带有饱和治疗函数的SIS模型的几类分支分析

研究了具有标准发生率和饱和治疗函数的SIS传染病模型的几类分支.该模型中使用的饱和治疗函数是一个连续且可微的函数,用以说明当治愈率较低以及感染人数较多时延迟治疗所产生的影响.讨论了系统无病平衡点和地方病平衡点的存在性,证明了该系统存在倒向分支,分析了系统平衡点的局部和全局稳定性,讨论了该系统Hopf分支和Bogdanov-Takens分支的存在情况,得出了相应结论并且给出了系统的分支相图,以及针对研究得出的数学结果提出了一些合理化建议.

具有饱和治疗率的霍乱模型稳定性分析

提出了一个具有饱和治疗率的SIRB霍乱传播模型,考虑人与人之间直接传播和人与环境之间间接传播两种传播方式。详细分析了模型的动力学性态,用中心流行理论证明了后向分支存在的充分条件,并用比较原理证明了当R^(*)<1时,无病平衡点是全局渐近稳定的;用几何方法证明了当R_0>1时,地方病平衡点是全局渐近稳定的。数值模拟支持了理论结果。

具有Beddington-DeAnglis发生率和饱和治疗率的SEIRS模型的研究

本文建立了具有Beddington-DeAnglis发生率和饱和治疗率的SEIRS模型,通过构造Lyapunov函数和Dulac函数,并利用Hurwitz判据来分析无病平衡点和地方性平衡点的稳定性。可以得到,当R0c<1时,无病平衡点是局部渐进稳定和全局渐进稳定的,根据平面定性理论以及Dulac函数,地方性平衡点是局部渐进稳定和全局渐进稳定的。

一类具有一般发生率和饱和治疗函数的SIS传染病模型的分支与稳定性分析（英文）

介绍带有一般发生率和饱和治疗函数的SIS模型,采用连续可微的饱和治疗函数,描述当医疗条件有限并且感染者的数量增加时,延迟治疗所产生的影响。采用的是一般发生率,包括双线性发生率与标准发生率。给出无病平衡点与地方性平衡点存在性与全局渐进稳定性成立的充分条件,证明当治疗能力很低时出现倒向分支,因此必须提高治疗的效率与能力。数值分析证明了Hopf分支的存在性。

一类带有饱和治疗函数的SIR模型的分支分析

本文研究一类带有饱和治疗函数的SIR模型.饱和治疗函数是描述在有限医疗资源以及感染者数量较大的情况下,感染者治疗被延误的影响.我们证明该模型随着参数的变化发生Bogdanov-Takens分支,并通过数值模拟直观展示结论的正确性.

具有饱和治疗函数与密度制约的SIS传染病模型的后向分支

讨论了一个具有饱和治疗函数以及出生率和死亡率均具有密度制约的SIS传染病模型,其中总人口的变化满足Logistic方程,治疗项采用一个连续可微的函数,描述在医疗条件有限的情况下患病者的治疗被耽误的影响.研究发现当患病者的治疗被耽误的影响较强时,模型将出现后向分支,因此基本再生数R_0=1不再是疾病是否消亡的阈值.另外还得到无病平衡点和地方平衡点全局稳定的充分条件.

冠状动脉内过饱和氧辅助治疗装置的研究进展

急性心肌梗死(AMI)是一种常见的心血管疾病,其病因主要为冠状动脉粥样硬化和冠状动脉血栓形成,临床多表现为严重的血流动力学紊乱和心输出量过低。目前,经皮冠状动脉介入治疗(PCI)仍是AMI的主要临床救治方法。尽管大多数AMI患者,在接受PCI后恢复了冠状动脉内主要血管的血流灌注,但仍存在大量冠状动脉内微血管阻塞的情况,使得梗死心肌未得到有效恢复。冠状动脉内过饱和氧辅助治疗装置可改善梗死相关动脉内的微血管循环,有效减少梗死面积,具有良好的应用前景。

