Stability assessment and risk analysis of aboveground river in lower Yellow River

Although the Chinese people have, through continuous efforts, built the constantly improving Yellow River flood control system, and created a miracle which has been tranquil for over 50 years, the tendency for the downstream watercourse of the Yellow River to uplift every year has not been fundamentally curbed, and the aboveground river is still the “scourge” of the sons and daughters of the Yellow River. By the use of a variety of modern investigation and survey methods, the geological environment characteristics of the downstream of the Yellow River have been identified basically, including the environmental and geological factors affecting the stability of aboveground rivercourse of the lower Yellow River such as the active fracture of the lower Yellow River, crustal uplift, land subsidence, seismic activity, geological conditions of dike foundation engineering, hydrodynamic conditions of rivers, and geomorphology of watercourses. After a comprehensive analysis of the inability mode of aboveground river on the downstream of the Yellow River and its corresponding impact factors, by using the fuzzy comprehensive evaluation method, we have evaluated the crustal stability of the aboveground river, dike foundation stability, watercourse landform stability and overall stability. The results of comprehensive results show that the stability of downstream aboveground rivercourse of the Yellow River can be divided into four grades and 11 sections, i e. “basically stable, unstable, very unstable and extremely unstable”. On the basis of the stability segmentation, we consider the influence of integrally the future structural faults, earthquakes, the difference of watercourse between forward and backward heights of dikes, river regime and river type, historical crevasses, foundation soil liquefaction and seepage deformation, and find out 17 most unstable danger points. Finally, from 17 danger points, we select 7 danger points which are most prone to instability including Wuzhi, Zhongmou, Kaifeng, Fengqiu, Dongming, Changyuan and Dong’e. The calculation and analysis of the range and area inundated by 7 danger points, area, and number of people threatened, possible economic loss, and environmental damage, the inability caused by any one of 7 points could bring disastrous consequences to the downstream.

根皮素聚乙二醇-聚乳酸纳米胶束的制备、表征及口服药动学研究

目的制备根皮素聚乙二醇-聚乳酸[methoxy poly(ethylene glycol)-poly(lactic acid),mPEG-PLA]纳米胶束(phloretin mPEG-PLA nanomicelles,Phl@mPEG-PLA/NM)处方,考察其口服药动学行为。方法薄膜分散-探头超声法制备Phl@mPEGPLA/NM。采用包封率、载药量、沉降率为指标,单因素结合Box-Behnken设计-效应面法优化处方。透射电子显微镜(TEM)观察外貌形态,透析法考察体外释药行为。SD大鼠分别ig给予根皮素混悬液和Phl@mPEG-PLA/NM,HPLC法测定根皮素血药浓度,计算主要药动学参数。结果Phl@mPEG-PLA/NM最佳处方为m PEG-PLA用量为105 mg、水化体积为9.5 mL、水化温度40℃。包封率、载药量、沉降率、粒径及ζ电位分别为(88.52±1.86)%、(8.84±0.32)%、(8.04±0.23)%、(85.07±6.12)nm和(-23.56±1.49)mV。纳米胶束外貌为球形。Phl@mPEG-PLA/NM的半衰期(t1/2)增加至(4.60±0.84)h,血药浓度(Cmax)增加至(1284.56±307.65)ng/mL,口服相对生物利用度提高至3.34倍。结论Phl@mPEG-PLA/NM显著促进了根皮素口服吸收。

IL-4、IL-6、IL-10、TNF-α基因多态性与药物性肝损伤相关性的Meta分析

目的:探讨IL-4、IL-6、IL-10和TNF-α基因多态性与药物性肝损伤(drug-induced liver injury,DILI)易感性关系。方法:检索Pubmed、Web of Science、Cochrane Library、EMBASE、知网与万方数据库,查找建库有关IL-4、IL-6、IL-10和TNF-α基因多态性与DILI发病风险的文献。应用STATA12.0对数据进行Meta分析。结果:共纳入10篇文献,共包括717例DILI患者和1 674例正常对照。所有研究都纳入Meta分析发现IL-6 rs1800796G>C中G等位基因携带者(OR=2.507, 95%CI[1.542, 4.074],P=0.000)患DILI的风险显著升高,而TNF-αrs1800629G>A中G等位基因携带者(OR=0.715, 95%CI[0.524, 0.976],P=0.035)患DILI的风险显著降低。在剔除一项显著的异质性研究后,携带IL-6 rs2066992G>T中G等位基因人群(OR=2.465, 95%CI[1.506, 4.036],P=0.000)人群患DILI风险显著增加,而携带IL-10 rs1800872A>C中C等位基因(OR=0.818, 95%CI[0.679, 0.985],P=0.034)人群患DILI风险则显著降低。本研究暂未发现IL-4各基因位点基因型与DILI有明显关联性。结论:TNF-α(rs1800629G>A)、IL-6(rs1800796G>C、rs2066992G>T)与IL-10(rs1800872A>C)与DILI发生有一定的关联性。

