Overexpression of hepatic plasminogen activator inhibitor type 1 mRNA in rabbits with fatty liver

INTRODUCTIONPlasminogen activator inhibitor type 1 ( PAI-I ), an approximately Mr 50000 glycoprotein, is the major physiological inhibitor of plasminogen activators. It is not only the priming factor for atherosclerosis and coronary thrombosis[1-3] , but also participates in the genesis of chronic hepatitis and liver fibrosis[4-11] . However, there has been no available report yet about the research of hepatic PAl-1 gene expression in hyperlipidemia and fatty liver. The present study aimed to explore the change of hepatic PAl-1 mRNA and its plasma activity by means of animal model.

THE INCREASE IN PLASMINOGEN ACTIVATOR INHIBITOR TYPE-1 EXPRESSION BY STIMULATION OF ACTIVATORS FOR PEROXISOME PROLIFERATOR-ACTIVATED RECEPTORS IN HUMAN ENDOTHELIAL CELLS

Objective.To investigate the effect of peroxis ome proliferator-activated recept ors(PPARs )activators on plasminogen activator inhibitor ty pe-1(PAI-1)expression in human umbilical vein e ndothelial cells and the possi-ble mechanism.Methods.Human umbilical vein endothelial ce lls(HUVECs )were obtained from normal fetus,and cul-tured conventionally.Then the HUVECs were exposed to test agents(linolenic acid,linoleic acid,oleic acid,stearic acid and prostaglandin J 2 respectively)in varying concentrations with fresh media.RT -PCR and ELISA were applied to determine the expression of PPARs and PAI-1in HUVECs.Results.PPARα,PPARδand PPARγmRNA were detected by using RT-PCR in HUVECs.Treatment of HUVECs with PPARαand PPARγactivators---linolenic acid,linoleic acid,oleic acid and prostaglandin J 2 respectively,but not with stearic a cid could augment PAI-I mRNA expression and protein secretion in a concentration-dependent manner.However,the mRNA expressions of 3subclasses of PPAR with their activators in HUVECs were not changed compared w ith controls.Conclusion.HUVECs express PPARs.PPARs activators may increase PAI-1expression in ECs,but the underlying mechanism remains uncle ar.Although PPARs expression was not enhanced after stimulated by their activators in ECs,the role of functionally active PPARs in regulating PA I-1expression in ECs needs to be further investigated by using transient gen e transfection assay.

Genetic and Metabolic Determinants of Plasminogen Activator Inhibitor 1 (PAI-1) in Tunisian Type 2 Diabetes Patients

Background: PAI-1 (plasminogen activator inhibitor-1) is a powerful regulator of fibrinolysis and plasma level is high in type 2 diabetes and cardio-vascular disease, which is determined by genetic polymorphisms in PAI-1 gene and environmental factors. The aim of the study was to examine the determinants of plasma PAI-1 Ag level among type 2 diabetes patients. Methods: 491 Tunisian type 2 diabetes patients had clinical evaluation (weight, high, BMI, Waist Circumference), laboratory investigations including FBG Hb1Ac, cholesterol, triglyceride;HDL-cholesterol was done;plasma PAI-1 antigen level was done with ELISA;&minus;675 4G/5G and &minus;844 G/A polymorphisms of PAI-1 gene was done by PCR-ASA and PCR-RFLP respectively. Results: The mean age for our patients was 58.3 ± 10.5 years;sex-ratio = 0.92;mean PAI-1 level was 34.6 ± 21.3 ng/ml. We didn’t find correlation between PAI-1 level and BMI, but we have found significant correlation between PAI-1 and waist circumference (p = 0.032), most enhanced in men (P = 0.002), T2D patients who have FBG > 11 mmol/l had PAI-1 Ag level higher than those who have FBG P = 0.034), but no difference found between T2D with high Hb1Ac > 8% and those with Hb1Ac < 8%, significant correlation was seen between PAI-1 level and LDL-cholesterol (P = 0.05), high correlation between PAI-1 Ag level and &minus;675 4G/5G polymorphism genotype was seen, 4G/4G carriers had the highest PAI-1 level, 4G/5G had intermediary level and 5G/5G had the lowest level (P &minus;844G/A polymorphism genotypes. Using multiple variable linear regression analysis, the independent factor associated with plasma PAI-1 level was &minus;675 4G/5G polymorphism (regression coefficient β = 4.6, P Conclusion: the present study identifies &minus;675 4G/5G not &minus;844 G/A polymorphism of PAI gene as the principal determinant of plasma PAI-1 level in Tunisian T2D patients, the android fat distribution, dyslipidemia and hyperglycemia play a modest role in this variation.