具有Logistic增长和治疗的SIRS传染病模型的后向分支

利用传染病动力学理论,建立一类具有Logistic增长和治疗的SIRS传染病模型,并假设模型中总人口增长满足Logistic方程,考虑治疗项为非线性的可微函数,以描述有限的医疗资源对延迟患者治疗的影响.综合运用微分方程稳定性理论中的Routh-Hurwitz判据、LaSalle不变集原理并构造适当的Lyapunov函数方法,获得了该模型的无病平衡点和地方病平衡点全局渐近稳定的代数判据及后项分支存在条件.结果表明,当延迟患者治疗的影响较严重时,该模型会出现后向分支现象,基本再生数已不再是疾病是否消亡的阀值,需要加强医疗资源建设,通过提供及时优质的医疗服务,才能有效控制或根除疾病.

一类具有脉冲扰动和饱和治愈率的媒介传染病模型研究

考虑到对染病宿主进行治疗并对传染媒介实施脉冲控制,本文建立了一个SIR-SI媒介传染病模型,分析了模型的动力学性态。利用脉冲微分方程理论讨论了无病周期解的存在性,同时证明阈值小于1时该无病周期解局部渐近稳定。当阈值大于1时,利用比较定理,证明了系统的一致持久性。数值模拟结果表明,饱和治疗项、脉冲控制周期及脉冲控制强度对模型有重要影响,出现了分支、混沌等丰富的动力学现象。

改变细胞膜脂肪酸组成防治大肠癌的基因治疗研究

目的:利用脂肪酸去饱和酶基因fat-1改变细胞膜脂肪酸组成,进行大肠癌的基因治疗研究。方法:将fat-1基因插入腺病毒载体中,与骨架载体同源重组,构建腺病毒重组载体(Ad-GFP-fat1),通过包装细胞系(293)产生的腺病毒,感染人大肠癌株HT-29细胞。提取细胞的总RNA,以fat-1基因的反义mRNA作探针,用Northern Blot检测fat-1基因在HT-29细胞内的表达。以流式细胞仪对HT-29细胞G_0/G_1期、S期、G_2/M期所占比例进行检测,分析fat-1基因对HT-29细胞增殖和凋亡的影响。以气相色谱分析仪分析fat-1基因对HT-29细胞细胞膜n-6 PUFAs和n-3 PUFAs含量及n-6/n-3PUFAs比例的影响。将HT-29细胞皮下接种于裸鼠右前肢腋下,建立裸鼠HT-29大肠癌细胞皮下移植瘤模型。成瘤后进行治疗实验,经连续5次治疗,于最后一次治疗后第3天处死小鼠,取肿瘤称重。分析fat-1基因裸鼠体内抗肿瘤效果。结果:通过基因重组技术,得到高滴度的含fat-1基因的重组病毒;腺病毒介导的fat-1基因能够在HT-29细胞中有效表达;fat-1基因的表达可降低HT-29细胞膜n-6/n-3PUFAs的比例,有效抑制HT-29细胞增殖,促进细胞凋亡并能抑制裸鼠移植瘤的发展。结论:fat-1基因的表达,可抑制HT-29细胞的体内外增殖并诱导细胞凋亡,在大肠癌基因治疗中可能具有良好利用价值。

ω-6脂肪酸脱氢酶基因在乳腺癌细胞内的表达和作用

为探讨ω- 6脂肪酸脱氢酶基因fat -1在人类乳腺癌细胞MCF- 7中表达和对其生长的作用,将fat -1基因插入到腺病毒载体中,构建腺病毒重组载体(Ad·GFP·fat1) .通过包装细胞系(2 93)产生重组腺病毒,感染MCF 7细胞.用核糖核酸酶保护性分析技术,检测fat -1基因在MCF- 7细胞内的表达,细胞增殖试剂盒(MTT)和凋亡染色试剂盒染色分析fat 1基因对MCF- 7细胞增殖和凋亡的影响,用酶联免疫分析花生酸类(eicosanoids)前列腺素E2 (prostaglandinE2 )的含量.结果显示,腺病毒介导的fat- 1基因能在MCF- 7细胞内有效异源表达,抑制MCF -7细胞的增殖且导致凋亡,前列腺素的含量也明显地减少.结果说明,fat- 1基因在乳腺癌的基因治疗中具有良好利用价值.

