基于氧化应激反应探讨慢性体表溃疡发病机理及象皮生肌膏联合托里消毒散的干预作用

目的 探讨慢性体表溃疡发病机理以及象皮生肌膏联合托里消毒散的干预作用。方法 将30只SPF级雄性SD大鼠按随机数字表法分为空白对照组、模型组、象皮生肌膏组、托里消毒散组、象皮生肌膏联合托里消毒散组,每组各6只。采用金黄色葡萄球菌造模,连续给药1周后,检测创面组织中血管内皮生长因子(Vascular endothelial growth factor,VEGF)、血管内皮细胞生长因子受体2(Vascular endothelial growth factor receptor 2,VEGFR-2)、核因子E2相关因子2(Nuclear factor erythroid 2-related factor 2,Nrf2)、NAD(P)H醌氧化还原酶1[NAD(P)H quinone oxidoreductase1,NQO1)、血红素加氧酶1(Heme oxygenase-1,HO-1)]表达水平。结果 与空白对照组比较,模型组创面组织中VEGF、VEGFR-2表达均明显降低,差异有统计学意义(P<0.01);与模型组比较,象皮生肌膏组、托里消毒散组、象皮生肌膏联合托里消毒散组VEGF、VEGFR-2表达均明显升高,差异有统计学意义(P<0.01)。与对照组比较,模型组中Nrf2、NQO1、HO-1表达水平升高,差异有统计学意义(P<0.01);与模型组比较,象皮生肌膏组、托里消毒散组、象皮生肌膏联合托里消毒散组Nrf2表达水平均明显升高,NQO1和HO-1表达降低,差异有统计学意义(P<0.01)。结论 大鼠慢性溃疡的形成可能与氧化应激反应抑制了VEGF通路及Nrf2通路有关,而象皮生肌膏联合托里消毒散可能通过调节上述通路促进溃疡处血管新生和抗氧化应激,进而提高创面愈合能力。

基于优化MaxEnt模型的黑木相思引种栽培区划

利用MaxEnt模型评估黑木相思在中国引种的潜在适生区,探讨影响其适生区分布的主要生态因子,并对适生区范围和类型进行划分,旨在为该树种在中国的引种区划提供依据。采用ENMeval数据包优化的MaxEnt模型,基于14个环境变量和159条黑木相思分布点,以我国95°-125°E、17°-38°N区域为模型投射空间范围,评估黑木相思的潜在适生地理分布;通过Spearman相关分析、方差膨胀因子(VIF)分析和刀切法检验,筛选出制约其潜在分布的主导环境因子。经ENMeval优化,当特征组合F C=Q HP,调控倍频R M=6时,A UC值为0.965,模型准确度极高。刀切法检验表明:最干月降雨量(40.1%)、月平均昼夜温差(26.9%)、年降水量(15.6%)、年均温(6.6%)、最冷月最低温(3.2%)和表层土壤酸碱度(2.8%)是影响黑木相思地理分布的重要生态因子,累计贡献率达95.2%。结果表明,黑木相思在中国适生区分为高(55.8354×10^(4) km^( 2))、中(152.9915×10^(4) km^( 2))、低(68.4567×10^(4) km^( 2))和非适生区(682.7165×10^(4) km^( 2)),其中高适生区为黑木相思引种栽培推广的重点地区,主要涵盖贵州、湖南、江西、福建、浙江东南部、台湾中部、云南西部和东部、广东北部和广西北部。该研究划分了黑木相思在中国适生分布范围,并分析了制约其分布的主要生态因子为水分和温度,为黑木相思在中国引种和推广提供科学依据。