Expression and prognostic value of plasminogen activator inhibitor type 1 in node-negative breast cancer

Objective:To investigate the expressions of plasminogen activator inhibitor type 1 (PAI-1), C-erbB-2, VEGF and Ki-67 by immunohistostaining and then to evaluate the prognostic value of PAI-1 in node-negative breast cancer. Methods:The study included a retrospective series of 62 female patients with axillary lymph node-negative breast cancer. Expressions of PAI-1, C-erbB-2, VEGF and Ki-67 were determined by immunohistostaining on formalin-fixed paraffin-embedded tissue sections from these patients after a median follow-up of 69 months (range 22–117 months). Correlations with well known clinicopathologic factors were assessed and multivariate survival analyses were performed. Results: High PAI-1 level was positively associated with high histologic grade of the tumors. Disease-free survival (DFS) was significantly shorter for the patients with moderate to intensive expression of PAI-1 than for those with negative (χ2 = 25.46, P < 0.001; χ2 = 23.07, P < 0.001) to mild expression (χ2 = 19.75, P < 0.001; χ2 = 17.40, P < 0.001). Although on univariate analysis of the prognostic factors, tumor size, location of primary tumor and age as well as expressions of PAI-1, VEGF and Ki-67 were all significantly prognostic factors for DFS (P < 0.05), PAI-1 was the only independent prognostic factor on multivariate analysis (P<0.0001; hazard ratio [HR], 4.041; 95% confidence interval [CI], 1.928–8.468). Conclusion: These results of the current study indicate that intermediate or high expression of PAI-1 represents a strong and independent unfavorable prognostic factor for the de-velopment of recurrence or metastases in axillary node-negative breast cancer.

Association of plasminogen activator inhibitor-1 4G/5G promoter polymorphism with recurrent cerebral infarction in China’s North Jiangsu Province

BACKGROUND： Many international studies have shown that plasminogen activator inhibitor-1 （PAl-l） 4G/5G promoter polymorphism does not increase the risk for cerebral infarction. OBJECTIVE： Using PCR methodology and agarose electrophoresis to detect PAI-1 4G/5G promoter polymorphism in patients with recurrent cerebral infarction in the North Jiangsu Province of China, and to compare results with healthy subjects and patients with first-occurrence cerebral infarction in the same region. DESIGN, TIME AND SETTING： Non-randomized, concurrent, control trial. A total of 122 cerebral infarction patients were admitted to Xuzhou Medical College Hospital＇s Department of Neurology and Xuzhou Central Hospital＇s Department of Neurology between July 2003 and August 2006. PARTICIPANTS： The patients consisted of 63 males and 59 females, aged （62 ± 10） years. They were divided into first-occurrence （n = 58） and recurrence （n = 64） groups. In addition, 50 healthy subjects that underwent physical examination in the outpatient department, including 26 males and 24 females, aged （60 ±12） years, were selected as controls. METHODS AND MAIN OUTCOME MEASURES： PAl-1 4G/5G promoter polymorphism was detected and analyzed using PCR methodology and agarose electrophoresis. RESULTS： Significant differences were determined in terms of genotypic frequency and allele frequency of PAI-1 4G/5G promoter polymorphism, in patients with first-occurrence or recurrent cerebral infarction, when compared with healthy subjects （P 〈 0.05）. There was, however, no significant difference between the first-occurrence and recurrence groups （P 〉 0.05）. CONCLUSION： PAl- 1 4G/5G promoter polymorphism is genetic risk factor for cerebral infarction in China. However, it may be associated with recurrence of cerebral infarction in patients from the North Jiangsu Province of China.

Study on Effect of Different Dosages of Ligustrazine on Level of Plasminogen Activator Inhibitor-1 Activity in Type 2 Diabetes Mellitus Patients

