 温占红 崔彩云 侯占鑫 纪志远 《山西大同大学学报(自然科学版)》 2023年第2期64-66,共3页
目的评估抗抑郁药物治疗对非小细胞肺癌术后抑郁患者认知功能和睡眠质量影响。方法将60例非小细胞肺癌术后抑郁患者随机分为对照组、度洛西汀组和舒肝解郁胶囊组,每组20例。对照组术后给予常规干预,度洛西汀组和舒肝解郁胶囊组在对照组... 目的评估抗抑郁药物治疗对非小细胞肺癌术后抑郁患者认知功能和睡眠质量影响。方法将60例非小细胞肺癌术后抑郁患者随机分为对照组、度洛西汀组和舒肝解郁胶囊组,每组20例。对照组术后给予常规干预,度洛西汀组和舒肝解郁胶囊组在对照组干预基础上加用度洛西汀或舒肝解郁胶囊治疗。分别于术前及术后1、3、6和12月,采用汉密尔顿抑郁量表(HAMD)、简易智能状态检查量表(MMSE)和匹兹堡睡眠指数量表(PSQI)对患者进行评估。结果与对照组相比,治疗后1、3和6月度洛西汀组和舒肝解郁胶囊组患者HADM评分降低(所有P<0.05);度洛西汀和舒肝解郁胶囊治疗非小细胞肺癌术后1、3和6月MMSE评分高于对照组,PSQI评分低于对照组(所有P<0.05)。结论度洛西汀或舒肝解郁胶囊治疗均可有效改善非小细胞肺癌术后抑郁患者认知障碍和睡眠障碍。 展开更多
关键词 肺癌 抑郁 度洛西汀 舒肝解郁胶囊
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气流和外加磁场对负电晕放电特性的影响
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作者 张泽力 孙树伟 +1 位作者 陈佳尧 钟方川 《核聚变与等离子体物理》 CAS CSCD 北大核心 2023年第4期477-481,共5页
利用线-筒电晕放电装置,研究了气体流动和外加磁场对负电晕放电的影响。当电压固定时,电晕放电电流随气体流量的增加先快速增大,并到达一个高点后迅速下降,随着流量的进一步上升,放电电流又开始缓慢增加。外加磁场能增加电晕放电的电流... 利用线-筒电晕放电装置,研究了气体流动和外加磁场对负电晕放电的影响。当电压固定时,电晕放电电流随气体流量的增加先快速增大,并到达一个高点后迅速下降,随着流量的进一步上升,放电电流又开始缓慢增加。外加磁场能增加电晕放电的电流,但在高的气体流速下,磁场将降低电晕放电的电流,同时外加磁场增加臭氧的产生,直到温度上升导致它的快速降解。 展开更多
关键词 负电晕 气体流速 磁场 放电电流 臭氧
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基于转录组学数据对肝细胞癌的研究 被引量:1
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作者 杨庆芳 彭彦 +2 位作者 郭飞 张泽立 杨庆霞 《浙江中西医结合杂志》 2021年第4期324-328,共5页
目的通过对肝细胞癌的转录组学数据进行分析,为肝细胞癌分子机制研究提供新的证据和思路。方法基于转录组学的肝细胞癌数据,通过t-检验和差异倍数筛选差异表达基因。应用差异表达基因进行基因本体学和信号通路的富集分析,以揭示肝细胞... 目的通过对肝细胞癌的转录组学数据进行分析,为肝细胞癌分子机制研究提供新的证据和思路。方法基于转录组学的肝细胞癌数据,通过t-检验和差异倍数筛选差异表达基因。应用差异表达基因进行基因本体学和信号通路的富集分析,以揭示肝细胞癌发生发展过程中所参与的生物过程及信号通路。结果通过差异表达基因的筛选,共鉴定出486个差异表达基因(其中包括157个上调基因和329个下调基因)。经基因本体学分析和KEGG富集分析,发现肝细胞癌的发病机制主要集中在细胞周期、细胞分裂等生物功能和视黄醇代谢、药物代谢-细胞色素P450、p53等信号通路。结论本研究对探索肝细胞癌的分子标记物和发生发展机制等研究提供了重要的参考信息。 展开更多
关键词 肝细胞癌 转录组 高通量测序 信号通路
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Sleep-related hypoxemia aggravates systematic inflammation in emphysematous rats 被引量:15
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作者 FENG Jing Ambrose An-Po Chiang +5 位作者 WU Qi CHEN Bao-yuan CUI Lin-yang LIANG Dong-chun zhang ze-li YAO Wo 《Chinese Medical Journal》 SCIE CAS CSCD 2010年第17期2392-2399,共8页
Background Sleep disturbance is common in patients with emphysema. This study aimed to develop a novel model of sleep-related hypoxemia (SRH) in emphysema (SRHIE) with rats, and to explore the inflammatory status ... Background Sleep disturbance is common in patients with emphysema. This study aimed to develop a novel model of sleep-related hypoxemia (SRH) in emphysema (SRHIE) with rats, and to explore the inflammatory status of SRHIE in lung, liver, pancreas, carotid artery and whole blood.Methods Seventy-five male Wistar rats were assigned to 5 groups with 15 per group according to the exposure conditions. The protocols varied with the degree of hypoxia exposure and severity of pre-existing emphysema caused by cigarette smoke exposure: (1) SRH control (SRHCtrl) group, sham smoke exposure (smoke exposure, exposed to smoke of 15 cigarettes twice everyday, 16 weeks) and SRH exposure (12.5% O2, 3 hours, SRH