Web页面开发模式演变历史研究

随着浏览器应用复杂度的提高,前端技术在不断的演进。经历了静态网页、后端动态程序、后端MVC、后端基于J2EE框架、前端的SPA时代和前端MVC设计方法。本文探索了这些设计方法的优缺点,阐述了推进技术变革的主要因素是效率和性能,相信随着浏览器的发展,会有更多更新的前端开发技术出现。

基于Go语言的区块链模型设计与实现

研究区块链技术原理、特点及POW工作量证明算法,构建基于Go语言的区块链模型,实现挖矿、交易数据打包、区块上链等操作。为了保证交易数据的安全性,模型对区块数据哈希校验,检验数据是否被篡改。在仿真实验中,使用Postman软件对指定端口进行post和get操作,实验结果证明,模型能完成工作量计算,能够实现交易数据上链等操作。

Z-没药甾酮对缺血性脑卒中大鼠氧化应激损伤的保护作用及分子机制

目的探讨Z-没药甾酮(Z-Guggulsterone,Z-GS)对缺血性脑卒中大鼠氧化应激损伤的保护作用及分子机制。方法SD大鼠36只分为假手术组、模型组、Z-GS组,每组12只,模型组大鼠行脑中动脉闭塞(MCAO)术模拟脑缺血,Z-GS组给予Z-GS 30 mg/(kg·d),7 d后,检测大鼠神经功能损伤、组织病理学变化和氧化应激水平,大脑组织Nrf2、HO-1 mRNA和蛋白表达情况。结果与模型组比较,Z-GS给药可显著降低大鼠神经功能评分,减少脑梗死体积,缓解组织病理损伤,可逆转造模对脑组织中抗氧化酶活性的抑制作用,降低氧化应激水平,且可显著促进大鼠脑组织Nrf2和HO-1 mRNA和蛋白的表达(P<0.05)。结论Z-GS可改善缺血性脑卒中大鼠神经功能损伤和氧化应激水平,其机制可能是通过激活Nrf2/HO-1通路发挥作用。

诃子酸抗肾间质纤维化的作用及机制研究

目的探讨诃子酸抗肾间质纤维化的作用及分子机制。方法36只雄性C57/BL小鼠被随机分为假手术组、模型组和诃子酸组。以单侧输尿管结扎术复制肾脏纤维化模型。诃子酸组造模后给予诃子酸灌胃给药。连续给药21天后取血液、肾脏组织。检测肾脏质量指数和血尿素氮(BUN)、血肌酐(Scr)。HE和Masson染色观察肾脏组织病理变化。免疫组化和Western blot检测相关蛋白表达水平。体外实验中,取人肾小管上皮HK-2细胞缺氧处理模拟肾脏纤维化,分为对照组、缺氧组、给药组(缺氧后给予诃子酸)以及转染组(转染siRNA-Klotho以敲减Klotho,然后缺氧并给予诃子酸),Western blot检测相关蛋白表达。结果诃子酸组肾脏质量指数、肾脏组织Klotho蛋白表达水平高于模型组,肾脏组织成纤维细胞生长因子2(FGF2)蛋白表达水平以及血清BUN和Scr水平低于模型组(P<0.05)。诃子酸组较模型组的病理变化明显缓解,纤维化程度以及转化生长因子-β1、α-平滑肌肌动蛋白表达水平降低。给药组的细胞活力、Klotho蛋白表达水平高于缺氧组,乳酸脱氢酶、FGF2蛋白表达水平低于缺氧组(P<0.05)。转染组Klotho蛋白表达水平低于给药组,FGF2蛋白表达水平高于给药组(P<0.05)。结论诃子酸可有效缓解肾间质纤维化水平,其机制可能是通过调控Klotho/FGF2通路发挥作用。诃子酸是潜在的治疗肾脏纤维化药物。

大学生利用学习类APP辅助学习的现状与分析——基于陕西省694名大学生的调查

随着社会经济的快速发展和教育信息化时代的到来,学习类APP的广泛应用对教育教学产生了深远影响。本研究采用问卷调查法,通过对陕西省694名在校大学生利用学习类APP辅助学习的情况进行调查分析,发现大学生存在利用学习类APP学习意识不强、缺乏计划性、缺乏自主学习能力以及对现有学习类APP资源不满的问题,提出加强学习类APP的宣传力度、引导学生有计划的使用学习类APP、提升大学生利用学习类APP的自主学习能力以及优化学习类APP资源的对策建议。

基于B/S架构的毕业设计管理系统研究与应用

针对当前高校毕业设计管理过程中急需实现自动化管理的问题,分析基于B/S架构设计通用毕业设计管理框架需求,从而优化设计毕业设计管理信息系统,并分析该系统框架在实际应用中的效益。结果表明,基于B/S架构设计实现的毕业设计管理信息系统较于传统毕业设计管理模式提高了毕业设计管理效率。

Z-Guggulsterone alleviated renal fibrosis and G_(2)/M cycle arrest through Klotho/P53 signaling

OBJECTIVE Chronic kidney disease(CKD)has become a global public health problem with 10%-15%incidence rate,and inhibiting the renal interstitial fibrosis is considered to be a potential strategy to delay the progression of CKD.Z-Guggulsterone(Z-GS),an active compound from derived from Commiphora mukul,has been proved to be effective in various diseases.The present study aimes to determine the protective effect and the molecular mechanism of Z-GS on renal fibrosis.METHODS Unilateral ureteral obstruction(UUO)mice and hypoxia-induced HK-2 cells were used to simulate renal fibrosis in vitro and in vivo,respectively.The mice and cells were treated with different doses of Z-GS to observe the pharmacological action.Renal function,including Scr,BUN,and UA,were detected by commercial kits.H&E and Masson staining were performed to observe histopathological changes of kidney.Cell viability and LDH release of HK-2 cells were detected by commercial kits.Cell cycle distribution and apoptosis rate were analyzed by flow cytometry.Fibrosis markers were detected by immunohistochemistry and immunofluorescence analysis.Cell cycle related proteins and Klotho/p53 signaling were analyzed by Western blotting.RESULTS The results showed that Z-GS decreased the rise of Scr,BUN,and UA and lightened renal histopathological injury,which were induced by UUO.Besides,Z-GS administration alleviated renal fibrosis in mice by inhibiting the expressions ofα-SMA,TGF-βand collagenⅣ,and delayed G2/M cell cycle arrest by promoting the expressions of CDK1 and cyclinD1/B1 rate.Experiments in vitro indicated that Z-GS treatment significantly increased the cell viability while decreased the LDH release in hypoxia-induced HK-2 cells.In addition,hypoxia induced fibrosis and G2/M cycle arrest in HK-2 cells were retarded by Z-GS.The study of its possible mechanism exhibited that Z-GS treatment increased the level of Klotho and inhibited P53 level.Nevertheless,the effect of Z-GS on Klotho/P53 signaling was reversed by siRNA-Klotho.Moreover,siRNA-Klotho treatment eliminated the effects of Z-GS on G2/M cell cycle arrest and fibrosis.CONCLUSION This study clarified that Z-GS alleviated renal fibrosis and G2/M cycle arrest through Klotho/P53 signaling pathway.People who have suffered CKD may potentially benefit from treatment with Z-GS.