Objective: To observe the effect of different dosages of ligustrazine (LG) on the level of plasminogen activator inhibitor-1 (PAI-1) activity in patients with type 2 diabetes mellitus. Methods: Ninety cases of type 2 diabetes mellitus inpatients were selected, and randomly divided into LG small dosage group (SDG), LG large dosage group (LDG) and control group. The 120 mg LG, 400 mg LG and normal saline 250 ml were given through intravenous dripping respectively, once daily, 20 days as one treatment course. Before and after treatment, all the patients had their fasting blood taken for PAI-1 and tissue plasminogen activator (t-PA) assessment test to perform the comparative study. Results:Seventy-three out of the 90 patients completed the observation course, the PAI-1 activity of three groups after treatment all lowered compared with that before treatment, and the difference between groups was also significant (all P<0. 01). After treatment the PAI-1 level of SDG and LDG of LG were all markedly lowered (all P<0. 01), the LDG's lowering was more evident than that of SDG, and comparison between these two groups of patients showed significant difference (P<0. 01). Although in the control group there was some difference between before and after treatment, it was not so significant like the above-mentioned two groups (P = 0. 0140). No adverse reaction occurred in the 3 groups during the observation period. Conclusion:LG could safely and effectively lower type 2 diabetes mellitus patient's plasma PAI-1 activity level, and LDG of LG proved to be particularly effective.

EFFECTS OF TGF-β_1 ON THE EXPRESSION OF PLASMINOGEN ACTIVATOR INHIBITOR TYPE 1 IN CULTURED HUMAN RENAL INTERSTITIAL FIBROBLASTS

Objective To investigate the effects of transforming growth factor-β1 (TGF-β1 ) on the expression of plasminogen activator inhibitor type 1 (PAI-1 ) mRNA in renal interstitial fibrosis in vitro. Methods Human renal interstitial fibroblasts were isolated and cultured in vitro. The cells wers stimulated by TGF-β1 with different concentration (0 to 10ng/ml ) at different time (0 to 48h). The expression of PAI-1 mRNA was assayed by RT-PCR. Results TGF-β1, had dose-dependent and time-dependent effects on the expression of PAI-1 mRNA in renal interstitial fibroblasts. Conclusion TGF-β1 may partic- ipate in renal fibrosis with inducing the expression of PAI-1 mRNA in renal fibroblasts and affecting the synthesis and degradation of extracellular matrix (ECM).

超声衰减参数联合血清PAI-1和ALT水平评估代谢相关脂肪性肝病患者肝脂肪变性程度的价值分析

目的分析超声衰减参数(UAP)联合血清纤溶酶原激活物抑制物1(PAI-1)和丙氨酸氨基转移酶(ALT)水平评估代谢相关性脂肪性肝病(MAFLD)患者肝脂肪变性程度的效能。方法2019年3月~2022年12月我院诊治的112例MAFLD患者均接受肝穿刺活检,所有受试者接受iLivTouch瞬时弹性成像检测UAP,采用ELISA法检测血清PAI-1水平,应用受试者工作特征(ROC)曲线分析UAP联合血清PAI-1和ALT水平评估MAFLD患者肝脂肪变性程度的效能。结果在112例MAFLD患者中,经肝组织病理学检查发现肝脂肪变1级(轻度)45例,2级(中度)42例和3级(重度)25例;重度肝脂肪变患者BMI、血清TC、TG和LDL-C水平分别为(32.6±2.4)kg/m^(2)、(6.6±0.9)mmol/L、(4.6±1.4)mmol/L和(4.0±0.9)mmol/L,显著高于中度患者【分别为(27.6±1.9)kg/m^(2)、(5.8±0.8)mmol/L、(3.5±0.9)mmol/L和(3.5±0.7)mmol/L,P<0.05】或轻度患者【分别为(24.1±0.9)kg/m^(2)、(5.1±0.7)mmol/L、(2.2±0.7)mmol/L和(3.0±0.5)mmol/L,P<0.05】,而血清HDL-C水平为(1.2±0.2)mmol/L,显著低于中度【(1.4±0.2)mmol/L,P<0.05】或轻度患者【(1.4±0.2)mmol/L,P<0.05】;重度组UAP、血清PAI-1和ALT水平分别为(312.7±32.6)dB/m、(36.5±4.2)mg/mL和(72.1±7.4)U/L,显著高于中度组【分别为(284.2±30.1)dB/m、(28.1±3.4)mg/mL和(36.3±4.1)U/L,P<0.05】或轻度组【分别为(257.4±26.4)dB/m、(20.4±2.4)mg/mL和(23.7±2.5)U/L,P<0.05】;ROC曲线分析显示,UAP联合血清PAI-1和ALT水平评估重度肝脂肪变性的曲线下面积(AUC)、特异度和敏感度分别为0.914(95%CI:0.883~0.990)、89.6%和93.3%,其特异度显著优于单一指标预测(P<0.05)。结论应用UAP联合血清PAI-1和ALT水平预测MAFLD患者严重肝脂肪变性有良好的评估价值,可为临床诊治提供参考依据。