exposure, divide total hypoxia time (1.5 hours or 3 hours) into 4 periods evenly (22.5 minutes or 45 minutes) and distribute these hypoxia periods evenly into physiological sleep time of rats identified by electroencephalogram, week 9 to week 16); (2) Emphysema control (ECtrl) group, smoke exposure and sham SRH exposure (21% O2, 3 hours); (3) Short SRH in emphysema (SRHShort) group, smoke exposure and short SRH exposure (12.5% O2, 1.5 hours); (4) Mild SRH in emphysema (SRHMild) group,smoke exposure and mild SRH exposure (15% O2, 3 hours); (5) Standard SRH in emphysema (SRHStand) group, smoke exposure and SRH exposure (12.5% O2, 3 hours). ECtrl, SRHShort, SRHMild and SRHStand groups were groups with emphysematous rats. Two days before the end of exposure, 5 rats in each group were randomly selected for arterial blood gas analysis. In the rest 10 rats in each group, we obtained blood samples and bronchoalveolar lavage fluid (BALF)for routine tests. We also obtained tissue blocks of lung, liver, pancreas, and right carotid artery for pathologic scoring and measurements of liver oxidative stress (measuring hepatic oxidative stress enzymes, superoxide dismutase (SOD) activity, catalase (CAT) activity and malondialdehyde (MDA) concentration).Results Emphysematous groups had higher mean linear intercept (MLI) and mean alveolar number (MAN) values than SRHCtrl group. MLI values in SRHStand group were the highest (ail P 〈0.05). O2Sat in SRHStand rats when SRH exposure was (83.45±1.76)%. Histological scores of lung, liver, pancreas and right carotid artery were higher in emphysematous groups than SRHCtrl group, and SRHStand group were the highest (all P 〈0.05) (SOD and CAT values were lower and MDA values were higher in groups with emphysema than without and in SRHStand group than in ECtrl group (all P 〈0.05)). MDA values were the highest in SRHStand group (all P 〈0.05). Total cellular score in BALF and White blood cell (WBC) in whole blood were the highest in SRHStand group (all P 〈0.05). Lymphocyte ratios were the highest in SRHStand group both in BALF and blood (all P 〈0.05). Red blood cell (RBC) and hemoglobin in emphysematous groups were higher than that in SRHCtrl group, and SRHStand group were higher than ECtrl group (all P 〈0.05).Conclusions With a proper novo model of SRHIE with Wistar rats, we have demonstrated SRH may aggravate the degree of emphysematous changes, polycythemia,oxidative stress and systematic inflammation. SRH and emphysema may have a synergistic action in causing systematic damages, and lymphocyte may be playing a central role in this process. Longer duration and more severe extent of SRHIE exposure also seem to result in more serious systematic damages. The mechanisms of all these concerned processes remain to be studied. 展开更多
关键词 sleep-related hypoxemia EMPHYSEMA INFLAMMATION oxidative stress bronchoalveolar lavage fluid superoxide dismutase CATALASE malondialdehyde
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