吴茱萸碱纳米结构脂质载体处方优化和SD大鼠体内口服药动学研究

目的优化吴茱萸碱纳米结构脂质载体(evodiamine nanostructured lipid carriers,Evo-NLC)处方,研究SD大鼠体内口服药动学特征。方法高压均质法制备Evo-NLC。单因素考察结合Box-Behnken响应面法优化Evo-NLC处方并进行表征,透析法考察体外释药情况。按照100 mg/kg剂量ig后采血,HPLC法测定血药浓度,计算吴茱萸碱和Evo-NLC的主要药动学参数。结果制备的Evo-NLC外观为淡蓝色乳光的透明液体。最佳处方为吴茱萸碱用量为64.13 mg,固-液脂质比为4.34∶1,表面活性剂用量为1.15%。测得Evo-NLC平均包封率为(87.84±1.62)%,平均粒径为(152.62±9.43)nm,Zeta电位为(-36.67±1.93)mV,载药量为(5.96±0.22)%。体外释药过程符合Weibull模型lnln[1/(1-M;/M;)]=0.514 4 lnt-1.311 2。口服药动学结果显示,与吴茱萸碱原料药相比,Evo-NLC的口服相对生物利用度提高至4.47倍。结论 Box-Behnken响应面法所建立的模型可用于Evo-NLC处方优化,Evo-NLC有效提高了吴茱萸碱的相对口服吸收生物利用度。

ApoE基因多态性对瑞舒伐他汀治疗高脂血症疗效的影响及其机制的研究

目的:探讨ApoE基因多态性对瑞舒伐他汀(rosuvastatin,RSS)治疗高脂血症疗效的影响及其具体机制。方法:选取2018年1月1日至12月31日在郑州大学第二附属医院诊断的高血脂患者910例,采用"基因芯片法(Gene Chip)"分析ApoE基因型,并依据等位基因分组(ε2组、ε3组及ε4组),于RSS用药前及连续用药8周后采集静脉血,比较各组患者RSS用药前后总胆固醇(total cholesterol,TC)、三酰甘油(triglyceride,TG)、高密度脂蛋白胆固醇(high density liptein cholesterol,HDL-C)、低密度脂蛋白(low density lipoprotein,LDL)及脂蛋白a[lipoprotein-a,Lp(a)]变化水平,RT-PCR法检测用药前后ApoE mRNA表达;无血清培养正常人L-02型肝细胞诱导低密度脂蛋白受体(low density lipoprotein receptor,LDL-R)活性,分别加入不同浓度ApoE2/3/4-DMPC复合物,ELISA法比较ApoE2/3/4竞争性结合LDL-R的能力,RT-PCR法比较RSS用药后ApoE2/3/4对LDLR mRNA、HMG-CoA mRNA表达的影响。结果:ε2组(ε2/ε2、ε2/ε3)患者RSS治疗后TC、TG、LDL-C、Lp(a)下降水平,HDL-C升高水平显著高于ε3组(ε3/ε3、ε2/ε4)及ε4组(ε3/ε4、ε4/ε4)患者,其中ε4组疗效最差;ε2组(ε2/ε2、ε2/ε3)及ε3组(ε3/ε3)、ε4组(ε3/ε4)RSS用药后较用药前ApoE mRNA相对表达量显著降低(P<0.05),但ε3组(ε2/ε4)与ε4组(ε4/ε4)两种基因型RSS用药前后无显著性统计学差异(P>0.05)。在L-02肝细胞中,ApoE2与LDL-R结合力高于ApoE3(P<0.05),ApoE4与LDL-R结合力最弱;与ApoE3比较,ApoE2可显著上调LDL-R mRNA表达(P<0.05),但ApoE4则抑制LDL-R mRNA表达(P<0.05);ApoE2抑制HMG-CoA mRNA表达的程度显著高于ApoE3(P<0.05),而ApoE4抑制HMG-CoA mRNA表达的程度显著低于ApoE3(P<0.05)。结论:RSS对于ApoEε2等位基因患者降低血脂的疗效最优,其次为ε3、ε4等位基因携带者,该作用可能与ApoE2诱导LDLR基因表达,增强ApoE2与LDLR亲和力,从而增强RSS对HMG-CoA基因表达抑制作用有关。