尤瑞克林治疗急性脑梗死对患者血清1型纤溶酶原激活物抑制剂水平及血小板参数的影响

目的探究尤瑞克林治疗急性脑梗死对患者血清1型纤溶酶原激活物抑制剂(PAI-1)水平及血小板参数的影响。方法回顾性分析2020年1月至2022年5月丰城市人民医院收治的82例急性脑梗死患者的临床资料,根据使用药物不同分为观察组(n=47)与对照组(n=35)。对照组采用阿司匹林联合氯吡格雷治疗,观察组在对照组基础上联合尤瑞克林治疗。比较两组临床疗效、美国国立卫生研究院卒中量表(NIHSS)、血清PAI-1、血小板计数(PLT)、血小板体积分布宽度(PDW)、血小板平均体积(MPV)、血小板压积(PCT)、血小板黏附率(PAdT)、血小板聚集率(PAgT)、全血黏度、血浆黏度、不良反应发生率。结果观察组治疗总有效率为89.36%,高于对照组的71.43%,差异有统计学意义(P<0.05)。治疗前、治疗7 d,两组NIHSS评分比较差异无统计学意义;治疗14 d,观察组NIHSS评分低于对照组,差异有统计学意义(P<0.05)。治疗14 d,两组血清PAI-1水平均低于治疗前,且观察组低于对照组,差异有统计学意义(P<0.05)。治疗14 d,两组PLT均高于治疗前,PDW均窄于治疗前,MPV、PCT均小于治疗前,PAdT、PagT均低于治疗前,且观察组PLT高于对照组,PDW窄于对照组,MPV、PCT均小于对照组,PAdT、PagT均低于对照组,差异有统计学意义(P<0.05)。治疗14 d,两组全血黏度、血浆黏度均低于治疗前,且观察组低于对照组,差异有统计学意义(P<0.05)。两组不良反应发生率比较差异无统计学意义。结论尤瑞克林治疗急性脑梗死效果显著,可降低患者血清PAI-1水平及全血黏度、血浆黏度,改善血小板参数,值得临床推广应用。

股骨颈骨折内固定术后血清学指标PAI-1作为股骨头坏死并发症风险因素的探究

目的 探究股骨颈骨折内固定术后股骨头坏死的风险因素,明确血清学指标纤溶酶原激活物抑制剂-1(PAI-1)对股骨头坏死的预测价值。方法 纳入该院2021年1月至2022年1月收治的股骨颈骨折内固定术患者95例。获取患者相关临床信息,并检测患者术前,术后1、2和3 d血清PAI-1水平;术后随访1年时间,根据患者是否发生股骨头坏死将患者分为坏死组和无坏死组;在术后1年收集所有患者视觉模拟评分(VAS)、西安大略麦克马斯特大学骨关节炎指数(WOMAC)和Harris髋关节评分(HHS)情况;比较坏死组和无坏死组患者的临床信息和术前、术后血清PAI-1水平差异,明确股骨头坏死的相关风险因素并进行Logistic回归分析;探究术后血清PAI-1水平与患者VAS、WOMAC和HHS之间的关系;绘制血清PAI-1作为股骨头坏死预测指标的受试者工作特征(ROC)曲线,明确其预测价值。结果 坏死组和无坏死组Garden分型、复位质量比较差异有统计学意义(P<0.05),坏死组术后1、2 d血清PAI-1水平均高于无坏死组(P<0.05);患者术后1、2 d血清PAI-1水平与VAS和WOMAC呈正相关(P<0.05),与HHS呈负相关(P<0.05);Logistic回归分析结果显示,术后1、2 d血清PAI-1水平升高是股骨头坏死的危险因素(P<0.05);ROC曲线结果显示,术后2 d血清PAI-1水平相较于术后1 d血清PAI-1水平预测价值更高,术后2 d血清PAI-1水平预测股骨头坏死的最佳截断值为44.8 ng/L,灵敏度为68.49%,特异度为86.36%,曲线下面积(AUC)为0.807。结论 股骨颈骨折内固定术后1、2 d血清PAI-1水平可用于预测术后股骨头坏死的发生,尤其是术后2 d血清PAI-1水平。