非酒精性脂肪性肝病临床分析及海狗油疗效观察

目的对照性分析非酒精性脂肪性肝病(NAFLD)临床特点,探讨海狗油ω-3多不饱和脂肪酸胶丸(海狗油)对NAFLD的治疗效果。方法①收集NAFLD患者和正常健康人资料各76例,以病例对照研究方法分析NAFLD的临床生化指标。②选取18例NAFLD患者,予以海狗油连续治疗12周,动态观察海狗油对NAFLD患者临床生化和影像学检查结果的影响。结果①NAFLD组体重指数(BMI)、谷丙转氨酶(ALT)、甘油三酯(TG)、极低密度脂蛋白胆固醇(VLDL-C)、空腹血糖(FPG)显著高于对照组(P<0.01),两组间AST和TCH差异无显著性。②NAFLD组合并肥胖、高血压、血脂紊乱、高血糖中两项或两项以上者和代谢综合征者分别为72.37%(55/76)和46.05%(35/76)。③与治疗前比较,海狗油治疗4周末和8周末时,NAFLD患者的血清LP-a显著降低(P<0.01);治疗12周末时,血清Apo-A1明显降低(P<0.05),肝/脾CT值比值的差异无显著性(P>0.05)。结论NAFLD与肥胖、血脂紊乱和高血糖密切相关,海狗油对NAFLD患者的血脂有一定调节作用。

Effects of n-3 polyunsaturated fatty acids from seal oils on nonalcoholic fatty liver disease associated with hyperlipidemia

AIM: To investigate the efficacy and safety of n-3 polyunsaturated fatty acids (PUFA) from seal oils for patients with nonalcoholic fatty liver disease (NAFLD) associated with hyperlipidemia. METHODS: One hundred and forty-four patients with NAFLD associated with hyperlipidemia were included in the 24-wk, randomized, controlled trial. The patients were randomized into two groups. Group A (n = 72) received recommended diet and 2 g n-3 PUFA from seal oils, three times a day. Group B (n = 72) received recommended diet and 2 g placebo, three times a day. Primary endpoints were fatty liver assessed by symptom scores, liver alanine aminotransferase (ALT) and serum lipid levels after 8, 12, 16, and 24 wk. Hepatic fat inf iltration was detected by ultrasonography at weeks 12 and 24 after treatment. RESULTS: A total of 134 patients (66 in group A, 68 in group B) were included in the study except for 10 patients who were excluded from the study. After 24 wk of treatment, no change was observed in body weight, fasting blood glucose (FBG), renal function and blood cells of these patients. Total symptom scores, ALT and triglyceride (TG) levels decreased more significantly in group A than in group B (P < 0.05). As expected, there was a tendency toward improvement in aspartate aminotransferase (AST), γ-glutamyltranspeptidase (GGT), and total cholesterol (TCHO) and high- density lipoprotein (HDL) cholesterol levels (P < 0.05) after administration in the two groups. However, no significant differences were found between the two groups. The values of low-density lipoprotein (LDL) were significantly improved in group A (P < 0.05), but no significant change was found in group B at different time points and after a 24-wk treatment. After treatment, complete fatty liver regression was observed in 19.70% (13/66) of the patients, and an overall reduction was found in 53.03% (35/66) of the patients in group A. In contrast, in group B, only f ive patients (7.35%, 5/68) achieved complete fatty liver regression (P = 0.04), whereas 24 patients (35.29%, 24/68) had a certain improvement in fatty liver (P = 0.04). No serious adverse events occurred in all the patients who completed the treatment. CONCLUSION: Our results indicate that n-3 PUFA from seal oils is safe and effi cacious for patients with NAFLD associated with hyperlipidemia and can improve their total symptom scores, ALT, serum lipid levels and normalization of ultrasonographic evidence. Further study is needed to confi rm these results.