益肾通癃汤对人前列腺癌DU-145细胞上皮-间质转化及Ras/ERK信号通路的影响

目的:观察益肾通癃汤对人前列腺癌DU-145细胞上皮-间质转化(EMT)及Ras/ERK信号通路的影响并探讨其作用机制。方法:将人前列腺癌DU-145细胞分为空白血浆组,益肾通癃汤含药血浆高、中、低剂量组(以下简称中药高、中、低剂量组)。运用CCK-8法观察各组DU-145细胞增殖情况,Annexin V&PI双染色法进行细胞凋亡检测,PI法进行细胞周期检测,Transwell小室及划痕实验法检测各组DU-145细胞侵袭能力及迁移情况,Western印迹检测益肾通癃汤干预后各组DU-145细胞EMT及Ras/ERK信号通路相关蛋白的表达变化,RT-PCR检测DU-145细胞EMT及Ras/ERK信号通路相关蛋白的基因表达情况。结果:与空白血浆组对比,中药高、中、低剂量组均可显著抑制DU-145细胞增殖,降低其贴壁生长能力并呈剂量依赖性(P<0.05,P<0.01);中药高、中、低剂量组可显著促进人前列腺癌DU-145细胞凋亡并呈剂量依赖性(P<0.01);中药高、中、低剂量组可显著调控DU-145细胞周期并呈剂量依赖性(P<0.05,P<0.01);中药高、中、低剂量组可显著降低人前列腺癌DU-145细胞体外侵袭、迁移能力并呈剂量依赖性(P<0.05);Western印迹结果显示,与空白血浆组比较,中药高、中、低剂量组人前列腺癌DU-145细胞中N-钙黏蛋白(N-cadherin)、锌指转录因子(Snail)、Ras、p-ERK1/2、ERK1/2、基质金属蛋白酶(MMP-9)等蛋白表达均存在一定程度的下调,而E-钙黏蛋白(E-cadherin)表达上调并存在显著差异(P<0.05,P<0.01);RT-PCR结果显示,中药高、中、低剂量人前列腺癌DU-145细胞N-cadherin mRNA、Ras、ERK1表达下调,而E-cadherin mRNA表达上调并存在显著差异(P<0.05,P<0.01)。结论:益肾通癃汤能够有效抑制人前列腺癌DU-145细胞的增殖并促进其凋亡,调控细胞周期,抑制其侵袭及迁移能力及EMT进程,益肾通癃汤治疗前列腺癌的作用机制可能是通过抑制前列腺癌细胞EMT进程及Ras/ERK信号通路表达有关。

标准滴定溶液的配制与标定标准化探讨

针对标准滴定溶液的配制与标定操作中对GB/T601-2016《化学试剂标准滴定溶液的制备》较难理解,配制和标定记录未表格化、标准化,记录信息不完善,无法溯源或进行不确定度的评定等,阐述了有关内容的理解和操作,给出了EDTA标准溶液的配制和标定记录标准化的编制示例,对检验检测、化工行业的质量管理及实验人员配制标准滴定溶液记录标准化有一定的参考作用。

Chinese Medicine as Supporting Therapy for Psoriasis:Past,Present,and Future

Psoriasis is a chronic skin disease and an important health concern.Western medicine and therapies are the main treatment strategies for psoriasis vulgaris(PV);however,the overall prognosis of patients with PV is still poor.Therefore,PV prevention is especially crucial.Chinese medicine(CM)has a long history of treating psoriasis,and it has unique wisdom in different cognitive angles and treatment modes from modern medicine.In this review,we first summarized the herbs and ancient CM formulas that have therapeutic effects on PV.Second,the research status and obstacles to the current development of CM in modern medicine were reviewed.Finally,the future of CM in the context of precision medicine and integrated medicine was discussed.After a detailed reading of the abundant literature,we believe that CM,through thousands of years of continuous development and clinical practice,has achieved high effectiveness and safety for PV treatment,despite its surrounding controversy.Moreover,precise analyses and systematic research methods have provided new approaches for the modernization of CM in the future.The treatment of PV with CM is worth popularizing,and we hope it can benefit more patients.

Synthesis and Crystal Structure of 6-Cyclohexyl-8-methylphenanthridine

The target compound Ⅳ (C_(20)H_(21)N) was synthesized through four-step reactions and structurally determined by single-crystal X-ray diffraction.The crystal of compound Ⅳ is in the orthorhombic system,space group Fdd2 with a=41.178(19),b=30.389(8),c=4.8182(17)Å,β=90°,C_(20)H_(21)N,M_(r)=275.38,D_(c)=1.213g/cm^(3),V=6029(4)Å^(3),Z=16,F(000)=2368,μ(Mo Ka)=0.527 mm^(-1),T=240(2) K,2200 independent reflections with 1233 observed ones (I>2σ(I)),R=0.1285 and w R=0.2589 with GOF=1.050 (R=0.2058 and w R=0.3055for all data).A one-dimensional interaction model of the title compound was formed by one kind of π-π interactions between the two phenyl rings of the adjacent molecules at upper and lower levels.The inhibition to the strand transfer process of HIV-1 integrase of the target compound was also evaluated.