脓毒症合并心肌损伤患者血清t-PAI-C、HBP、HMGB1水平与预后的关系研究

目的 探究脓毒症合并心肌损伤患者血清组织纤溶酶原激活物-纤溶酶原激活物抑剂-1复合物(t-PAI-C)、肝素结合蛋白(HBP)、外周血高迁移率组蛋白B1(HMGB1)水平与其预后的关系。方法 回顾性分析2020年3月至2023年3月蚌埠医学院第一附属医院收治的105例脓毒症合并心肌损伤患者的临床资料,依据患者治疗后28 d存活情况将其分为存活组与死亡组。比较两组临床资料(性别、年龄、体重指数、感染部位、平均动脉压、射血分数)、血清心肌肌钙蛋白I(cTnI)、t-PAI-C、HBP、HMGB1水平以及急性生理学和慢性健康状况评价Ⅱ(APACHEⅡ)评分,分析影响脓毒症合并心肌损伤患者预后的影响因素;探究t-PAI-C、HBP、HMGB1水平与cTnI、APACHEⅡ评分的相关性;绘制受试者工作特征(ROC)曲线分析t-PAI-C、HBP、HMGB1诊断脓毒症合并心肌损伤患者预后的价值。结果 脓毒症合并心肌损伤患者随访期间出现死亡30例(28.57%),存活75例(71.43%)。死亡组患者的cTnI、t-PAI-C、HBP、HMGB1水平以及APACHEⅡ评分分别为(1.58±0.43)μg/L、(16.75±4.00)ng/mL、(45.68±9.25)ng/mL、(125.00±20.18)μg/L、(17.63±2.66)分,均高于存活组[(0.65±0.11)μg/L、(13.20±2.68)ng/mL、(38.00±8.63)ng/mL、(96.69±11.25)μg/L、(11.50±1.68)分],差异均有统计学意义(P<0.05)。cTnI、t-PAI-C、HBP、HMGB1以及APACHEⅡ评分均为影响脓毒症合并心肌损伤患者预后的独立危险因素(P<0.05)。t-PAI-C、HBP、HMGB1与cTnI、APACHEⅡ评分之间均呈正相关(P<0.05)。t-PAI-C、HBP、HMGB1三者联合诊断脓毒症合并心肌损伤患者预后的曲线下面积(AUC)为0.950(0.889~0.983),敏感度与特异度分别为83.33%和93.33%,诊断效能均优于单一的t-PAI-C、HBP、HMGB1指标(P<0.05)。结论 t-PAI-C、HBP、HMGB1水平与cTnI、APACHEⅡ评分相关性较好,可作为临床诊断脓毒症合并心肌损伤的潜在生物学标记物,三者联合预测脓毒症合并心肌损伤患者预后效能较好。

血浆纤溶酶原激活剂抑制物-1联合C反应蛋白与白蛋白比值对老年脓毒症患者28天预后的评估价值

目的 探讨纤溶酶原激活剂抑制物-1(PAI-1)联合C反应蛋白与白蛋白比值(CAR)对老年脓毒症患者28 d预后的预测价值。方法 90例老年脓毒症患者作为研究组,30名同期老年体检健康者作为对照组;比较研究组入院次日、对照组体检当日的血浆PAI-1水平和CAR,记录研究组的白细胞计数、血小板计数及淋巴细胞计数,计算序贯器官衰竭评分(SOFA)和急性生理学与慢性健康状况评分Ⅱ(APACHEⅡ);分析老年脓毒症患者血浆PAI-1水平和CAR与病情严重程度的相关性,不同预后(根据患者28 d的生存结局分为生存组和死亡组)老年脓毒症患者一般资料、实验室指标及血浆PAI-1水平和CAR,采用多因素logistic回归分析影响老年脓毒症患者28 d预后的独立危险因素,采用受试者工作特征(ROC)曲线下面积(AUC)评价血浆PAI-1、CAR对老年脓毒症患者入院28 d预后的预测价值。结果 研究组血浆PAI-1水平和CAR均高于对照组,差异有统计学意义(P<0.05);老年脓毒症患者血浆PAI-1、CAR与SOFA评分、APACHEⅡ评分分别呈正相关关系(P<0.05);28天内,老年脓毒症患者死亡31例(34.44%)、存活59例(65.56%),生存组的淋巴细胞计数高于死亡组,SOFA评分、血浆PAI-1水平及CAR低于死亡组(P<0.05);多因素logistic回归分析结果表明血浆PAI-1水平和CAR是影响老年脓毒症患者28 d预后的独立危险因素(P<0.05),ROC曲线分析结果显示,血浆PAI-1、CAR及两者联合预测老年脓毒症患者28 d内死亡的AUC分别为0.752(95%CI为0.642~0.862,P<0.001),0.842(95%CI为0.745~0.939,P<0.001)及0.887(95%CI为0.796~0.977,P<0.001)。结论 老年脓毒症患者的血浆PAI-1水平和CAR升高,两者联合对患者28 d预后具有较好的预测价值。