高原环境下饱和吸氧治疗急性高原反应1例

急性高原反应(acute mountain sickness,AMS)是人群从平原进入海拔3000 m以上地区或久居高原者进入更高的海拔地区,多在数小时内发病并表现一系列非特异性临床表现的临床综合征[1]。AMS以呼吸困难、发绀、头昏、头痛、恶心、呕吐、睡眠障碍、心悸、气短、乏力、心率增加、食欲减退等临床症状为主要表现[2],部分症状严重者可出现高原肺水肿和高原脑水肿,救治不及时甚至可导致死亡。

他汀类药物对急性冠状动脉综合征患者vWF因子的影响

目的:探讨洛伐他汀和氟伐他汀对急性冠脉综合征(ACS)患者血浆血管性血友病因子(vonWillebrand-factor,vWF)及血脂水平的影响。方法:88例ACS患者随机单盲分为3组,其中对照组(A组)18例;洛伐他汀组(B组)34例,20mg/d;氟伐他汀组(C组)36例,20mg/d;检测患者治疗前后30d血清vWF浓度和血脂浓度变化。结果:B、C组能显著降低血总胆固醇(TC)、甘油三酯(TG)及低密度脂蛋白(LDL)水平、升高血高密度脂蛋白(HDL);两组间疗效无明显差异;B、C组能显著降低vWF的浓度,两组间疗效无明显差异;B、C组患者的血清vWF水平降低与血清TC、TG、LDL的水平降低、HDL的水平升高不相关。结论:洛伐他汀和氟伐他汀治疗急性冠脉综合征患者30天就可明显改善血脂,降低vWF水平,具有完善内皮功能、抑制血小板黏附聚集等作用。

Omega-3 fatty acids for the treatment of non-alcoholic fatty liver disease

Non-alcoholic fatty liver disease （NAFLD） has been recognized as a major health burden. It is the most important cause of chronic liver disease and a major in- dependent cardiovascular risk factor. Lacking a definite treatment for NAFLD, a specific diet and an increase in physical activity represent the most commonly used therapeutic approaches. In this review, major literature data about the use of omega-3 polyunsaturated fatty ac- ids （n-3 PUFAs） as a potential treatment of NAFLD have been described, n-3 PUFAs, besides having a beneficial impact on most of the cardio-metabolic risk factors （hy- pertension, hyperlipidemia, endothelial dysfunction and atherosclerosis） by regulating gene transcription factors [i.e., peroxisome proliferator-activated receptor （PPAR） cz, PPARy, sterol regulatory element-binding protein-i, carbohydrate responsive element-binding protein], im- pacts both lipid metabolism and on insulin sensitivity. In addition to an enhancement of hepatic beta oxidation and a decrease of the endogenous lipid production, n-3 PUFAs are able to determine a significant reduction of the expression of pro-inflammatory molecules （tumor necrosis factor-~ and interleukin-6） and of oxygen reac- tive species. Further strengthening the results of the in vitro studies, both animal models and human interven- tion trials, showed a beneficial effect of n-3 PUFAs on the severity of NAFLD as expressed by laboratory pa- rameters and imaging measurements. Despite available results provided encouraging data about the efficacy of n-3 PUFAs as a treatment of NAFLD in humans, well- designed randomized controlled trials of adequate size and duration, with histological endpoints, are needed to assess the long-term safety and efficacy of PUFA, as well as other therapies, for the treatment of NAFLD and non-alcoholic steatohepatitis patients. It is worthwhile to consider that n-3 PUFAs cannot be synthesized by the human body and must be derived from exogenous sources （fish oil, flaxseeds, olive oil） which are typical foods of the Mediterranean diet, known for its beneficial effects in preventing obesity, diabetes and, in turn, cardiovascular events. According to these data, it is important to consider that most of the beneficial effects of n-3 PUFAs can also be obtained by an equilibrate nutrition program.