阿尔茨海默病患者脑脊液SMOC1和OLFML3水平表达及对病情程度的评估价值

目的探讨阿尔茨海默病(Alzheimer’s disease,AD)患者脑脊液人类SPARC相关模块化钙结合蛋白1(SPARC related modular calcium binding 1,SMOC1)、嗅觉介导素3(olfactomedin-3,OLFM3)水平表达及对病情程度的评估价值。方法选取2020年1月~2023年1月宝鸡市人民医院诊治的AD患者108例(AD组),以同期行腰椎穿刺检查的非认知功能障碍患者60例为对照组。应用酶联免疫吸附实验(ELISA)检测脑脊液SMOC1,OLFML3,β-淀粉样蛋白(Aβ1-40,Aβ1-42)和P-Tau蛋白水平。采用Pearson相关分析探讨脑脊液SMOC1,OLFML3水平与临床指标的相关性。采用Logistic回归分析影响AD患者病情程度的因素。采用受试者工作特征(ROC)曲线研究脑脊液SMOC1,OLFML3对AD病情程度的预测价值。结果AD组脑脊液SMOC1(68.47±11.23 ng/L),OLFML3(110.58±21.39 ng/L),P-Tau(569.07±97.24 ng/L)及CDR评分(1.5分)高于对照组(22.60±4.16 ng/L,36.94±6.97ng/L,182.66±55.37 ng/L,0),脑脊液Aβ1-42(292.23±55.36 ng/L),MoCA评分(7.88±2.05分)、MMSE评分(13.15±2.39分)低于对照组(397.16±60.57ng/L,23.13±4.31分,28.02±4.26分),差异具有统计学意义(t=30.465,25.885,28.313,51.211,11.380,31.038,29.013,均P<0.05)。AD组脑脊液SMOC1,OLFML3分别与P-Tau,CDR评分呈正相关(r=0.703,0.634;0.682,0.713,均P<0.05),与Aβ1-42,MoCA评分、MMSE评分呈负相关(r=-0.662,-0.599;-0.660,-0.588;-0.745,-0.731,均P<0.05)。中重度组AD患者脑脊液SMOC1(89.90±12.17 ng/L),OLFML3(142.46±22.48ng/L),P-Tau(618.83±98.19 ng/L)高于轻度组(56.36±10.52 ng/L,92.56±20.25 ng/L,542.25±95.30 ng/L),而脑脊液Aβ1-42(260.76±53.60 ng/L)低于轻度组(310.02±56.54 ng/L),差异具有统计学意义(t=15.029,11.818,3.968,4.430,均P<0.05)。脑脊液SMOC1(OR=1.451,95%CI:1.120~1.879),OLFML3(OR=1.442,95%CI:1.096~1.897),P-Tau(OR=1.589,95%CI:1.258~2.006)是影响中重度AD发生的危险因素,Aβ1-42(OR=0.628,95%CI:0.493~0.799)是保护因素。脑脊液SMOC1,OLFML3及联合预测对中重度AD患者评估的曲线下面积(95%CI)分别为0.882(0.844~0.929),0.846(0.805~0.877)和0.931(0.883~0.965),联合预测大于各单项指标检测,差异具有统计学意义(Z=3.558,4.172,P=0.004,0.000)。结论AD患者脑脊液SMOC1,OLFML3水平升高,两者与AD患者病情程度有关,脑脊液SMOC1,OLFML3联合检测对中重度AD具有较高的预测价值。

人SMOC1重组腺病毒载体的构建及其在主动脉瓣间质细胞中的表达

目的 :利用AdEasyTMvector system构建携带人SMOC1基因的重组腺病毒表达载体,感染人主动脉瓣间质细胞(hAVICs)并检测外源性SMOC1在细胞中的表达和对细胞增殖的影响。方法:用PCR的方法扩增SMOC1 cDNA,将其克隆到pGEM-T Easy载体中并测序鉴定。经NotⅠ和XhoⅠ双酶切后接入pShuttle-CMV穿梭载体,构建重组腺病毒的穿梭质粒pShuttle-CMV-SMOC1。将经PmeⅠ线性化的pShuttle-CMV穿梭载体与pAdEasyTMDNA电穿孔共转化BJ5183重组细菌,获取重组腺病毒质粒pAdEasy-SMOC1,再将经PacⅠ线性化的重组病毒骨架质粒转染HEK293A包装细胞,包装并扩增重组腺病毒(Ad-SMOC1)。用Ad-SMOC1感染hAVICs,以Western blot法和免疫荧光染色法检测重组SMOC1在hAVICs中的表达与定位,用MTS法检测SMOC1对主动脉瓣间质细胞增殖的影响。结果:成功构建并包装表达SMOC1蛋白的重组腺病毒,该重组腺病毒在体外能有效感染hAVICs并高表达SMOC1蛋白,且其介导表达的SMOC1蛋白主要定位于hAVICs的胞浆和胞膜上,MTS分析表明重组SMOC1能够显著促进主动脉瓣间质细胞的增殖。结论:成功地构建了携带人SMOC1基因的重组腺病毒,并证实SMOC1具有促进增殖的作用。本研究为进一步研究SMOC1在瓣膜间质细胞中的作用奠定了实验基础。

Effects of epinephrine on angiogenesis-related gene expressions in cultured rat cardiomyocytes

Epinephrine is often used for the treatment of patients with heart failure, low cardiac output and cardiac arrest. It can acutely improve hemodynamic parameters; however, it does not seem to improve longer term clinical outcomes. Therefore, we hypothesized that epinephrine may induce unfavorable changes in gene expression of cardiomyocyte. Thus, we investigated effects of epinephrine exposure on the mediation or modulation of gene expression of cultured cardiomyocytes at a genome-wide scale. Our investigation revealed that exposure of cardiomyocytes to epinephrine in an in vitro environment can up-regulate the expression ofangiopoietin-2 gene （~ 2.1 times）, and down-regulate the gene expression of neuregulin 1 （-3.7 times）, plasminogen activator inhibitor-1 （-2.4 times） and SPARC-related modular calcium-binding protein-2 （-4.5 times）. These changes suggest that epinephrine exposure may induce inhibition of angiogenesis-related gene expressions in cultured rat cardiomyocytes. The precise clinical significance of these changes in gene expression, which was induced by epinephrine exposure, warrants further experimental and clinical investigations.