慢性阻塞性肺疾病急性加重期患者血清CCR5、PAI-1水平与肺功能及病情严重程度的关系

目的 探究慢性阻塞性肺疾病急性加重期(AECOPD)患者血清细胞趋化因子受体5(CCR5)、纤溶酶原激活物抑制剂-1(PAI-1)水平变化与肺功能及病情严重程度之间的关系。方法 选取该院2020年1月至2022年1月急诊收治的114例AECOPD患者为AECOPD组,并选取同期稳定期慢性阻塞性肺疾病(COPD)患者114例为对照组。采用酶联免疫吸附试验(ELISA)测定CCR5、PAI-1水平;比较AECOPD组与对照组及不同病情程度AECOPD患者血清CCR5、PAI-1水平及肺功能指标;Pearson相关性分析AECOPD患者血清CCR5、PAI-1水平与肺功能指标之间的关系;Spearman相关性分析AECOPD患者血清CCR5、PAI-1水平与病情严重程度之间的关系。结果 与对照组相比,AECOPD组患者血清CCR5、PAI-1水平均显著升高,差异均有统计学意义(P<0.05),肺功能指标:第1秒用力呼气量(FEV_(1))、FEV_(1)与用力肺活量比值(FEV_(1)/FVC)、FEV_(1)占预计值百分比(FEV_(1)%pred)、最大呼气中期流量(MMEF)占预计值百分比(MMEF%pred)均显著降低,差异有统计学意义(P<0.05),且随着病情程度的增加,血清CCR5、PAI-1水平逐渐增加(P<0.05),FEV_(1)、FEV_(1)/FVC、FEV_(1)%pred、MMEF%pred水平逐渐降低(P<0.05);Pearson相关性分析结果显示,血清CCR5、PAI-1水平与FEV_(1)、FEV_(1)/FVC、FEV_(1)%pred、MMEF%pred均呈显著负相关(P<0.05);Spearman相关性分析结果显示,AECOPD患者血清CCR5、PAI-1水平与病情程度呈显著正相关(r_(1)=0.432,r_(2)=0.451,P<0.05)。结论 AECOPD患者血清CCR5、PAI-1水平显著升高,且血清CCR5、PAI-1水平与AECOPD患者肺功能及病情程度密切相关。

血清PAI-1、Flk-1与深部浸润型子宫内膜异位症及其腹腔镜保守治疗效果的关系研究

目的 分析血清纤溶酶原激活物抑制物(PAI)-1、胎肝激酶-1(Flk-1)与深部浸润型子宫内膜异位症(DIE)及其腹腔镜保守治疗效果的关系。方法 回顾性选择自2020年1月至2022年11月在淄博市妇幼保健院行腹腔镜保守治疗的120例子宫内膜异位症患者作为研究对象。根据是否为DIE分为DIE组(n=48)和非DIE组(n=72)。比较DIE组与非DIE组的年龄、病程、癌抗原125(CA125)、美国生育学会修正分期法(r-AFS)评分、血清PAI-1及Flk-1表达水平;分析DIE患者血清PAI-1、Flk-1表达水平与病程、CA125、r-AFS评分的关系;采用受试者工作特征(ROC)曲线评价血清PAI-1、Flk-1对腹腔镜保守治疗后病情复发的预测效能。结果 DIE组病程为(7.42±4.56)年,长于非DIE组[(5.12±2.18)年],CA125水平、r-AFS评分及PAI-1、Flk-1表达水平分别为(61.42±8.75) kU/L、(47.57±6.08)分、(231.47±46.87) mg/L、(52.42±10.17) ng/mL,均高于非DIE组[(43.08±4.67) kU/L、(34.25±4.26)分、(156.24±16.93) mg/L、(21.65±4.53) ng/mL],差异均有统计学意义(P<0.05)。经多因素Logistic回归分析,病程、CA125、r-AFS评分、PAI-1、Flk-1均是DIE的独立危险因素(P<0.05)。经Pearson相关性分析,DIE患者血清PAI-1、Flk-1表达水平均与病程、CA125水平、r-AFS评分呈正相关(P<0.05)。在48例DIE患者中,腹腔镜保守治疗无效6例,占12.50%;无效患者血清PAI-1、Flk-1表达水平均高于有效患者,差异均有统计学意义(P<0.05)。经ROC曲线分析结果显示,血清PAI-1联合Flk-1预测DIE患者腹腔镜保守治疗后病情复发的曲线下面积(AUC)为0.931。结论 血清PAI-1、Flk-1与DIE严重程度密切相关,联合应用可提高对腹腔镜保守治疗后病情复发的预测效能。

中性粒细胞外诱捕网、纤溶酶原激活抑制剂1对早产急性呼吸窘迫综合征患儿预后的影响

目的探讨中性粒细胞外诱捕网(NETs)、纤溶酶原激活抑制剂1(PAI-1)对早产急性呼吸窘迫综合征(ARDS)患儿预后的影响。方法选取2020年1月至2022年12月北京市通州区妇幼保健院收治的早产ARDS患儿125例作为ARDS组,根据患儿预后将其分为预后良好组和预后不良组。比较两组血浆游离DNA(cf-DNA)、中性粒细胞弹性蛋白酶(NE)和肿瘤坏死因子-α(TNF-α)、PAI-1水平;分析早产ARDS患儿cf-DNA与NE、TNF-α的相关性;分析早产ARDS患儿预后不良的影响因素;cf-DNA、PAI-1对早产ARDS患儿预后不良的预测价值采用受试者操作特征曲线评估。结果125例早产ARDS患儿预后不良47例,预后良好78例。预后不良组cf-DNA、NE、TNF-α、PAI-1水平高于预后良好组(P<0.05)。早产ARDS患儿cf-DNA与NE、TNF-α呈正相关(r=0.645、0.687,P<0.05)。cf-DNA、PAI-1水平升高是早产ARDS患儿预后不良的危险因素(OR=2.188、2.303,P<0.05)。cf-DNA、PAI-1联合预测早产ARDS患儿预后不良的曲线下面积高于各指标单独预测(Z=3.272、2.229,P<0.05)。结论NETs组成成分cf-DNA、PAI-1水平升高是早产ARDS患儿预后不良的危险因素,二者联合检测对患儿的预后具有较高的预测效能。

早孕先兆流产患者血FVⅢ活性、PAI-1水平及其对保胎结局的影响

目的:探究凝血因子Ⅲ(FVⅢ)活性、纤溶酶原激活物抑制剂-1(PAI-1)对早孕先兆流产保胎结局的预测价值。方法:回顾性分析本院于2020年1月-2022年12月收治的345例早孕先兆流产患者临床资料,根据保胎结局分为保胎失败组124例、成功组221例,检测两组血FVⅢ活性、PAI-1水平,超声检测子宫内膜厚度(EST),血清β-人绒毛膜促性腺激素(β-hCG)、雌二醇(E_(2))、孕酮(P),采用多因素logistic回归分析早孕先兆流产保胎成功影响因素。结果:失败组FVⅢ活性(168.31±25.84)%、PAI-1(54.39±6.05μg/l)均高于成功组(138.64±24.61)%、(49.31±5.87μg/l),EST(10.06±3.26 mm)、β-hCG(1763.86±706.77 U/L)、E_(2)(1051.16±369.57 poml/L)、P(32.96±15.72 noml/L)水平均低于成功组(12.55±1.91 mm、3299.46±1831.59 U/L、3571.36±1126.29 poml/L、64.38±17.24 noml/L)(均P<0.05)。多因素logistic回归分析显示,FVⅢ活性升高,β-hCG、E_(2)、P水平降低为影响早孕先兆流产保胎成功的危险因素(P<0.05),而PAI-1为保胎成功非危险因素。结论:FVⅢ活性升高影响保胎成功,临床可予以参考,减少盲目保胎带来的风险。

尼卡地平联合酚妥拉明对妊高征患者血清AGEs、PAI-1及儿茶酚抑素水平的影响

目的 观察尼卡地平联合酚妥拉明对妊娠高血压综合征(简称妊高征)患者血清晚期糖基化终末产物(AGEs)、纤溶酶原激活物抑制剂-1(PAI-1)及儿茶酚抑素(CST)水平的影响。方法 按随机数字表法将2021年3月至2023年3月于乐平市妇幼保健院收治的96例妊高征患者随机分为两组,各48例。对照组采用酚妥拉明治疗,观察组加用尼卡地平治疗。比较两组临床疗效,血清AGEs、PAI-1、CST水平,血压指标,血流动力学,妊娠结局以及不良反应。结果 观察组总有效率较对照组高(P<0.05)。治疗后,观察组AGEs、PAI-1、CST水平均较对照组低(P<0.05);观察组收缩压、舒张压、脐血流、外周阻力等指标水平均较对照组低(P<0.05);观察组不良妊娠结局总发生率较对照组低(P<0.05)。两组不良反应总发生率比较差异无统计学意义(P>0.05)。结论 尼卡地平联合酚妥拉明用于治疗妊高征患者的效果较好,能够明显改善患者血清AGEs、PAI-1、CST水平,降低其血压指标,改善血流动力学与母婴妊娠结局,且应用安全性较高,临床应用效果较好。

外周血sLox-1、tPAI-1水平与冠心病PCI术后MACE发生的关系

目的:研究外周血可溶性凝集素样氧化型低密度脂蛋白受体-1(sLox-1)、组织纤维蛋白溶解酶原激活物抑制剂-1(tPAI-1)水平与冠心病经皮冠状动脉介入术(PCI)后不良心血管事件(MACE)发生的关系。方法:选取161例行PCI术治疗的冠心病病人作为观察组,同期选取健康体检志愿者56名作为对照组,检测并比较2组外周血sLox-1、tPAI-1水平。观察组病人随访观察12个月,根据病人在随访期间是否发生MACE分为MACE组和非MACE组,分析冠心病病人PCI术后发生MACE的影响因素。结果:观察组外周血sLox-1、tPAI-1水平均明显高于对照组(P<0.01)。单因素分析显示,MACE组病人cTnI、hs-CRP、sLox-1、tPAI-1水平均明显高于非MACE组(P<0.01);logistic回归分析显示,cTnI、hs-CRP、sLox-1、tPAI-1水平均为冠心病PCI术后MACE的独立危险因素(P<0.01)。ROC曲线分析显示,外周血sLox-1联合tPAI-1水平预测冠心病病人PCI术后MACE的灵敏度、准确度、AUC分别为91.37%、93.12%、0.901,均高于外周血sLox-1、tPAI-1单独预测。结论:冠心病病人PCI术后外周血sLox-1、tPAI-1水平升高为术后MACE的危险因素,二者联合对冠心病PCI术后MACE具有较高预测价值。

tPA Involvement in Ovulation──Studies on Mechanism of Ovulation：Role of Tissue Type Plasminogen Activator

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PAI-1基因4G/5G多态性与行羟氯喹联合肝素治疗的不明原因复发性流产妊娠结局的相关性

目的探究纤溶酶原激活物抑制物-1(PAI-1)基因4G/5G多态性与行羟氯喹联合肝素治疗不明原因复发性流产(URSA)患者妊娠结局的相关性。方法选取2019年1月至2021年1月肇庆市第一人民医院收治的138例URSA患者为研究对象,检测所有受试者PAI-1基因4G/5G位点基因多态性。患者均采用羟氯喹联合肝素治疗,根据妊娠结局分为良好妊娠结局组和不良妊娠结局组。观察两组间PAI-1基因4G/5G基因位点基因型及等位基因的分布差异,并分析PAI-1基因4G/5G位点基因多态性与行羟氯喹联合肝素治疗URSA患者妊娠结局的相关性。结果138例患者中117例患者在治疗后妊娠成功,妊娠成功率为84.78%(117/138)。117例妊娠成功的患者中6例失访,失访率为5.13%(6/117)。111例患者中流产22例,低体质量儿6例,死胎、新生儿死亡各2例,不良妊娠结局发生率为28.83%(32/111)。两组职业类别、工作性质、PAI-1基因型分布比较差异有统计学意义(P<0.05或P<0.01),不良妊娠结局组大专及以上的比例低于良好妊娠结局组[37.50%(12/32)比60.76%(48/79)](P<0.05),生化妊娠史占比高于良好妊娠结局组[81.25%(26/32)比50.63%(40/79)](P<0.01)。不良妊娠结局组PAI-1基因4G等位基因频率高于良好妊娠结局组[65.63%(42/64)比37.97%(60/158)](P<0.01)。多因素Logistic回归分析结果显示,PAI-1基因型4G/4G、4G等位基因及生化妊娠史是行羟氯喹联合肝素治疗URSA患者不良妊娠结局发生的危险因素(OR=3.747,95%CI 1.470~6.024;OR=4.204,95%CI 1.672~6.736;OR=2.672,95%CI 1.269~4.076)(P<0.01)。结论PAI-1基因型4G/4G和4G等位基因与行羟氯喹联合肝素治疗URSA患者发生不良妊娠结局关系密切,是导致行羟氯喹联合肝素治疗URSA患者不良妊娠结局发生的危险因素。